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A placebo-controlled trial of cyclosporine enemas for mildly to moderately active left-sided ulcerative colitis
A Placebo-Controlled Trial of Cyclosporine Enemas for Mildly to Moderately Active Left-Sided Ulcerative Colitis WILLIAM J. SANDBORN,* WILLIAM J. TREMAINE,* KENNETH W. SCHROEDER,* KENNETH P. BATTS,? GEORGE M. LAWSON,’ BETTY L. STEINER,* JAY M. HARRISON,” and ALAN R. ZINSMEISTER5 *Inflammatory Bowel Disease Clinic, Division of Gastroenterology, ‘Department Biostatistics, Mayo Clinic and Mayo Foundation, Rochester, Minnesota
Background/Aims: Uncontrolled studies suggest that cyclosporine administered as an enema may be of benefit for left-sided ulcerative colitis and safer than intravenous or oral administration. The efficacy and safety of cyclosporine enemas for left-sided ulcerative colitis in a placebo-controlled trial was assessed. Methods: Steroid and mesalamine enemas were withdrawn be fore the study. Forty patients were assigned to 1 of 4 strata: no concomitant therapy, oral steroids, oral salicylates, or oral steroids and salicylates. After stratification, patients were randomized to nightly treatment with 350 mg cyclosporine (n = 20) or placebo (n = 20) enemas. Clinical response was determined at baseline and 4 weeks by endoscopy, physician assessment, and a patient diary of daily symptoms. Trough blood cyclosporine levels were measured by high-performance liquid chromatography. Results: At 4 weeks, 8 of 20 patients (40%) who received cyclosporine showed clinical improvement compared with 9 of 20 patients (45%) who received placebo. One patient receiving cyclosporine had reversible neutropenia attrib utable to sulfasalazine, and another patient receiving cyclosporine was unable to tolerate the enema vehicle. No other toxicity was noted during the trial. Blood cyclosporine levels were detectable in only two patients. Conclusions: Cyclosporine enemas administered in a dosage of 350 mg/day for 4 weeks are not efficacious in mildly to moderately active left-sided ulcerative colitis.
of Laboratory Medicine and Pathology, *Section of
toxicity
cyclosporine
treatment
C
is a cyclic endecapeptide
that has revolu-
tionized solid organ transplantation because of its unique ability to selectively inhibit cellular immunity.’ Multiple uncontrolled studies have suggested that cyclosporine administered orally or intravenously is of benefit in patients with severe ulcerative colitis who are refractory to standard therapy.2-‘7 Two controlled trials of oral or intravenous cyclosporine in patients with mildly to moderately active18 and severely activer” ulcerative colitis have confirmed these observations. Serious,
oral
and
of inflammatory
intravenous
bowel disease has
been minimal,
but there is a high incidence of cyclosporexperience with side effects.20 Furthermore,
ine-related cyclosporine
in other settings,
such as organ transplanta-
tion, has shown that serious toxicity In an attempt avoiding
to reduce
can occur.
cyclosporine
small bowel absorption,
side effects by
cyclosporine
has been
administered as an enema. We have previously reported a pharmacokinetic study showing that blood concentrations are negligible
and colonic
tissue concentrations
are
quite high after enema administration of cyclosporine.21 Four uncontrolled studies of cyclosporine enema treatment
for patients
with
left-sided
ulcerative
colitis
have
reported response rates ranging from 50% - 7 5 % .22-26 No side effects attributable to cyclosporine have been reported
after enema administration.
sults of a 4-week (350 mg/day)
controlled
in patients
We report
trial of cyclosporine
with active left-sided
the reenemas
ulcerative
colitis.
Materials Study
and Methods
Design
This study was a randomized, double-blind, placebocontrolled trial using 350 mg/day ofcyclosporine administered as an enema in patients with mildly to moderately active leftsided ulcerative colitis. Patients were assigned to 1 of 4 strata based on treatment
yclosporine
during
irreversible
no treatment, olsalazine, roids,
with
oral mesalamine),
or treatment
Patients
at the time of enrollment
treatment with
were not stratified
oral salicylates treatment
oral salicylates
with
into the study: (sulfasalatine, oral corticoste-
and corticosteroids.
for topical therapy (topical cortico-
steroids or mesalamine) because these medications were discontinued before beginning the study medication for reasons discussed within
below. To maintain a balance of treatment groups each stratum, randomization was performed separately
0 1994 by the American Gastroenterological Association 00165085/94/$3.00
GASTROENTEROLOGY Vol. 106, No. 6
1430
SANDBORN ET AL.
within
each of the four strata using a randomization
developed
sequence
in the Section of Biostatistics.
