- Email: [email protected]
Cryptococcus meningitis in a child successfully treated with amphotericin B, with a review of the pediatric literature
The Journal of P E D I A T R I C S
577
Cryptococcus meningitis in treated Mtb amplootericin B, vitb a review of the pediatric literature B. Emanuel, M.D., ~ E. Ching, M.D., A. D. Lieberman, M.D., and M. Goldin, M.S. CHICAGO~
ILL.
also known a s torulosis or European blastomycosis, is a mycotic disease of m a n and animals caused by Cryptococcus neoformans (Torula histoIytica or Cryptococcus hom{nis). T h e first case reported was by Zenker 1 in 1861 in a m a n dying from a fungous infection involving the central nervous system, and it is most probable that the organism was C. neoformans. Biisse 2 and Buschke S independently recovered yeastlike organisms f r o m a w o m a n with bone lesions who died from generalized involvement. Tile organisms w e r e referred to as Saccharomyces neoformans. Vuillemin 4 recognized the lack of ascospores, thus differentiating it from true yeast, and called it C. homlnls. T h e generic term Cryptococcus was used or given by KiltC R Y P T O C O C C O S I S ~
From the Departments o[ Pediatrics and Microbiology, Chicago Medical School, and Mount Sinai Hospital, Chicago, Ill. e'Address, Department o[ Ped{atr{cs, Mount S{nai Hospital, Cali[ornla Avenue at 15th Street, Chicago 8, Ill.
zing2 I n 1902, Frothingham G recovered the organism from a pulmonary lesion in a horse, and Von H a n s e m a n n 7 in 1905 recovered the organism for the first time from a m a n dying of meningitis. I n 1916, Stoddard and Cutler s recorded the clinical and pathologic features of the disease, described the morphologic and cultural characteristics of C. neoformans, and proved it to be a true yeast, reproduced by budding only. Because it fails to produce 'mycelium or ascospores, it is now classified with the anascosporogenous yeasts. I n Lodder's '~ classification Cryptococcus has 25 species, all saprophytic except C. neoformans. Saprophytic strains are Widespread in nature, 1~ and are found in soil, 11 food, and the skin and gastrointestinal tract of m a n ~2 and animals. 1~ Pathogenic strains have been recovered from peachesff 3 milk, and from the oropharynx, gastrointestinal and vaginal tracts of apparently healthy carriers? 4 Some relation seems to exist to pigeon manure. 10 T h e yeasts are thought to enter the body
5 78
Eraanuel et al.
F i g . 1. R i g h t m i t t i n g film.
middle
lobe i n f i l t r a t e s e e n o n a d -
through the respiratory tract, which explains the frequency of lung involvement, 14 although the tonsils and skin are considered the portal of entry by Freeman? 5 Cryptococcosis is world wide in distribution but the largest number of cases has been reported in the United States, where approximately 450 cases have been recorded in adults. The actual incidence of the disease cannot be estimated accurately by the number of published cases. Alteration of the host-parasite relationship, disturbance in the reticuloendothelial system, and debilitating disease contribute to the lowering of resistance to the organisms. Coexistence of cryptococcosis with Hodgkin's disease, 2~ leukemia, reticulum cell sarcoma,2~, 27 histoplasmosis,2S tuberculosis,2S moniliasis, 2~ and diabetes 2~ have been previously described. The organism most likely reaches the central nervous system by way of the blood stream, 16 producing 3 varied types of pathologic pictures: (1) meningitis, where the subarachnoid space of the base of the brain is most frequently involved; (2) meningoencephalitis, where the gray matter is mostly
October 1961
affected with a honeycomb appearance of the cortex, basal ganglia, brain stem, thalamus, or cerebellum; and (3) cryptococcal granuloma, which is frequently found in the cerebellum and cerebrum. Other organl~ such as the lung, liver, spleen, skin, and lymph nodes are less frequently involved. 14 In 1937 Levin ~7 reviewed the literature and since then numerous other reviews have been published,14, 18, 19 but none in the pediatric literature. The prognosis, except for the localized, cutaneous type, is grave, especially when the central nervous system is involved. Until the advent of amphotericin B, ~ these cases were nearly always fatal. We have recently encountered in a child a case of C. neoformans meningitis associated with tuberculosis of the lung. To our knowledge, this is the first child with cryptocoecal meningitis to have apparently recovered completely when treated with amphotericin B. Certain aspects of this case will be discussed and the review of the pediatric literature on cryptococeal meningitis is included. CASE
REPORT
G. H.,t an 18-month-old Negro boy, was brought in a comatose condition to the emergency room of the Mount Sinai Hospital, Chicago, on Aug. 21, 1960, with tonic and clonic convulsions and a temperature of 104 ~ F. For about one month prior to admission, the child had had frequent colds, a cough, and fever but improved when given penicillin by a local physician. Three days prior to admission, the child again developed a dry cough, rhinorrhea, and fever. On the day of admission, shortness of breath was also noted. In the emergency room, the child was comatose; the pupils were equal, dilated, and unresponsive to light. There was a slight ptosis of the left eyelid, the neck was supple,
"X'The trade-mark of E. R, Squibb & Sons for amphoterlcln B is Fungizone. tFrom the service of Dr. H. S. Go/don.
Volume 59 Number 4
Amphotericin B in cryptococcus meningitis
and Kernig's, Brudzinski's, and Babinski's signs could not be elicited. The throat was slightly reddened, the ears clear, and no significant Iymphadenopathy could be found. The breath sounds were harsh, but with no r~les or dullness to percussion. The heart was normal, but there was a tachycardia. The abdomen was soft, and no organs or masses could be felt. Phenobarbital, intramuscularly, and aspirin suppositories were given, but convulsions continued for another half hour. A roentgenogram of the chest was immediately taken and a moderate pneumonia of the right middle lobe of the Iung was visualized (Fig. 1). The fundi showed no papilledema, and a lumbar puncture was performed. The pressure was slightly elevated, and the clear fluid obtained included 217 cells per cubic millimeter, predominantly neutrop.hils. T h e protein was elevated, and the P a n @ test was positive. Glucose and chloride concentrations were normal. Organisms resembling Cryptococcus were seen in this specimen, but, unfortunately, no cultures were made on it. Examination of the blood showed a hemoglobin of 8.1 Gm. per 100 ml., hematocrit 28, red blood ceils 3.75 million per cubic millimeter, and color index 0.69. T h e leukocyte count was 8,100 per cubic millimeter with 3 per cent bands, 55 per cent neutrophils, 34 per cent tymphocytes, 5 per cent eosinophils, 2 per cent monocytes, and 1 per cent basophils. The sedimentation rate was 30 mm. per hour. '* The blood urea nitrogen was 18.5 rag. per cent. The child was given 1,000,000 units of penicillin, intravenously, twice a day; 250 mg. sulfadiazine, intravenously, every 6 hours; and 50 rag. per kilogram chloramphenicol, intramuscularly, every 6 hours. On the second hospital day, his neck become slightly rigid. A Mantoux test (t:10,000 OT.) was markedly positive after 24 hours. The child was then immediately placed on
*Wintrobe method.
579
para-amin0salicylic acid, 750 rag., 3 times a day; isoniazid, 100 mg., 3 times a day; streptomycin, 50 rag., intramuscularly, twice a day; and prednisone, 10 mg., twice a day. One the third hospital day, the patient was alert and free of convulsions. The lumbar puncture was repeated, the cell count was 207 per cubic millimeter; 90 per cent of them, however, were lymphocytes in this specimen. India ink preparations showed numerous encapsulated ceils morphologically typical of C. neoformans. A direct count of the organisms showed them to be greater than 10,000 per cubic millimeter. A diagnosis of cryptococcal meningitis was m a d e and amphotericin B, 15 mg. given intravenously in 500 ml. of dextrose in water with addition of 0.5 ml. heparin as a precaution against thrombophlebitis, was added to the therapeutic regimen. Potassium iodide was also given, starting at 3 drops twice a day and increased by 1 drop per day until a dose of 12 drops twice a day was reached. This was stopped on the sixty-second day of hospitalization when the lung lesion was felt to be a tuberculous rather than a cryptococcal granuloma. T h e history from the child's parents revealed that the patient was in close contact with an uncle who had been treated for tuberculosis since February, 1960. It was also learned that the child had been playing around pigeon excreta. The course of the disease and the treatment are shown in Fig. 2. The prednisone, chloramphenicol, and penicillin were discontinued after the third hospital day. The amphotericin B was given every other day or 3 times weekly when the blood urea nitrogen became abnormally elevated. This dosage was found to be best. During the last 2 weeks of therapy, amphotericin B was given once a week in a dose of 30 mg. Despite intensive drug therapy, liver function tests remained normal, and the drug was well tolerated. Throughout the long hospital course, every effort was made to isolate the tubercle bacillus from gastric washings, spinal fluids, and bronchial aspirations. All smears, cultures, and guinea pig inoculations were negative for acid-fast bacilli. Skin and serologic tests
5S..1
ioi ~
,io~"
la3"
I
I L
CPSC'SC"
I
\
\
1'
14
!
IAMPHOTEmC.,,ml
+
CHLORIDE
I
]
21
~lLl:&rll AZlN E
~J
PSC"
"lk.
'%
S'FREPTOMV ~iN
I f'
C" SO"
\~r \,~
\,o
I
,
.
58
THERAPY
§ ]
l
I--
42
49
[] [] []
PSC'
[]
88
[]
"
.
__-----------
.............
!
o
CPSC"
o
o
?0
l i l t -~= . . . . . . . . .
,
CHLORIDI~8 PROTEIN SUGAR CELLS
PROTEIN
C P S C'
-'---II. . . . . . . . . . . . . .
rNH
[] [] []
___
........
,
Fig. 2. Clinical course, therapy, and laboratory findings.
28
PAS
[] [] []
SPINAL TAPS
CELLS
. . . . . . . . . . . . .
:
BLOOD UREA NITROGEN
TEI~PERATURE
[]
CPSC"
77
[]
ILL.-'"
L
."
| ...............
.'