Patients From September patients
with mildly
1991 to November
to moderately
colitis were referred by colleagues
1992, 40 adult
active left-sided
ulcerative
at the Mayo Clinic for enroll-
ment into the study. Active ulcerative
colitis was diagnosed
the usual symptomatic,
and endoscopic
criteria.
disease were excluded
because
Patients
radiographic,
with newly diagnosed
we wished to study patients to standard tutional
treatment.27
Review
gave informed,
who tended
The study was approved
and/or
continued
at prestudy
been changed
during doses
studying topical
(sulfasalazine,
oral corticosteroids
corticosteroid
therapies
120
the previous >20
were
Corticosteroid at least
perrectal
medications.
During
to take metronidazole, azathioprine,
to avoid
1 week
ova and parasites,
were required
evaluations
or other investiexamination
Women
to have a negative
count,
chemistry
pregnancy
tients
with renal dysfunction >2X
a trough
whole
(serum (alkaline
normal)
nine levels were measured performance
blood
panel,
test
complete
and urinalysis.
creatinine
Pa-
> 1.5X
phosphatase
nor-
or aspartate
were excluded.
Serum creati-
after 2 weeks of treatment,
cyclospotine
concentration
liquid chromatography)
and
(by high-
was determined
Throughout
the study, patients
at the 4-
kept a daily record of
the number of their stools, any rectal bleeding,
their subjective
sense of well-being,
the degree of abdominal
discomfort,
any other symptoms
coinciding
sent adverse reactions. of
during the trial. Laboratory
screening
mal) or hepatic dysfunction aminotransferase
for
capable
at the initial and 4-week visits included
blood
Disease Activity Assessment
6-
a negative stool culture for enteric pathogens,
and asked to practice contraception
Index
Stool frequency 0, Normal number of stools for this patient 1, l-2 stools more than normal 2, 3-4 stools more than normal 3, 5 or more stools more than normal Rectal bleeding 0, No blood found 1, Streaks of blood with stool less than half the time 2, Obvious blood with stool most of the time 3, Blood alone passed Sigmoidoscopic findings 0, Normal or inactive disease 1, Mild disease (etythema, decreased vascular pattern, mild friability) 2, Moderate disease (marked erythema, absent vascular pattern, friability, erosions) 3, Severe disease (spontaneous bleeding, ulceration) Physician’s global assessment 0, Normal 1, Mild disease 2, Moderate disease 3, Severe disease
the study, patients
had a negative toxin.
Activity
before
oral cyclosporine,
methotrexate,
Clostridim difiile
and a negative conception
each patient
Disease
with retention
drugs.
Before entry,
Colitis
and mesalamine
difficulties
mercaptopurine,
were
receiving
excluded
were discontinued
were not allowed
mesala-
mg/day)
2 weeks. Patients
mg/day
the study to avoid potential
of multiple
gational
olsalazine,
(dose,
doses during the trial if the doses had not
severely ill patients.
entering
by the Insti-
and all patients
consent.
Oral salicylate compounds mine)
to be more refractory
Board of the Mayo Clinic, written
by
Table1. Ulcerative
Patients
and after 4 weeks according that
measured
findings,
stool
severe) reflected
endoscopic physical
findings,
findings
rectal
and pertinent
and performance
mesalamine
ment was determined
physician
at the 4-week visit and from patient
remission
and clinical
sigmoidoscopy. marcation
Left-sided
disease extent
between endoscopically
was defined
as a de-
inflamed and endoscopically
normal colonic mucosa located not more than 60 cm from the anal verge. If the demarcation
was at exactly 60 cm (as mea-
sured by a 60-cm flexible sigmoidoscope), normal
colonic
mucosa
the tip of the endoscope. between
endoscopically
tissue was >60 the study.
then endoscopically
had to be clearly visible Patients inflamed
in which
proximal
and endoscopically
normal
cm from the anal verge were excluded
Colonic
mucosal
biopsy
during
each endoscopy
to confirm
severity
of histological
inflammation,
Ionic tissue concentration
specimens
from
were obtained
the diagnosis, and determine
of cyclosporine.