,
114
[]
I~0
P..PIr
Ill
r
P I
|10 9
r
0
BOO
Sl O00
I it] -,,o
1,
{000
lEO0
cr)
(3
0
CO C~
r
Volume 59 Number 4
Amphotericin B in cryptococcus meningitis
for blastomycosis, coccidioidomycosis, and histoplasmosis were all negative. The cryptococci were seen in large numbers in the first 5 specimens of spinal fluid, but none in the succeeding 4 specimens. The number of organisms, the size of the capsule, and the amount of budding diminished strikingly with each succeeding specimen. Every effort to culture the organism, however, failed. All animal inoculations were also negative. I t is probable that the intensive therapy with the antibiotics and amphotericin B were responsible for the negative cultures. Ordinarily, this organism grows with ease on ordinary laboratory media, either at room or incubator temperature.l~, 14 T h e child progressively improved during his hospitalization, although the lung lesion did not diminish in size (Figs. 3, 4, and 5). The child was discharged from the hospital after the spinal fluid findings returned to normal on his eighty-seventh hospital day. He was continued, however, on antituberculosis therapy. Five months after discharge, the child has remained in good health, is gaining weight, and is mentally normal, with a normal electroencephalogram. The pulmonary lesion has decreased in size on the continued antituberculosis therapy (Figs. 6A and 6B). REVIEW
OF THE
58 1
liver in 8, the spleen in 7, the kidney in 5, the eyes in 4, the skin in 3, the bones, adrenals, and thyroid in 2, and the pancreas, heart, and lymph nodes in 1. In the pediatric age group, cryptococcosis is also frequently associated with other diseases such as histoplasmosis, a9 moniliasis, 4a Hodgkin's disease, 37 sarcoidosis, ~6 and tuberculosis. 49 Cryptococcosis is a subacute or chronic
Fig. 3. Persisting lung lesion, 1 month later.
LITERATURE
T o date, including the report of the prcsent case, we have been able to find only 23 cases of cryptococcus meningitis in children less than 15 years of age. Table I summarizes the significant data on these cases. The ages of the patients ranged from 20 minutes post partum to 15 years of age. The presence of the disease in a 20-minute-old newborn ~s is definite evidence of the existence of a congenital cryptococcal infection. Of the 23 cases, 3 definite cases and 3 equivocal cases appeared in the neonatal period. The sex distribution, as in the adults, favors the males, although such a distribution is difficult to explain. The disease is not limited to the white race; 5 of the patients were Negroes. The brain and the meninges were involved in 23 cases, the lungs in 9, the
Fig. 4. Persistance of lung lesion, 2 months later,
58 2
E m a n u e l et al.
October 1961
T a b l e I. R e v i e w of tile w o r l d p e d i a t r i c l i t e r a t u r e
Duration
of
A g e , sex, race
symptoms be[ore Cerebrospinal Physical findings and admission presenting symptoms findings 4 weeks Diarrhea, irritability, drowsiness, No definite number and signs of meningeal irritacells, all lymphocytes tion 1'Pressure
Author Barlow 2~
Country Year Australia 1923
Carton and Mount 30
United States
1933
12, F, W
6 weeks
Reeves, Butt, and Hammack al
India
1938
15, F, W
9 months Headache, vomiting, stiff neck, 97 cells, mostly polymorphonublurred vision, cough, fever, clear leukocytes, emaciation, and optic atrophy lymphocytes later "]'Pressure at first, normal later Protein1'
Longmire and Goodwin a2
United States
1939
4, F, W
3 months Fever, dyspnea, convulsions, stu- 100 to 400 cells, por, deafness and blindness, polymorphonuemaciation, cyanosis, stiff neck, clear leukocytes and papilledema 75, lymphocytes 25 "]'Pressure Protein~" Glucose 35
D'Aunoy and Lafferty sa
United States
1939
7, M, N
Sudden
Stiff neck, semicoma, and acute 100 to 250 ceils illness ~'Pressure
Marshall and Teed 3~
United States
1942
9, F, W
6 weeks
Fever, headache, nausea, irritabil- 8 to 15 Cells ity, vomiting, much rigidity, 1"Pressure Kcrnig +, papilledema, and retinal hemorrhage
Dormer, et al. 3~ South Africa
1945
12, M, N
Hamilton and United Thompson aG States
1946
6, M, N
2 weeks
Debre, et a l Y
1946
12, M, W
Unknown
France
3, F, W
Headache, vomiting, poor vision, hyporeflexia, Babinski and Kernig +, left ptosis, sixth nerve palsy, papilledema, retinal hemorrhage and exudation, coma, and death
88 cells, 90% lymphocytes 1'Pressure Protein 100 Glucose 40
4 months Cough, headaches, anorexia, Many polymorphoweight loss, clubbing of fingers, nuclear leukocytes fever, and dullness in right upper chest
Malaise, anorexia, fever, head- 320 cells, mostly ache, vomiting, generalized conpolymorphonuvulsion, papilledema, stiff neck, clear Ieukocytes Brudzinski +, and hyporeflexia ~'Pressure Protein 180 Glucose ) I0
Headache, vomiting, fever, con- Not done vulsions, photophobia, opisthotonos, papilledema, hepatosplenomegaly, ulcer on neck, and mass over clavicle
Volume 59
Number 4
A m p h o t e r i c i n B in cryptococcus meningitis
5 83
Antimot-
Direct smear
tern diagnosis Yes
Duration of illness Organs involved 3 months Brain
Autopsy Treatment Yes None
Yes
5 weeks
Brain
No
Positive chest abscess aspiration
Yes
2 years
Brain
_
Positive from CSF
Positive from CSF
Yes
3 months Brain, meninges, lung, thyroid, liver spleen, and kidney
Positive from CSF
Positive from CSF
No
48 hours
Positive from CSF
Positive from CSF
Yes
5 months Brain
Sulfadiazine
Living, well, subnormal intelligence 4 years later
Positive from CSF
Positive in guinea pig
Yes
5 months Lung and brain
Sulfadiazine, KI
Postoperative meningitis following right upper pulmonary lobectomy Patient survived, no follow-up
Positive from CSF Positive from sputum
Positive from cisternal puncture; positive from sputum
Yes
Sulfadiazine
Chest x-ray--nonspecific lung infiltration Pneumoencephalogram--enlargement of one ventricle and other not visualized
Positive from CSF
Yes
KI
Coexisting Hodgkin's disease
of cryptocoeeus -Positive from CSF
Culture
Positive from CSF
Positive from CSF
Positive from CSF and chest abscess
aspiration
72 days
2 weeks
Brain
Skull x-ray showed signs of increased intracranial pressure
Sulfadiazine Skull x-ray--inTorula creased marking antigen, K I Chest x-ray--interlobar empyema CSF still positive 2 years later Reported to be well 9 years later, but with sequelae
Yes
Yes
Lungs
Skin, lungs, heart, spleen, liver, and brain
K I orally, NaI intravenously, 5 % NaI, and acriflavine intrathecally
Remarks Optic atrophy prior to death
Yes
584
E m a n u e l et al.
October 1961
Table I. Cont'd Duration
of Country
Year
Age, sex, race
symptoms before admission
Cox and Tolhurst ss
Australia
1946
7, M, W
5 weeks
Mider, Smith, and Bray a9
United States
1947
12, M, N
Greening and Menville 40
United States
1947
6, M, N
2 weeks
Upper respiratory infection, head- 300 cells, lymphoache, vomiting, convulsion, and cytes 30% stiff neck ]'Pressure ++Pandy Protein]` Glucose, normal
Cloward ~1
Hawaii
1948
51,/.~, M, Chinese
1 week
Septic temperature, headache, ir- 450 cells, lympho-. ritability, convulsions, paralysis, cytes 33 % retinal hemorrhages, and papiI- ?Pressure ledema Protein 114 to 140
Neuhauser and United Tucker ~42 States
1948
7 weeks, M, W
7 weeks
Vomiting, twitching, rigidity, hy- 27 to 36 cells, 75% drocephalus, cataract and cholymphocytes rioretinitis, ankle clonus, and Protein 1,400 Babinski + Glucose 69
Neuhauser and United Tucker ~ 2 States
1948
19 days, M, W
19 days
Jaundice since birth, hepatosplenomegaly, dark urine and clay stool, hydrocephalus, and malnourishment
Neuhauser and United Tucker *.42 States
1948
17 days, M, W
4 days
Irritability, convulsions, hypertonieity, frequent clonic motions of extremities, hepatosplenomegaly and chorioretinitis
Spicer, Hiatt, United and Kessel~3 States
1948
4 years
Headache and lethargy, repeated Cloudy episodes of pulmonary infiltra- "]'Pressure tion with chronic cough, and septic temperature
Nassau and WeinbergHeiruti 44
Israel
1948
12 days, M, W
5 days
Cyanosis and generalized convul- 5,000, later 263 sion, no nuchal rigidity, hypocells reflexia, Kernig +, splenomeg- Protein 238 to 240 aly, skin macular and papular Glucose 14 my. lesions, and hydrocephalus
Health 4~
United States
I950
27 days, IV[, W
Lepau, et al. ~6 United States
1953
10, F, N
Author
8, M, W
Physical findings and presenting symptoms
Cerebrospinal findings
Headache, vomiting, leg pain, 41 to 50 cells, 40 to semicoma, active deep reflex, 46% lymphoeytes paralysis of right leg and arm, ]`Pressure stiff neck, and papilledema Protein]"
3 months Weakness, weight loss, anorexia, fever, and red swollen sternoclavicular region which drained, generalized lymphadenopathy
Endophthalmitls with separation of retina
massive
_
3 months Anorexia, weakness and general- 2,720 cells, 95% ized lymphadenopathy, later polymorphonuheadache, fever, vomiting, clear leukocytes, coma, and death later 16,000 cells Protein 70 to 200 o GlUcose 10 to 20 C1 110 to 121
Volume 59
Number 4
Amphotericin B in cryptococcus meningitis
5 85
AntimOT-
Direct smear
of cryptoeoeeus
Culture
Positive from CSF
Positive from CSF
Positive from blood and bone marrow
Positive from CSF
_
Duration of illness
Yes
289
Au-
Organs involved
topsy
Treatment
Remarks
Lungs and brain
Yes
_
Chest x-ray--fibrosis and small nodules
Brain, liver, kidney, and bones
Yes
months
No
11 days
Yes
Positive from CSF
Yes
28 days
No
23 days
Associated with generalized histoplasmosis
No
KI, sulfadiazinc, and penicillin intrathecally
Died
Brain
Yes
Penicillin, sulfadiazine
Pneumoencephalogram performed Exploratory trephination for brain abscess-negative
Brain, eyes, and lungs
Yes
Skull x-ray---calcification of frontal region Punctate and calcification along ventricles
2 months Brain
Positive from CSF
_
Positive from CSF
tern diagnosis
Positive postmortem from CSF
No
4 days
Spleen, liver, brain, and bone
Yes
Skull x - r a y - - p u n c t a t e calcification of the brain
Positive postmortem from CSF
No
10 days
Brain, liver, spleen, kidney, lungs, and eyes
Yes
Skull x-ray calcifications of cortex and brain substance
Positive from CSF and urine
No
35 days
Brain, lungs, kidney, spleen, pancreas, adrenal, and liver
Yes
Sulfadiazine
Positive from CSF after death
No
Brain and skin
Yes
Penicillin, sulfadiazinc
Positive from CSF
No
27 days
Many organs including eyes and brain
Yes
Positive fl'om CSF, nose and throat
Yes
61 days
Brain
Yes
6 weeks
_
Associated with generalized candidiasis
Congenital origin Combined lesion with toxoplasmosis
Polymyxin B, Coexisting Boeck's intramussarco{d cularly, and nystatin intrathecally
586
October 1961
E m a n u e l et al.
T a b l e I. Cont'd Duration
of Year
.Age~ sex~ race
Soysal, Unat, Turkey and Tahsinglu 47
1954
7, M, W
Oliviera Campos 4s
Portugal
1955 32 weeks, premature, F, W
Nanda, et al. ~9 United States
1956 10, M, W
Author
Country
symptoms be[ore admission
Physical findings and presenting symptoms
Cerebrospinal findings
3 months Ulcerative crusting skin lesions, 'acute illness, cough, fever, lymphadenopathy, membranous tonsils, papilledema, and hepatosplenomegaly At birth
3 weeks
"Xpersonal communication with the authors indicates that the
infection. Cases with pulmonary involvement are usually asymptomatic or m a y have a slight cough, scanty mueoid sputum, and infrequent hemoptysis. There is rarely fever, malaise, and weight loss. Clinical symptoms and physical signs become evident when meningitis supervenes. Fever, headache, vertigo, nausea, irritability, vomiting, stupor, confusion, lethargy, and convulsions are noted. Nuchal rigidity, positive Brudzinski's and Kernig's signs, as seen in other meningitides, appear. Later, increasing intracranial pressure develops with its associated signs of papilledema, ophthalmoplegia, and cranial nerve involvement. Fever is seldom above 101 ~ F., the leukocyte count is variable, and the erythrocyte sedimentation rate is usually normal. The spinal fluid is under increased pressure. It m a y be clear but is generally turbid, and, on rare occasions, x a n t h o chromic. The cell count is usually between 40 and 1,000 cells with an average of 200 to 300 per cubic millimetera; the cells are mostly lymphocytes, although at an early stage they m a y be polymorphonuelear ieuko-
Cyanosis, brachycardia, weak respiration, anasarca, hydrocephalus, and hepatosplenomegaly Headache, nausea and vomiting, 84 cells, 80% emaciation, lethargy and weaklymphocytes ness, bilateral papilledema and ~'Pressure nuchal rigidity, ankle clonus, and Babinski +
3 cases quoted had toxoplasmosis and the cryptococcosis was not
cytes. Total protein is increased and glucose and chlorides are slightly decreased. In the neonatal period, cryptococcosis presents itself with different symptoms than in older children. Cyanosis, convulsions, failure to thrive, jaundice, hepatosplenomegaly, chorioretinitis, skin rash, and punctate calcifications in the brain m a y be noted. Thus cryptococcal meningitis must be differentiated from other diseases, especially congenital toxoplasmosis and cytomegalic inclusion disease. 56-5s Cryptococcosis, or other fungous invaders of the central nervo~as system, should be considered in the differential diagnosis of meningitis or expanding intracranial lesions. This will be frequently suggested by pleocytosis of the cerebrospinal fluid, reduced glucose and chloride levels, and increase in protein and pressure. Specimens of fluid should be cultured for fungi on Sabouraud's and other media and India ink preparations should be examined. The pathogenicity of strains of C. neo[orraans is determined by Iaboratory methods such as those described by Benham. 12 The
Volume 59
Number 4
f
Araphotericin B in cryptococcus meningitis
58 7
Antimottern
pirect smear
o~ cryptococeus
Culture
diag- Duration nosis o[ illness No 10 days
No
positive from Positive from CSF CSF
Yes
Organs involved
Autopsy
Brain, skin, lymph Yes nodes, thyroid, tonsils, liver, spleen, kidney, adrenal, and eyes
20 minutes Brain, liver, and spleen
6 months Brain
Treatment Remarks Penicillin and Chest x-ray--normal sulfadiazinc
Lived for 20 minutes
Yes
_
Ethyl vanillate
Coexisting tuberculous meningitis Living with residual spasticity of left hand and wrist, and hyperkinetic behavior EEG--diffuse organic dysrhythmia
I etinitely proved.
characteristic features are f e r m e n t a t i o n of all sugars, e x c e p t lactose, good g r o w t h on most c u l t u r e media, a n d p a t h o g e n i c i t y to mice. Staining of the capsule with m u c i c a r mine a n d the a p p e a r a n c e in I n d i a ink p r e p a rations are p a t h o g n o m o n i c of this o r g a n ism. 14 T r e a t m e n t of cryptococcosis was a challenge until a m p h o t e r i c i n B was introduced. Previous t r e a t m e n t consisted of roentgen therapy,40 sulfonamides,S~, Sl diamidines,~2 iodides, 1~ penicillin, tetracycline, ethyl vanillate,49, s4 nystatln,S3 a n d c y c l o h e x i m i d e ? ~ T h e prognosis was p o o r a n d most p e d i a t r i c patients died. O u t of the g r o u p reviewed, only 5 survived, b u t with neurological sequelae in 3; 2 h a d no follow-up. DISCUSSION
T h e r e are three interesting features in our case: the association of tuberculosis a n d cryptococcosis; the failure to c u l t u r e the fungus despite the n u m e r o u s organisms seen; and the uneventful recovery with a m p h o t e r i cin B.
Fig. 5. Lung lesion still present 3 months later.
588
Emanuel
et al.
Fig. 6A. Lung lesion decreasing in size on antituberculosis therapy, 5 months later.
The diagnosis of pulmonary tuberculosis in the child was supported by the history of contact with the disease, the positive tuberculin test, and the resolution of the persisting pulmonary lesion during prolonged antituberculosis therapy. Additional evidence for the diagnosis was the location of the lung lesion. In cryptococcosis, the lesion is twice as common in the lower lobe as in the upper and middle lobes. In 50 per cent of reported cases, there is involvement of 2 or more lobes and in about one third there is diffuse involvement of both lungs26' 60-62 This is in contrast to our case, where the lesion was in the right middle lobe. The failure to recover tubercle bacilli on culture and animal inoculation could be attributed to the intensive antituberculous therapy instituted prior to bacteriologic examination. The failure to culture Cryptococcus despite the numerous organisms repeatedly seen on smear, may likewise be due to the intense antibiotic and amphotericin B therapy. On administration of the drug, the capsule of the fungus decreased very strikingly in size. The uneventfuI recovery from this usually fatal disease, we feel, is due to the very intense therapy with the antifungaI antibiotic amphotericin B.
October 1961
It is recommended that therapy with amphotericin B be started with 0.25 my. per kilogram daily and that the dose be gradually increased until an optimum level is attained; this is generally achieved with 1.0 mg. per kilogram. A dose exceeding 1.5 rag. per kilogram is cautioned against. We instituted therapy with a dose of 1.25 mg. per kilogram and maintained this dose despite the azotemia. There were rare occasions when symptoms of nausea, vomiting, and irritability were manifested. When the drug was administered every other day or 3 times weekly, the azotemia disappeared. During the last 3 weeks of hospitalization the dose was doubled to 2.5 mg. per kilogram, but was given only once a week. This did cause, once again, an elevation of the blood urea nitrogen but was otherwise well tolerated. The patient received a total of 490 mg. of the drug during a 12-week course. Liver function studies were within normal limits.
Fig. 6B. Lateral film showing regression of middle lobe lesion.
Volume 59 Number 4
Amphotericin B in cryptococcus meningitis
5 89
and tuberculosis manifesting m e n i n g e a l s y m p t o m s should be w a t c h e d for s u p e r i m posed c r y p t o c o c c a l infection. T h e a l m o s t 100 p e r cent m o r t a l i t y rate of the 23 cases reviewed before the use of a m p h o t e r i c i n B stresses the p a r a m o u n t role the d r u g plays in the m a n a g e m e n t a n d t r e a t m e n t of this fungal disease. ADDENDUM
Fig. 7. X-ray 7 months after patient was discharged from the hospital The chest x-ray revealed further resolution of the right middle lobe lesion. The patient is still being maintained on antituberculosis therapy as indicated in our paper.
A n o t h e r side effect of the d r u g is anemia. This m a y h a v e been the cause of the slight d r o p n o t e d in o u r p a t i e n t ' s h e m o g l o b i n level despite s u p p l e m e n t a l iron t h e r a p y , b u t this was only t r a n s i e n t and soon r e t u r n e d to its previous level. SUMMARY
A case of c r y p t o c o c c a l meningitis associated w i t h p u h n o n a r y tuberculosis is reported. T h e t r e a t m e n t of the disease with a m p h o tericin B is discussed; the drug was effective a n d well tolerated. A review of cryptococcosis in the p e d i a t r i c age group f r o m the world l i t e r a t u r e is presented a n d the differences in the clinical manifestations of the disease in the n e o n a t e and the o l d e r child are stressed. Evidence is presented for the occurrence of congenital c r y p t o c o c c a l meningitis. I n the p e d i a t r i c age group, patients with histoplasmosis, moniliasis, H o d g k i n ' s disease, leukemia, sarcoidosis,
Since this article was submitted for publication a paper has appeared in the British Medical fournaI (vol. 2, pp. 91-93, 1961) entitled "Cryptocoecal Meningo-Encephalitis," by W. F. Twining McMath and K. K. Hussain. This article deals with a case of cryptococcal meningoencephalitis in a 4-year-old boy. The child was treated with steroid therapy, 5 mg. doses of prednisolone, tetracycline, 250 mg. every 6 hours, amphotericin B, 0.5 mg. in 5 ml. of water intrathecally and 20 mg. in 250 ml. of 5 per cent dextrose by intravenous drip. He died 3 days following institution of therapy. We wish to thank Dr. H. S. Gordon and the pediatric staff, and the nursing staff, headed by Miss D. Melchior, at Mount Sinai Hospital, Chicago, Ill., for their help. REFERENCES
1. Zenker, F. A.: Encephalitis mit Pilzentwicklungem Gehlrn, Jahresb. d Gesellsch. f. nat.u. Heilk. in Dresd. 62: 51, 1861. 2. Biisse, O.: Ueber parasit~re Zelleinschliisse und ihre Ziichtung, Zentralbl. f. Bakt. 16: 175, 1894. 3. Buschke, A.: Ueber eine durch Coccidien hervorgerufene Krankheit des Menschen, Deutsche reed. Wchnschr. 21: t4, 1895. 4. Vuillemin, P.: Les Blastomycetes pathog&nes, Rev. G6n. de se. pures et Appliq., Paris 12: 732, 1901. 5. Kiitzing, F.: Algarum aqua dulcis germaniae Decas III (1833) (Cited by Benham, 1933). 6. Frothingham, L.: A Tumor-Like Lesion in the Lung of a Horse Caused by a Blastomyces (Torula), J. M. Res. 9: 31, 1902. 7. Von Hansemann, D.: Ueber eine bisher nlcht beobachtete Gehirnerkrankung durch Helen, Verhandl. d. deutsch, path. Gesellsch, f. Chir. 9: 21, 1905. 8. Stoddard, J. L., and Cutler, E. C.: Torula Infection in Man, Monograph of the Rockefeller Institute for Medical Research, New York, 1916, No. 6, p. 1. 9. Lodder, J.: I. Die Hefesammlung des centraal Bureau voor Schimmelcultures. II. Die Anaskosporogenen He fen. Verhand. Akademie
590
10. 11. 12. 13.