to
the demarcation
assess the the co-
improvement
indices
such
as
criteria
and Baron et a12’
appearance, has been used
in other studies of oral mesalamine
week visit. The extent and severity of colonic mucosal involveat the initial and 4-week visits by flexible
mild,
symptoms,
ofTtuelove’s28
the degree of clinical activity
enemas.32-33 Adverse
(quiescent,
recorded
clinical
criteria for grading the sigmoidoscopic previously
endoscopic
(Table 1). The phy-
status. This disease activity
index, which was based on modifications for classifying
bleeding,
of disease activity the patient’s
at study entry
disease activity index
global assessment
sician’s global assessment moderate,
were evaluated
to a 12-point
frequency,
and physician’s
and
with therapy that might repre-
therapy3”-3’ and
events were evaluated
by a
diaries. Clinical
were defined
as a disease
activity index score of zero and a decrease in the disease activity index of at least three points, respectively. Histological disease activity was also assessed at study entry and after 4 weeks according to a four-point histological disease activity index (Table 2).22 Assessed features included the nature (polymorphonuclear vs. entirely mononuclear) and distribution (lamina propria vs. cryptal) of the inflammatory cell infiltrate as well as the degree of glandular destruction and/or ulceration. Endoscopic biopsy specimens were obtained from the site in the distal colon that appeared to have the most severe inflammatory change. The histological disease activity index score was determined by a single pathologist (K.P.B.) who was
CYCLOSPORINE ENEMAS FOR ULCERATIVE COLITIS
June 1994
Table 2. Histological
Disease
Activity Index
0, Normal (normocellular lamina propria, PMNs absent) 1, inactive chronic colitis (hypercellular lamina propria, PMNs absent) 2, Mild active chronic colitis (scant PMNs in lamina propria, occasional cryptitis but few crypt abscesses, minimal glandular destruction or ulceration) 3, Moderately active chronic colitis (moderate numbers of PMNs in lamina propria with ct-yptitis and crypt abscesses prominent, some glandular destruction) 4. Severely active chronic colitis (numerous PMNs with abundant cryptitis, crypt abscesses, extensive glandular destruction, ulceration may be prominent) PMN, polymorphonuclear
cyclosporine as previously described.‘s.2’-23 The last enema was taken approximately 15 hours before the biopsies were performed. The tissue samples from each patient were frozen at -20°C in a drop of Tissue Tek (Miles Inc., Diagnostic Division,
Elkhart,
thawed, stool,
rinsed
IN). At the time of assay, the samples were
in 0.9%
or cyclosporine
and weighed.
saline
(to remove
adherent
Cyclosporine
minutes.
any Tissue
was extracted
by placing
the tissue
and homogenizing
The samples were then assayed for cyclosporine
the same methodology
that
Tek,
to the surface of the tissue),
in 2 mL of 9:l acetonitrile/methanol
for 2 using
we use for the measurement
whole blood cyclosporine.3’-‘6 tions were expressed
leukocyte.
1431
Tissue cyclosporine
in nanograms
of
concentra-
per gram wet tissue.
Statistical Methods blinded
to patient
identification,
point
in time (entry
week), and clinical status. The slides were reviewed sitting
in a randomized
histological activity
fashion.
improvement
Histological
disease activity
remission
and
disease
in the histological
index of at least one point,
The treatment
at a single
were defined as a histological
index score of zero and a decrease
vs. 4-
respectively.
baseline
demographic
and histological
Treatment Patients
consisted
were instructed
to add 3.5 mL of blinded-study
cation to the enema vehicle and retain
retention
were recorded
Each enema vehicle was composed
(Ruger Chemical Co., Irvington, methylcellulose
(Spectrum
isoosmolar
and the carboxymethylcellulose
added
to suspend
The vehicle,
into individual
This
g of sorbitol described
Corp.,
dose of sorbitol
reported
(Sandimmune East Hanover,
oral solution;
olive oil, were each dispensed
that the cremophors
castor oil for intravenous
oxyethylated
oleic glycerides
to extract
Sandoz Phar-
NJ), and the placebo
oxyethylated potential
was dispensed
The active study medi-
in llO-mL
glass bottles. The blinded-study medications cebo) were not mixed with the vehicle until because of concern
brown
in cyclosporine concentrate
phthlate
study
(active vs. plajust before use
for the oral solution)
diethylhexyl
(poly-
and polyhave the
from the polyvinyl
chloride enema bottles into the solution. s* Compliance determined by review of the patient diaries.