14. 15. 16. 17. 18.
19.
20. 21.
22. 23. 24. 25.
26. 27. 28.
EmanueI et al.
Wetenschappen Amsterdam, Afdeeling Natuurkunde, Series 2, 32: 1, 1934. Emmons, C. W.: The Significance of Saprophytism in the Epidemology of the Mycoses, Tr. New York Acad. Sc. 17: 157, 1954. Emmons, C. W.: Isolation of Cryptococcus neoformans From Soil, J. Bact. 62: 685, 1951. Benham, R. W.: Cryptococci---Their Identification by Morphology and by Serology, J. Infect. Dis. 57: 255, 1935. Sanfelice, F.: Contributo alla morfologia e biologia dei blastomiceti the si sviluppano nei suechi di alcuni frutti, Ann. d'Hig., Rome 4: 463, 1894. Littman, M. L., and Zimmerman, L. E.: Cryptococcosis (Torulosis), New York, 1956, Grune & Stratton, Inc. Freeman, W.: Torula Meningoencephalitis; Comparative Pathology in 19 Cases, Tr. Am. Neurol. A. 56: 203, 1930. Carton, C. A., and Mount, L. A.: Neurosurgical Aspect of Cryptococcosis, J. Neurosurg. 8: 143, 1951. Levin, E. A.: Torula Infection of the Central Nervous System, Arch. Int. Med. 59: 667, 1937. Voyles, G. Q., and Beck, E. M.: Systemic Infection Due to Torula Histolytica. Report of 4 Cases and Review of the Literature, Arch. Int. Med. 77: 504, 1946. Cox, L. B., and Tolhurst, J. C.: Human Torulosis. A Clinical Pathological and Microbiological Study With a Report of I3 Cases, Melbourne, 1946, Melbourne University Press. Fitchett, M. S., and Weidman, F.: Generalized Torulosis Associated With Hodgkin's Disease, Arch. Path. 18: 225, 1934. Zimmerman, L. E., and Rappaport, H.: Occurrence of Cryptococcosis in Patients With Malignant Disease of Reticuloendothelial System, Am. J. Clin. Path. 24: 1050, 1954. Smith, F. B., and Crawford, J. S.: Fatal Granulomatosis of the Central Nervous System Due to a Yeast, J. Path. & Bact. 33: 291, 1930. Cabot, R. C., editor: Case Records of the Massachusetts General Hospital, New England J. Med. 210: 1291, 1934. Hoff, C. L.: Immunity Studies of Cryptococcus hominis (Torula histolytica) in Mice, J. Lab. & Clin. Med. 27: 751, 1942. Boshes, L. D., Sherman, I. C., Hesser, C. J., Milzer, A., and Maclean, H.: Fungus Infection of the Central Nervous System; Experience in Treatment of Cryptococcosis With Cycloheximide (Actidione), A. M. A. Arch. Neurol. & Psychiat. 75: 175, 1956. Johns, F. M., and Attaway, C. L.: Torula Meningitis. Report of a Case and Summary of Literature, Am. J. Clin. Path. 3: 45, 1933. Cohen, M.: Binocular Papilledema in a Case of Torulosis Associated With Hodgkin's Disease, Arch. Ophth. 32: 477, 1944. Rodger, R. C., Terry, L. L., and Binford, C. H.: Histoplasmosis, Cryptococcosis and Tuberculosis Complicating Hodgkin's Disease. Report of a Case, Am. J. Clin. Path. 21: 153, 1951.
October 1961
29. Barlow, D. L.: Primary Blastomycotic Meningitis Occurring in Children, M. J. Australia 2: 302, 1923. 30. Carton, C., and Mount, L.: Neurological Aspects of Cryptococcosis, J. Neurol. 8: 143, 1951. 31. Reves, D. L., Butt, E. M., and Hammack, R. N.: Torula Infection of Lungs and Central Nervous System, Arch. Int. Med. 68: 57, 1941. 32. Longmire, W. P., and Goodwin, T. C.: Generalized Torula Infection, Case Report With Review and Observation on Pathogenesis, Bull. Johns Hopkins Hosp. 64: 22, 1939. 33. D'Aunoy, R., and Lafferty, C. R.: Torula Meningitis in a Child, Am. J. Clin. Path. 9: 236, 1939. 34. Marshall, M., and Teed, R. W.: Torula Histolytica Meningoencephalitis. Recovery Following Bilateral Mastoidectomy and Sulfonamide Therapy; Preliminary Report; J. A. M. A. 120: 527, 1942. 35. Dormer, B. A., Friedlander, J., Wiles, F. J., and Simpson, F. W.: Tumor of Lungs Due to Cryptococcus histolyticus, J. Thoracic Surg. 14: 322, 1945. 36. Hamilton, L. C., and Thompson, P. E.: Treatment of Meningitis (Due to Cryptococcus neoformans) With Penicillin, Am. J. Dis. Child. 72: 334, 1946. 37. Debre, R., and others: Development of Meningitis Due to Torula histolytlca in Child 12 Years Old With Malignant Lymphogranulomatosis, Bull. Acad. de m$d., Paris, 130: 443, 1946. 38. Cox, L. B., and Tolhurst, J. C.: Human Torulosis. A Clinical Pathological and Microbiological Study With a Report of 13 Cases, Melbourne, 1946, Belbourne University Press. 39. Mider, G. B., Smith, F. D., and Bray, W. E., Jr.: Systemic Infection With Cryptoeoecus neoformans and Histoplasma capsulation in Same Patient, Arch. Path. 43: 102, 1947. 40. Greening, R. R., and MenviIle, L. G.: Roentgen Findings in Torulosis. Report of 4 Cases, Radiology 48: 381, 1947. 41. Cloward, R. B.: Torula Meningitis. First Case to be Reported in Hawaii, Hawaii M. J. 7: 377, 1948. 42. Neuhauser, E. B. D., and Tucker, A.: The Roentgen Changes Produced by Diffuse Torulosis in the Newborn, Am. J. Roentgen. 59: 805, 1948. 43. Spicer, C., Hiatt, W. O., and Kessel, J. F.: Candida albieans and Cryptococcus neoformans Occurring as Infective Agents in an 8-Year-Old Boy, J. PEDIAT. 33: 761, 1948. 44. Nassau, E., and Weinberg-Heiruti, C.: Torulosis of the Newborn, Harefuah 35: 50, 1948. 45. Health, P.: Massive Separation of Retina in Full Term Infants and Juveni!es, J. A. M. A. 144: 1148, 1950. 46. Lepau, H., Rubinstein, L., Cohn, F., and Shandra, J.: A Case of Cryptococcus neoformans Meningoencephalitis Complicating Boeek's Sarcoid, Pediatrics 19: 377, 1957. 47. Soysal, S. S., Unat, E. K., and Tahslnglu:
Volume 59 Number 4
48.
49. 50.
51.
52.
53. 54.
55.
Amphotericin B in cryptococcus meningitis
Un cas de cryptococcus, Arch. fran~, p~diat. 11: 246, 1954. Oliviera Campos, J.: Congenital Meningoencephalitis Due to Torulosis neoformans. Preliminary Report, Bol. clin. dos Hopit. Civis., Lisbon 18: 609, 1954. Nanda, S., Kass, I., Cohn, M., and Dressier, S.: Coexistence of Tuberculosis and Cryptococcal Meningitis, Pediatrics 20: 45, 1957. Benham, R. W.: The Genus Cryptococcus. The Present Status and Criteria for Identification of Species, Tr. New York Acad. Sc. 17: 418, 1955. Fisher, A. M.: The Clinical Picture Associated With Infections Due to Cryptococcus neoformans (ToruIa histolytica); Report of 3 Cases With Some Experimental Studies, Bull. Johns Hopkins Hosp. 86: 383, 1950. Whitehill, M. R., and Rawson, A. J.: Treatment of Generalized Cryptococcosls With 2Hydroxystilbamidine, Virginia M. Month. 81: 591, 1954. Hall, B. D., and Mardis, R. E.: Treatment of Cryptococcosis With Terramycin, U.S. Armed Forces M. J. 4: 1061, 1953. Christie, A., Middleton, J. G., Peterson, J. C., and McVickar, D. L.: Treatment of Disseminated Histoplasmosis With Ethyl Vanillate, Pediatrics 7: 7, 1951. Wilson, H. M., and Duryea, A. W.: Cryptococcus Meningitis (Torulosis) Treated With a New Antibiotic, Actidione, A.M.A. Arch.
59 1
Neurol. & Psychiat. 66: 470, 1951. 56. Weller, T. H., Maculey, J. C., Craig, J. M., and Wirth, P.: Isolation of Intranuclear Inclusion Producing Agents From Infants With Illness Resembling Cytomegalic Inclusion Disease, Proc. Soc. Exper. Biol. & Med. 94: 4, 1957. 57. Guyton, T. B., Ehrlich, F., Blanc, W. A., and Becker, M. H.: New Observation in Generalized Cytomegalic Inclusion Disease of the Newborn, New England J. Med. 257: 803, 1957. 58. Sabin, A. B., and Feldman, H. A.: Chorioretinopathy Associated With Other Incidence of Cerebral Damage in Childhood Syndrome of Unknown Etiology Separable From Congenital Toxoplasmosis, J. PEDIAT. 55: 296, 1949. 59. Bomati, J., Rogers, J. V., and Hopkins, W. A.: Pulmonary Cryptococcosis, Radiology 66: 188, 1956. 60. Berk, M., and Gerstl, B.: Torulosis Producing a Solitary Pulmonary Lesion; Report of a Four Year Case With Lobectomy, J. A. M. A. 149: 1310, 1952. 61. Evans, E. E., and Harrell, E. R.: Cryptococcosis: A Review of Recent Cases, Univ. Michigan, M. Bull. 18: 43, 1952. 62. Ratcliffe, H. E., and Cook, W. R.: Cryptococcosis: Review of the Literature and Report of a Case With Initial Puhnonary Findings, U.S. Armed Forces M. J. 1: 957, 1950.
577
Cryptococcus meningitis in treated Mtb amplootericin B, vitb a review of the pediatric literature B. Emanuel, M.D., ~ E. Ching, M.D., A. D. Lieberman, M.D., and M. Goldin, M.S. CHICAGO~
ILL.
also known a s torulosis or European blastomycosis, is a mycotic disease of m a n and animals caused by Cryptococcus neoformans (Torula histoIytica or Cryptococcus hom{nis). T h e first case reported was by Zenker 1 in 1861 in a m a n dying from a fungous infection involving the central nervous system, and it is most probable that the organism was C. neoformans. Biisse 2 and Buschke S independently recovered yeastlike organisms f r o m a w o m a n with bone lesions who died from generalized involvement. Tile organisms w e r e referred to as Saccharomyces neoformans. Vuillemin 4 recognized the lack of ascospores, thus differentiating it from true yeast, and called it C. homlnls. T h e generic term Cryptococcus was used or given by KiltC R Y P T O C O C C O S I S ~
From the Departments o[ Pediatrics and Microbiology, Chicago Medical School, and Mount Sinai Hospital, Chicago, Ill. e'Address, Department o[ Ped{atr{cs, Mount S{nai Hospital, Cali[ornla Avenue at 15th Street, Chicago 8, Ill.
zing2 I n 1902, Frothingham G recovered the organism from a pulmonary lesion in a horse, and Von H a n s e m a n n 7 in 1905 recovered the organism for the first time from a m a n dying of meningitis. I n 1916, Stoddard and Cutler s recorded the clinical and pathologic features of the disease, described the morphologic and cultural characteristics of C. neoformans, and proved it to be a true yeast, reproduced by budding only. Because it fails to produce 'mycelium or ascospores, it is now classified with the anascosporogenous yeasts. I n Lodder's '~ classification Cryptococcus has 25 species, all saprophytic except C. neoformans. Saprophytic strains are Widespread in nature, 1~ and are found in soil, 11 food, and the skin and gastrointestinal tract of m a n ~2 and animals. 1~ Pathogenic strains have been recovered from peachesff 3 milk, and from the oropharynx, gastrointestinal and vaginal tracts of apparently healthy carriers? 4 Some relation seems to exist to pigeon manure. 10 T h e yeasts are thought to enter the body
5 78
Eraanuel et al.
F i g . 1. R i g h t m i t t i n g film.
middle
lobe i n f i l t r a t e s e e n o n a d -
through the respiratory tract, which explains the frequency of lung involvement, 14 although the tonsils and skin are considered the portal of entry by Freeman? 5 Cryptococcosis is world wide in distribution but the largest number of cases has been reported in the United States, where approximately 450 cases have been recorded in adults. The actual incidence of the disease cannot be estimated accurately by the number of published cases. Alteration of the host-parasite relationship, disturbance in the reticuloendothelial system, and debilitating disease contribute to the lowering of resistance to the organisms. Coexistence of cryptococcosis with Hodgkin's disease, 2~ leukemia, reticulum cell sarcoma,2~, 27 histoplasmosis,2S tuberculosis,2S moniliasis, 2~ and diabetes 2~ have been previously described. The organism most likely reaches the central nervous system by way of the blood stream, 16 producing 3 varied types of pathologic pictures: (1) meningitis, where the subarachnoid space of the base of the brain is most frequently involved; (2) meningoencephalitis, where the gray matter is mostly
October 1961
affected with a honeycomb appearance of the cortex, basal ganglia, brain stem, thalamus, or cerebellum; and (3) cryptococcal granuloma, which is frequently found in the cerebellum and cerebrum. Other organl~ such as the lung, liver, spleen, skin, and lymph nodes are less frequently involved. 14 In 1937 Levin ~7 reviewed the literature and since then numerous other reviews have been published,14, 18, 19 but none in the pediatric literature. The prognosis, except for the localized, cutaneous type, is grave, especially when the central nervous system is involved. Until the advent of amphotericin B, ~ these cases were nearly always fatal. We have recently encountered in a child a case of C. neoformans meningitis associated with tuberculosis of the lung. To our knowledge, this is the first child with cryptocoecal meningitis to have apparently recovered completely when treated with amphotericin B. Certain aspects of this case will be discussed and the review of the pediatric literature on cryptococeal meningitis is included. CASE
REPORT
G. H.,t an 18-month-old Negro boy, was brought in a comatose condition to the emergency room of the Mount Sinai Hospital, Chicago, on Aug. 21, 1960, with tonic and clonic convulsions and a temperature of 104 ~ F. For about one month prior to admission, the child had had frequent colds, a cough, and fever but improved when given penicillin by a local physician. Three days prior to admission, the child again developed a dry cough, rhinorrhea, and fever. On the day of admission, shortness of breath was also noted. In the emergency room, the child was comatose; the pupils were equal, dilated, and unresponsive to light. There was a slight ptosis of the left eyelid, the neck was supple,
"X'The trade-mark of E. R, Squibb & Sons for amphoterlcln B is Fungizone. tFrom the service of Dr. H. S. Go/don.
Volume 59 Number 4
Amphotericin B in cryptococcus meningitis
and Kernig's, Brudzinski's, and Babinski's signs could not be elicited. The throat was slightly reddened, the ears clear, and no significant Iymphadenopathy could be found. The breath sounds were harsh, but with no r~les or dullness to percussion. The heart was normal, but there was a tachycardia. The abdomen was soft, and no organs or masses could be felt. Phenobarbital, intramuscularly, and aspirin suppositories were given, but convulsions continued for another half hour. A roentgenogram of the chest was immediately taken and a moderate pneumonia of the right middle lobe of the Iung was visualized (Fig. 1). The fundi showed no papilledema, and a lumbar puncture was performed. The pressure was slightly elevated, and the clear fluid obtained included 217 cells per cubic millimeter, predominantly neutrop.hils. T h e protein was elevated, and the P a n @ test was positive. Glucose and chloride concentrations were normal. Organisms resembling Cryptococcus were seen in this specimen, but, unfortunately, no cultures were made on it. Examination of the blood showed a hemoglobin of 8.1 Gm. per 100 ml., hematocrit 28, red blood ceils 3.75 million per cubic millimeter, and color index 0.69. T h e leukocyte count was 8,100 per cubic millimeter with 3 per cent bands, 55 per cent neutrophils, 34 per cent tymphocytes, 5 per cent eosinophils, 2 per cent monocytes, and 1 per cent basophils. The sedimentation rate was 30 mm. per hour. '* The blood urea nitrogen was 18.5 rag. per cent. The child was given 1,000,000 units of penicillin, intravenously, twice a day; 250 mg. sulfadiazine, intravenously, every 6 hours; and 50 rag. per kilogram chloramphenicol, intramuscularly, every 6 hours. On the second hospital day, his neck become slightly rigid. A Mantoux test (t:10,000 OT.) was markedly positive after 24 hours. The child was then immediately placed on
*Wintrobe method.
579
para-amin0salicylic acid, 750 rag., 3 times a day; isoniazid, 100 mg., 3 times a day; streptomycin, 50 rag., intramuscularly, twice a day; and prednisone, 10 mg., twice a day. One the third hospital day, the patient was alert and free of convulsions. The lumbar puncture was repeated, the cell count was 207 per cubic millimeter; 90 per cent of them, however, were lymphocytes in this specimen. India ink preparations showed numerous encapsulated ceils morphologically typical of C. neoformans. A direct count of the organisms showed them to be greater than 10,000 per cubic millimeter. A diagnosis of cryptococcal meningitis was m a d e and amphotericin B, 15 mg. given intravenously in 500 ml. of dextrose in water with addition of 0.5 ml. heparin as a precaution against thrombophlebitis, was added to the therapeutic regimen. Potassium iodide was also given, starting at 3 drops twice a day and increased by 1 drop per day until a dose of 12 drops twice a day was reached. This was stopped on the sixty-second day of hospitalization when the lung lesion was felt to be a tuberculous rather than a cryptococcal granuloma. T h e history from the child's parents revealed that the patient was in close contact with an uncle who had been treated for tuberculosis since February, 1960. It was also learned that the child had been playing around pigeon excreta. The course of the disease and the treatment are shown in Fig. 2. The prednisone, chloramphenicol, and penicillin were discontinued after the third hospital day. The amphotericin B was given every other day or 3 times weekly when the blood urea nitrogen became abnormally elevated. This dosage was found to be best. During the last 2 weeks of therapy, amphotericin B was given once a week in a dose of 30 mg. Despite intensive drug therapy, liver function tests remained normal, and the drug was well tolerated. Throughout the long hospital course, every effort was made to isolate the tubercle bacillus from gastric washings, spinal fluids, and bronchial aspirations. All smears, cultures, and guinea pig inoculations were negative for acid-fast bacilli. Skin and serologic tests
5S..1
ioi ~
,io~"
la3"
I
I L
CPSC'SC"
I
\
\
1'
14
!
IAMPHOTEmC.,,ml
+
CHLORIDE
I
]
21
~lLl:&rll AZlN E
~J
PSC"
"lk.
'%
S'FREPTOMV ~iN
I f'
C" SO"
\~r \,~
\,o
I
,
.
58
THERAPY
§ ]
l
I--
42
49
[] [] []
PSC'
[]
88
[]
"
.
__-----------
.............
!
o
CPSC"
o
o
?0
l i l t -~= . . . . . . . . .
,
CHLORIDI~8 PROTEIN SUGAR CELLS
PROTEIN
C P S C'
-'---II. . . . . . . . . . . . . .
rNH
[] [] []
___
........
,
Fig. 2. Clinical course, therapy, and laboratory findings.
28
PAS
[] [] []
SPINAL TAPS
CELLS
. . . . . . . . . . . . .
:
BLOOD UREA NITROGEN
TEI~PERATURE
[]
CPSC"
77
[]
ILL.-'"
L
."
| ...............
.'
,
114
[]
I~0
P..PIr
Ill
r
P I
|10 9
r
0
BOO
Sl O00
I it] -,,o
1,
{000
lEO0
cr)
(3
0
CO C~
r
Volume 59 Number 4
Amphotericin B in cryptococcus meningitis
for blastomycosis, coccidioidomycosis, and histoplasmosis were all negative. The cryptococci were seen in large numbers in the first 5 specimens of spinal fluid, but none in the succeeding 4 specimens. The number of organisms, the size of the capsule, and the amount of budding diminished strikingly with each succeeding specimen. Every effort to culture the organism, however, failed. All animal inoculations were also negative. I t is probable that the intensive therapy with the antibiotics and amphotericin B were responsible for the negative cultures. Ordinarily, this organism grows with ease on ordinary laboratory media, either at room or incubator temperature.l~, 14 T h e child progressively improved during his hospitalization, although the lung lesion did not diminish in size (Figs. 3, 4, and 5). The child was discharged from the hospital after the spinal fluid findings returned to normal on his eighty-seventh hospital day. He was continued, however, on antituberculosis therapy. Five months after discharge, the child has remained in good health, is gaining weight, and is mentally normal, with a normal electroencephalogram. The pulmonary lesion has decreased in size on the continued antituberculosis therapy (Figs. 6A and 6B). REVIEW
OF THE
58 1
liver in 8, the spleen in 7, the kidney in 5, the eyes in 4, the skin in 3, the bones, adrenals, and thyroid in 2, and the pancreas, heart, and lymph nodes in 1. In the pediatric age group, cryptococcosis is also frequently associated with other diseases such as histoplasmosis, a9 moniliasis, 4a Hodgkin's disease, 37 sarcoidosis, ~6 and tuberculosis. 49 Cryptococcosis is a subacute or chronic
Fig. 3. Persisting lung lesion, 1 month later.
LITERATURE
T o date, including the report of the prcsent case, we have been able to find only 23 cases of cryptococcus meningitis in children less than 15 years of age. Table I summarizes the significant data on these cases. The ages of the patients ranged from 20 minutes post partum to 15 years of age. The presence of the disease in a 20-minute-old newborn ~s is definite evidence of the existence of a congenital cryptococcal infection. Of the 23 cases, 3 definite cases and 3 equivocal cases appeared in the neonatal period. The sex distribution, as in the adults, favors the males, although such a distribution is difficult to explain. The disease is not limited to the white race; 5 of the patients were Negroes. The brain and the meninges were involved in 23 cases, the lungs in 9, the
Fig. 4. Persistance of lung lesion, 2 months later,
58 2
E m a n u e l et al.
October 1961
T a b l e I. R e v i e w of tile w o r l d p e d i a t r i c l i t e r a t u r e
Duration
of
A g e , sex, race
symptoms be[ore Cerebrospinal Physical findings and admission presenting symptoms findings 4 weeks Diarrhea, irritability, drowsiness, No definite number and signs of meningeal irritacells, all lymphocytes tion 1'Pressure
Author Barlow 2~
Country Year Australia 1923
Carton and Mount 30
United States
1933
12, F, W
6 weeks
Reeves, Butt, and Hammack al
India
1938
15, F, W
9 months Headache, vomiting, stiff neck, 97 cells, mostly polymorphonublurred vision, cough, fever, clear leukocytes, emaciation, and optic atrophy lymphocytes later "]'Pressure at first, normal later Protein1'
Longmire and Goodwin a2
United States
1939
4, F, W
3 months Fever, dyspnea, convulsions, stu- 100 to 400 cells, por, deafness and blindness, polymorphonuemaciation, cyanosis, stiff neck, clear leukocytes and papilledema 75, lymphocytes 25 "]'Pressure Protein~" Glucose 35
D'Aunoy and Lafferty sa
United States
1939
7, M, N
Sudden
Stiff neck, semicoma, and acute 100 to 250 ceils illness ~'Pressure
Marshall and Teed 3~
United States
1942
9, F, W
6 weeks
Fever, headache, nausea, irritabil- 8 to 15 Cells ity, vomiting, much rigidity, 1"Pressure Kcrnig +, papilledema, and retinal hemorrhage
Dormer, et al. 3~ South Africa
1945
12, M, N
Hamilton and United Thompson aG States
1946
6, M, N
2 weeks
Debre, et a l Y
1946
12, M, W
Unknown
France
3, F, W
Headache, vomiting, poor vision, hyporeflexia, Babinski and Kernig +, left ptosis, sixth nerve palsy, papilledema, retinal hemorrhage and exudation, coma, and death
88 cells, 90% lymphocytes 1'Pressure Protein 100 Glucose 40
4 months Cough, headaches, anorexia, Many polymorphoweight loss, clubbing of fingers, nuclear leukocytes fever, and dullness in right upper chest
Malaise, anorexia, fever, head- 320 cells, mostly ache, vomiting, generalized conpolymorphonuvulsion, papilledema, stiff neck, clear Ieukocytes Brudzinski +, and hyporeflexia ~'Pressure Protein 180 Glucose ) I0
Headache, vomiting, fever, con- Not done vulsions, photophobia, opisthotonos, papilledema, hepatosplenomegaly, ulcer on neck, and mass over clavicle
Volume 59
Number 4
A m p h o t e r i c i n B in cryptococcus meningitis
5 83
Antimot-
Direct smear
tern diagnosis Yes
Duration of illness Organs involved 3 months Brain
Autopsy Treatment Yes None
Yes
5 weeks
Brain
No
Positive chest abscess aspiration
Yes
2 years
Brain
_
Positive from CSF
Positive from CSF
Yes
3 months Brain, meninges, lung, thyroid, liver spleen, and kidney
Positive from CSF
Positive from CSF
No
48 hours
Positive from CSF
Positive from CSF
Yes
5 months Brain
Sulfadiazine
Living, well, subnormal intelligence 4 years later
Positive from CSF
Positive in guinea pig
Yes
5 months Lung and brain
Sulfadiazine, KI
Postoperative meningitis following right upper pulmonary lobectomy Patient survived, no follow-up
Positive from CSF Positive from sputum
Positive from cisternal puncture; positive from sputum
Yes
Sulfadiazine
Chest x-ray--nonspecific lung infiltration Pneumoencephalogram--enlargement of one ventricle and other not visualized
Positive from CSF
Yes
KI
Coexisting Hodgkin's disease
of cryptocoeeus -Positive from CSF
Culture
Positive from CSF
Positive from CSF
Positive from CSF and chest abscess
aspiration
72 days
2 weeks
Brain
Skull x-ray showed signs of increased intracranial pressure
Sulfadiazine Skull x-ray--inTorula creased marking antigen, K I Chest x-ray--interlobar empyema CSF still positive 2 years later Reported to be well 9 years later, but with sequelae
Yes
Yes
Lungs
Skin, lungs, heart, spleen, liver, and brain
K I orally, NaI intravenously, 5 % NaI, and acriflavine intrathecally
Remarks Optic atrophy prior to death
Yes
584
E m a n u e l et al.
October 1961
Table I. Cont'd Duration
of Country
Year
Age, sex, race
symptoms before admission
Cox and Tolhurst ss
Australia
1946
7, M, W
5 weeks
Mider, Smith, and Bray a9
United States
1947
12, M, N
Greening and Menville 40
United States
1947
6, M, N
2 weeks
Upper respiratory infection, head- 300 cells, lymphoache, vomiting, convulsion, and cytes 30% stiff neck ]'Pressure ++Pandy Protein]` Glucose, normal
Cloward ~1
Hawaii
1948
51,/.~, M, Chinese
1 week
Septic temperature, headache, ir- 450 cells, lympho-. ritability, convulsions, paralysis, cytes 33 % retinal hemorrhages, and papiI- ?Pressure ledema Protein 114 to 140
Neuhauser and United Tucker ~42 States
1948
7 weeks, M, W
7 weeks
Vomiting, twitching, rigidity, hy- 27 to 36 cells, 75% drocephalus, cataract and cholymphocytes rioretinitis, ankle clonus, and Protein 1,400 Babinski + Glucose 69
Neuhauser and United Tucker ~ 2 States
1948
19 days, M, W
19 days
Jaundice since birth, hepatosplenomegaly, dark urine and clay stool, hydrocephalus, and malnourishment
Neuhauser and United Tucker *.42 States
1948
17 days, M, W
4 days
Irritability, convulsions, hypertonieity, frequent clonic motions of extremities, hepatosplenomegaly and chorioretinitis
Spicer, Hiatt, United and Kessel~3 States
1948
4 years
Headache and lethargy, repeated Cloudy episodes of pulmonary infiltra- "]'Pressure tion with chronic cough, and septic temperature
Nassau and WeinbergHeiruti 44
Israel
1948
12 days, M, W
5 days
Cyanosis and generalized convul- 5,000, later 263 sion, no nuchal rigidity, hypocells reflexia, Kernig +, splenomeg- Protein 238 to 240 aly, skin macular and papular Glucose 14 my. lesions, and hydrocephalus
Health 4~
United States
I950
27 days, IV[, W
Lepau, et al. ~6 United States
1953
10, F, N
Author
8, M, W
Physical findings and presenting symptoms
Cerebrospinal findings
Headache, vomiting, leg pain, 41 to 50 cells, 40 to semicoma, active deep reflex, 46% lymphoeytes paralysis of right leg and arm, ]`Pressure stiff neck, and papilledema Protein]"
3 months Weakness, weight loss, anorexia, fever, and red swollen sternoclavicular region which drained, generalized lymphadenopathy
Endophthalmitls with separation of retina
massive
_
3 months Anorexia, weakness and general- 2,720 cells, 95% ized lymphadenopathy, later polymorphonuheadache, fever, vomiting, clear leukocytes, coma, and death later 16,000 cells Protein 70 to 200 o GlUcose 10 to 20 C1 110 to 121
Volume 59
Number 4
Amphotericin B in cryptococcus meningitis
5 85
AntimOT-
Direct smear
of cryptoeoeeus
Culture
Positive from CSF
Positive from CSF
Positive from blood and bone marrow
Positive from CSF
_
Duration of illness
Yes
289
Au-
Organs involved
topsy
Treatment
Remarks
Lungs and brain
Yes
_
Chest x-ray--fibrosis and small nodules
Brain, liver, kidney, and bones
Yes
months
No
11 days
Yes
Positive from CSF
Yes
28 days
No
23 days
Associated with generalized histoplasmosis
No
KI, sulfadiazinc, and penicillin intrathecally
Died
Brain
Yes
Penicillin, sulfadiazine
Pneumoencephalogram performed Exploratory trephination for brain abscess-negative
Brain, eyes, and lungs
Yes
Skull x-ray---calcification of frontal region Punctate and calcification along ventricles
2 months Brain
Positive from CSF
_
Positive from CSF
tern diagnosis
Positive postmortem from CSF
No
4 days
Spleen, liver, brain, and bone
Yes
Skull x - r a y - - p u n c t a t e calcification of the brain
Positive postmortem from CSF
No
10 days
Brain, liver, spleen, kidney, lungs, and eyes
Yes
Skull x-ray calcifications of cortex and brain substance
Positive from CSF and urine
No
35 days
Brain, lungs, kidney, spleen, pancreas, adrenal, and liver
Yes
Sulfadiazine
Positive from CSF after death
No
Brain and skin
Yes
Penicillin, sulfadiazinc
Positive from CSF
No
27 days
Many organs including eyes and brain
Yes
Positive fl'om CSF, nose and throat
Yes
61 days
Brain
Yes
6 weeks
_
Associated with generalized candidiasis
Congenital origin Combined lesion with toxoplasmosis
Polymyxin B, Coexisting Boeck's intramussarco{d cularly, and nystatin intrathecally
586
October 1961
E m a n u e l et al.
T a b l e I. Cont'd Duration
of Year
.Age~ sex~ race
Soysal, Unat, Turkey and Tahsinglu 47
1954
7, M, W
Oliviera Campos 4s
Portugal
1955 32 weeks, premature, F, W
Nanda, et al. ~9 United States
1956 10, M, W
Author
Country
symptoms be[ore admission
Physical findings and presenting symptoms
Cerebrospinal findings
3 months Ulcerative crusting skin lesions, 'acute illness, cough, fever, lymphadenopathy, membranous tonsils, papilledema, and hepatosplenomegaly At birth
3 weeks
"Xpersonal communication with the authors indicates that the
infection. Cases with pulmonary involvement are usually asymptomatic or m a y have a slight cough, scanty mueoid sputum, and infrequent hemoptysis. There is rarely fever, malaise, and weight loss. Clinical symptoms and physical signs become evident when meningitis supervenes. Fever, headache, vertigo, nausea, irritability, vomiting, stupor, confusion, lethargy, and convulsions are noted. Nuchal rigidity, positive Brudzinski's and Kernig's signs, as seen in other meningitides, appear. Later, increasing intracranial pressure develops with its associated signs of papilledema, ophthalmoplegia, and cranial nerve involvement. Fever is seldom above 101 ~ F., the leukocyte count is variable, and the erythrocyte sedimentation rate is usually normal. The spinal fluid is under increased pressure. It m a y be clear but is generally turbid, and, on rare occasions, x a n t h o chromic. The cell count is usually between 40 and 1,000 cells with an average of 200 to 300 per cubic millimetera; the cells are mostly lymphocytes, although at an early stage they m a y be polymorphonuelear ieuko-
Cyanosis, brachycardia, weak respiration, anasarca, hydrocephalus, and hepatosplenomegaly Headache, nausea and vomiting, 84 cells, 80% emaciation, lethargy and weaklymphocytes ness, bilateral papilledema and ~'Pressure nuchal rigidity, ankle clonus, and Babinski +
3 cases quoted had toxoplasmosis and the cryptococcosis was not
cytes. Total protein is increased and glucose and chlorides are slightly decreased. In the neonatal period, cryptococcosis presents itself with different symptoms than in older children. Cyanosis, convulsions, failure to thrive, jaundice, hepatosplenomegaly, chorioretinitis, skin rash, and punctate calcifications in the brain m a y be noted. Thus cryptococcal meningitis must be differentiated from other diseases, especially congenital toxoplasmosis and cytomegalic inclusion disease. 56-5s Cryptococcosis, or other fungous invaders of the central nervo~as system, should be considered in the differential diagnosis of meningitis or expanding intracranial lesions. This will be frequently suggested by pleocytosis of the cerebrospinal fluid, reduced glucose and chloride levels, and increase in protein and pressure. Specimens of fluid should be cultured for fungi on Sabouraud's and other media and India ink preparations should be examined. The pathogenicity of strains of C. neo[orraans is determined by Iaboratory methods such as those described by Benham. 12 The
Volume 59
Number 4
f
Araphotericin B in cryptococcus meningitis
58 7
Antimottern
pirect smear
o~ cryptococeus
Culture
diag- Duration nosis o[ illness No 10 days
No
positive from Positive from CSF CSF
Yes
Organs involved
Autopsy
Brain, skin, lymph Yes nodes, thyroid, tonsils, liver, spleen, kidney, adrenal, and eyes
20 minutes Brain, liver, and spleen
6 months Brain
Treatment Remarks Penicillin and Chest x-ray--normal sulfadiazinc
Lived for 20 minutes
Yes
_
Ethyl vanillate
Coexisting tuberculous meningitis Living with residual spasticity of left hand and wrist, and hyperkinetic behavior EEG--diffuse organic dysrhythmia
I etinitely proved.
characteristic features are f e r m e n t a t i o n of all sugars, e x c e p t lactose, good g r o w t h on most c u l t u r e media, a n d p a t h o g e n i c i t y to mice. Staining of the capsule with m u c i c a r mine a n d the a p p e a r a n c e in I n d i a ink p r e p a rations are p a t h o g n o m o n i c of this o r g a n ism. 14 T r e a t m e n t of cryptococcosis was a challenge until a m p h o t e r i c i n B was introduced. Previous t r e a t m e n t consisted of roentgen therapy,40 sulfonamides,S~, Sl diamidines,~2 iodides, 1~ penicillin, tetracycline, ethyl vanillate,49, s4 nystatln,S3 a n d c y c l o h e x i m i d e ? ~ T h e prognosis was p o o r a n d most p e d i a t r i c patients died. O u t of the g r o u p reviewed, only 5 survived, b u t with neurological sequelae in 3; 2 h a d no follow-up. DISCUSSION
T h e r e are three interesting features in our case: the association of tuberculosis a n d cryptococcosis; the failure to c u l t u r e the fungus despite the n u m e r o u s organisms seen; and the uneventful recovery with a m p h o t e r i cin B.
Fig. 5. Lung lesion still present 3 months later.
588
Emanuel
et al.
Fig. 6A. Lung lesion decreasing in size on antituberculosis therapy, 5 months later.
The diagnosis of pulmonary tuberculosis in the child was supported by the history of contact with the disease, the positive tuberculin test, and the resolution of the persisting pulmonary lesion during prolonged antituberculosis therapy. Additional evidence for the diagnosis was the location of the lung lesion. In cryptococcosis, the lesion is twice as common in the lower lobe as in the upper and middle lobes. In 50 per cent of reported cases, there is involvement of 2 or more lobes and in about one third there is diffuse involvement of both lungs26' 60-62 This is in contrast to our case, where the lesion was in the right middle lobe. The failure to recover tubercle bacilli on culture and animal inoculation could be attributed to the intensive antituberculous therapy instituted prior to bacteriologic examination. The failure to culture Cryptococcus despite the numerous organisms repeatedly seen on smear, may likewise be due to the intense antibiotic and amphotericin B therapy. On administration of the drug, the capsule of the fungus decreased very strikingly in size. The uneventfuI recovery from this usually fatal disease, we feel, is due to the very intense therapy with the antifungaI antibiotic amphotericin B.
October 1961
It is recommended that therapy with amphotericin B be started with 0.25 my. per kilogram daily and that the dose be gradually increased until an optimum level is attained; this is generally achieved with 1.0 mg. per kilogram. A dose exceeding 1.5 rag. per kilogram is cautioned against. We instituted therapy with a dose of 1.25 mg. per kilogram and maintained this dose despite the azotemia. There were rare occasions when symptoms of nausea, vomiting, and irritability were manifested. When the drug was administered every other day or 3 times weekly, the azotemia disappeared. During the last 3 weeks of hospitalization the dose was doubled to 2.5 mg. per kilogram, but was given only once a week. This did cause, once again, an elevation of the blood urea nitrogen but was otherwise well tolerated. The patient received a total of 490 mg. of the drug during a 12-week course. Liver function studies were within normal limits.
Fig. 6B. Lateral film showing regression of middle lobe lesion.
Volume 59 Number 4
Amphotericin B in cryptococcus meningitis
5 89
and tuberculosis manifesting m e n i n g e a l s y m p t o m s should be w a t c h e d for s u p e r i m posed c r y p t o c o c c a l infection. T h e a l m o s t 100 p e r cent m o r t a l i t y rate of the 23 cases reviewed before the use of a m p h o t e r i c i n B stresses the p a r a m o u n t role the d r u g plays in the m a n a g e m e n t a n d t r e a t m e n t of this fungal disease. ADDENDUM
Fig. 7. X-ray 7 months after patient was discharged from the hospital The chest x-ray revealed further resolution of the right middle lobe lesion. The patient is still being maintained on antituberculosis therapy as indicated in our paper.
A n o t h e r side effect of the d r u g is anemia. This m a y h a v e been the cause of the slight d r o p n o t e d in o u r p a t i e n t ' s h e m o g l o b i n level despite s u p p l e m e n t a l iron t h e r a p y , b u t this was only t r a n s i e n t and soon r e t u r n e d to its previous level. SUMMARY
A case of c r y p t o c o c c a l meningitis associated w i t h p u h n o n a r y tuberculosis is reported. T h e t r e a t m e n t of the disease with a m p h o tericin B is discussed; the drug was effective a n d well tolerated. A review of cryptococcosis in the p e d i a t r i c age group f r o m the world l i t e r a t u r e is presented a n d the differences in the clinical manifestations of the disease in the n e o n a t e and the o l d e r child are stressed. Evidence is presented for the occurrence of congenital c r y p t o c o c c a l meningitis. I n the p e d i a t r i c age group, patients with histoplasmosis, moniliasis, H o d g k i n ' s disease, leukemia, sarcoidosis,
Since this article was submitted for publication a paper has appeared in the British Medical fournaI (vol. 2, pp. 91-93, 1961) entitled "Cryptocoecal Meningo-Encephalitis," by W. F. Twining McMath and K. K. Hussain. This article deals with a case of cryptococcal meningoencephalitis in a 4-year-old boy. The child was treated with steroid therapy, 5 mg. doses of prednisolone, tetracycline, 250 mg. every 6 hours, amphotericin B, 0.5 mg. in 5 ml. of water intrathecally and 20 mg. in 250 ml. of 5 per cent dextrose by intravenous drip. He died 3 days following institution of therapy. We wish to thank Dr. H. S. Gordon and the pediatric staff, and the nursing staff, headed by Miss D. Melchior, at Mount Sinai Hospital, Chicago, Ill., for their help. REFERENCES
1. Zenker, F. A.: Encephalitis mit Pilzentwicklungem Gehlrn, Jahresb. d Gesellsch. f. nat.u. Heilk. in Dresd. 62: 51, 1861. 2. Biisse, O.: Ueber parasit~re Zelleinschliisse und ihre Ziichtung, Zentralbl. f. Bakt. 16: 175, 1894. 3. Buschke, A.: Ueber eine durch Coccidien hervorgerufene Krankheit des Menschen, Deutsche reed. Wchnschr. 21: t4, 1895. 4. Vuillemin, P.: Les Blastomycetes pathog&nes, Rev. G6n. de se. pures et Appliq., Paris 12: 732, 1901. 5. Kiitzing, F.: Algarum aqua dulcis germaniae Decas III (1833) (Cited by Benham, 1933). 6. Frothingham, L.: A Tumor-Like Lesion in the Lung of a Horse Caused by a Blastomyces (Torula), J. M. Res. 9: 31, 1902. 7. Von Hansemann, D.: Ueber eine bisher nlcht beobachtete Gehirnerkrankung durch Helen, Verhandl. d. deutsch, path. Gesellsch, f. Chir. 9: 21, 1905. 8. Stoddard, J. L., and Cutler, E. C.: Torula Infection in Man, Monograph of the Rockefeller Institute for Medical Research, New York, 1916, No. 6, p. 1. 9. Lodder, J.: I. Die Hefesammlung des centraal Bureau voor Schimmelcultures. II. Die Anaskosporogenen He fen. Verhand. Akademie
590
10. 11. 12. 13.
14. 15. 16. 17. 18.
19.
20. 21.
22. 23. 24. 25.
26. 27. 28.
EmanueI et al.
Wetenschappen Amsterdam, Afdeeling Natuurkunde, Series 2, 32: 1, 1934. Emmons, C. W.: The Significance of Saprophytism in the Epidemology of the Mycoses, Tr. New York Acad. Sc. 17: 157, 1954. Emmons, C. W.: Isolation of Cryptococcus neoformans From Soil, J. Bact. 62: 685, 1951. Benham, R. W.: Cryptococci---Their Identification by Morphology and by Serology, J. Infect. Dis. 57: 255, 1935. Sanfelice, F.: Contributo alla morfologia e biologia dei blastomiceti the si sviluppano nei suechi di alcuni frutti, Ann. d'Hig., Rome 4: 463, 1894. Littman, M. L., and Zimmerman, L. E.: Cryptococcosis (Torulosis), New York, 1956, Grune & Stratton, Inc. Freeman, W.: Torula Meningoencephalitis; Comparative Pathology in 19 Cases, Tr. Am. Neurol. A. 56: 203, 1930. Carton, C. A., and Mount, L. A.: Neurosurgical Aspect of Cryptococcosis, J. Neurosurg. 8: 143, 1951. Levin, E. A.: Torula Infection of the Central Nervous System, Arch. Int. Med. 59: 667, 1937. Voyles, G. Q., and Beck, E. M.: Systemic Infection Due to Torula Histolytica. Report of 4 Cases and Review of the Literature, Arch. Int. Med. 77: 504, 1946. Cox, L. B., and Tolhurst, J. C.: Human Torulosis. A Clinical Pathological and Microbiological Study With a Report of I3 Cases, Melbourne, 1946, Melbourne University Press. Fitchett, M. S., and Weidman, F.: Generalized Torulosis Associated With Hodgkin's Disease, Arch. Path. 18: 225, 1934. Zimmerman, L. E., and Rappaport, H.: Occurrence of Cryptococcosis in Patients With Malignant Disease of Reticuloendothelial System, Am. J. Clin. Path. 24: 1050, 1954. Smith, F. B., and Crawford, J. S.: Fatal Granulomatosis of the Central Nervous System Due to a Yeast, J. Path. & Bact. 33: 291, 1930. Cabot, R. C., editor: Case Records of the Massachusetts General Hospital, New England J. Med. 210: 1291, 1934. Hoff, C. L.: Immunity Studies of Cryptococcus hominis (Torula histolytica) in Mice, J. Lab. & Clin. Med. 27: 751, 1942. Boshes, L. D., Sherman, I. C., Hesser, C. J., Milzer, A., and Maclean, H.: Fungus Infection of the Central Nervous System; Experience in Treatment of Cryptococcosis With Cycloheximide (Actidione), A. M. A. Arch. Neurol. & Psychiat. 75: 175, 1956. Johns, F. M., and Attaway, C. L.: Torula Meningitis. Report of a Case and Summary of Literature, Am. J. Clin. Path. 3: 45, 1933. Cohen, M.: Binocular Papilledema in a Case of Torulosis Associated With Hodgkin's Disease, Arch. Ophth. 32: 477, 1944. Rodger, R. C., Terry, L. L., and Binford, C. H.: Histoplasmosis, Cryptococcosis and Tuberculosis Complicating Hodgkin's Disease. Report of a Case, Am. J. Clin. Path. 21: 153, 1951.
October 1961
29. Barlow, D. L.: Primary Blastomycotic Meningitis Occurring in Children, M. J. Australia 2: 302, 1923. 30. Carton, C., and Mount, L.: Neurological Aspects of Cryptococcosis, J. Neurol. 8: 143, 1951. 31. Reves, D. L., Butt, E. M., and Hammack, R. N.: Torula Infection of Lungs and Central Nervous System, Arch. Int. Med. 68: 57, 1941. 32. Longmire, W. P., and Goodwin, T. C.: Generalized Torula Infection, Case Report With Review and Observation on Pathogenesis, Bull. Johns Hopkins Hosp. 64: 22, 1939. 33. D'Aunoy, R., and Lafferty, C. R.: Torula Meningitis in a Child, Am. J. Clin. Path. 9: 236, 1939. 34. Marshall, M., and Teed, R. W.: Torula Histolytica Meningoencephalitis. Recovery Following Bilateral Mastoidectomy and Sulfonamide Therapy; Preliminary Report; J. A. M. A. 120: 527, 1942. 35. Dormer, B. A., Friedlander, J., Wiles, F. J., and Simpson, F. W.: Tumor of Lungs Due to Cryptococcus histolyticus, J. Thoracic Surg. 14: 322, 1945. 36. Hamilton, L. C., and Thompson, P. E.: Treatment of Meningitis (Due to Cryptococcus neoformans) With Penicillin, Am. J. Dis. Child. 72: 334, 1946. 37. Debre, R., and others: Development of Meningitis Due to Torula histolytlca in Child 12 Years Old With Malignant Lymphogranulomatosis, Bull. Acad. de m$d., Paris, 130: 443, 1946. 38. Cox, L. B., and Tolhurst, J. C.: Human Torulosis. A Clinical Pathological and Microbiological Study With a Report of 13 Cases, Melbourne, 1946, Belbourne University Press. 39. Mider, G. B., Smith, F. D., and Bray, W. E., Jr.: Systemic Infection With Cryptoeoecus neoformans and Histoplasma capsulation in Same Patient, Arch. Path. 43: 102, 1947. 40. Greening, R. R., and MenviIle, L. G.: Roentgen Findings in Torulosis. Report of 4 Cases, Radiology 48: 381, 1947. 41. Cloward, R. B.: Torula Meningitis. First Case to be Reported in Hawaii, Hawaii M. J. 7: 377, 1948. 42. Neuhauser, E. B. D., and Tucker, A.: The Roentgen Changes Produced by Diffuse Torulosis in the Newborn, Am. J. Roentgen. 59: 805, 1948. 43. Spicer, C., Hiatt, W. O., and Kessel, J. F.: Candida albieans and Cryptococcus neoformans Occurring as Infective Agents in an 8-Year-Old Boy, J. PEDIAT. 33: 761, 1948. 44. Nassau, E., and Weinberg-Heiruti, C.: Torulosis of the Newborn, Harefuah 35: 50, 1948. 45. Health, P.: Massive Separation of Retina in Full Term Infants and Juveni!es, J. A. M. A. 144: 1148, 1950. 46. Lepau, H., Rubinstein, L., Cohn, F., and Shandra, J.: A Case of Cryptococcus neoformans Meningoencephalitis Complicating Boeek's Sarcoid, Pediatrics 19: 377, 1957. 47. Soysal, S. S., Unat, E. K., and Tahslnglu:
Volume 59 Number 4
48.
49. 50.
51.
52.
53. 54.
55.
Amphotericin B in cryptococcus meningitis
Un cas de cryptococcus, Arch. fran~, p~diat. 11: 246, 1954. Oliviera Campos, J.: Congenital Meningoencephalitis Due to Torulosis neoformans. Preliminary Report, Bol. clin. dos Hopit. Civis., Lisbon 18: 609, 1954. Nanda, S., Kass, I., Cohn, M., and Dressier, S.: Coexistence of Tuberculosis and Cryptococcal Meningitis, Pediatrics 20: 45, 1957. Benham, R. W.: The Genus Cryptococcus. The Present Status and Criteria for Identification of Species, Tr. New York Acad. Sc. 17: 418, 1955. Fisher, A. M.: The Clinical Picture Associated With Infections Due to Cryptococcus neoformans (ToruIa histolytica); Report of 3 Cases With Some Experimental Studies, Bull. Johns Hopkins Hosp. 86: 383, 1950. Whitehill, M. R., and Rawson, A. J.: Treatment of Generalized Cryptococcosls With 2Hydroxystilbamidine, Virginia M. Month. 81: 591, 1954. Hall, B. D., and Mardis, R. E.: Treatment of Cryptococcosis With Terramycin, U.S. Armed Forces M. J. 4: 1061, 1953. Christie, A., Middleton, J. G., Peterson, J. C., and McVickar, D. L.: Treatment of Disseminated Histoplasmosis With Ethyl Vanillate, Pediatrics 7: 7, 1951. Wilson, H. M., and Duryea, A. W.: Cryptococcus Meningitis (Torulosis) Treated With a New Antibiotic, Actidione, A.M.A. Arch.
59 1
Neurol. & Psychiat. 66: 470, 1951. 56. Weller, T. H., Maculey, J. C., Craig, J. M., and Wirth, P.: Isolation of Intranuclear Inclusion Producing Agents From Infants With Illness Resembling Cytomegalic Inclusion Disease, Proc. Soc. Exper. Biol. & Med. 94: 4, 1957. 57. Guyton, T. B., Ehrlich, F., Blanc, W. A., and Becker, M. H.: New Observation in Generalized Cytomegalic Inclusion Disease of the Newborn, New England J. Med. 257: 803, 1957. 58. Sabin, A. B., and Feldman, H. A.: Chorioretinopathy Associated With Other Incidence of Cerebral Damage in Childhood Syndrome of Unknown Etiology Separable From Congenital Toxoplasmosis, J. PEDIAT. 55: 296, 1949. 59. Bomati, J., Rogers, J. V., and Hopkins, W. A.: Pulmonary Cryptococcosis, Radiology 66: 188, 1956. 60. Berk, M., and Gerstl, B.: Torulosis Producing a Solitary Pulmonary Lesion; Report of a Four Year Case With Lobectomy, J. A. M. A. 149: 1310, 1952. 61. Evans, E. E., and Harrell, E. R.: Cryptococcosis: A Review of Recent Cases, Univ. Michigan, M. Bull. 18: 43, 1952. 62. Ratcliffe, H. E., and Cook, W. R.: Cryptococcosis: Review of the Literature and Report of a Case With Initial Puhnonary Findings, U.S. Armed Forces M. J. 1: 957, 1950.