was
Measurement of Colonic Tissue Cyclosporine Concentration We obtained four mucosal pinch biopsy specimens from the rectosigmoid colon during flexible sigmoidoscopy performed
at the
4-week
visit
group between
treatment
group
change
a difference,
for assay of colonic
tissue
time
in the disease tissue
was considered
activity
index
vs.
concentra-
significant. group
and 20 in
there was 75% power for de-
corresponding
group
vs.
and were used
cyclosporine
in the placebo-treated group,
change in
vs. not improved)
retention
P <0.05
20 patients
the cyclosporine-treated tecting
(improved
and colonic
tions. A two-tailed With
index
and enema
separately
to 80%
compared
improvement
in
with 40% improvement
in
test at a type I error rate
of 5%.
Results
is well
to cause a cathartic
previously,*i~**
100-mL enema bottles.
cation, cyclosporine medication,
Corp.,
the vehicle
cyclosporine.
activity
NJ), and 500 mg carboxyto make
improvement,
rank tests or extensions Logistic regression
the placebo group using a two-sided
Manufacturing
to
between
of 60 mL water, 5 g sorbitol
was added
below the 20-30
maceutical
and the
on a daily basis.
clinical
using
the cyclosporine
Chemical
CA). The sorbitol
the hydrophobic effect.
of 1 hour or overnight
The time that the enema was administered of enema
Gardena,
medi-
just before use, shake vigorously,
the enema for a minimum
if possible. duration
for 4 weeks.
characteristics,
improvement
with regard
models were used to assess the relationship treatment
of one enema nightly
were compared
of Fisher’s Exact Test for ordered categories. the disease
Cyclosporine Enema Treatment
groups
There were no significant cyclosporine
and placebo
comparisons
of demographic
severity (Table 3), initial and current or previous
groups
differences
between
the
with regard to baseline
characteristics
and disease
disease assessment (Figure l), drug therapy (Table 4). The
duration of symptoms can be classified as follows for the cyclosporineand placebo-treated patients, respectively: recent flare (< 30 days), 0 of 20 and 1 of 20; intermediate duration (30-90 days), 5 of 20 and 4 of 20; and chronically active (>90 days), 15 of 20 and 15 of 20. The median
duration
of symptoms
in the cyclosporine
and
placebo groups was 210 and 225 days, respectively (Table 3). Only six patients (two receiving cyclosporine and four receiving placebo) were not receiving concomitant oral corticosteroids and/or salicylates during the study; of these, four had topical corticosteroids or mesalamine therapy withdrawn 2 weeks before the study. Thus, the majority of patients in both groups had chronically active and refractory disease as evidenced by a long duration of
1432 SANDBORN ET AL.
Table 3. Patient
Demographic
40 Patients Treated
GASTROENTEROLOGY Vol. 106, No. 6
Data and Disease
With Left-Sided
Ulcerative
With Cyclosporine
43
Age at entry (yf) Duration of ulcerative colitis (yr) Duration of current symptoms (days) Extent of disease (cm) Initial DAI score (range, O-12) Initial HDAI score (range, O-4)
Median
Range
38
l-4
26-68 o-21
5 210 43
5-11
3 IO/IO
Sex (M/F)
Range
14-6570 lo-60
8
42-3650 12-60
8
4-10
3 13/7
l-4
NOTE. No significant differences were detected for any of these characteristics (P > 0.05). DAI. clinical disease activity index; HDAI, histological disease activity index.
symptoms
and the need
with corticosteroids The
for concomitant
and/or
rates of clinical
oral therapy
salicylates.
and
histological
improvement
after 4 weeks of therapy were not significantly between the placebo and cyclosporine groups patients
with left-sided
ema treatment the 4-week
ulcerative
was discontinued
treatment
period
and Previous
With Left-Sided
Drug Therapy
Ulcerative
colitis
in 40 Patients
Treated
With
Current drug therapy No current treatment Salicylatesa Steroids Salicylates” and steroids Recently discontinued drug therapyb Topical steroids Topical mesalamine Previous drug therapyC Oral steroids Topical steroids Sulfasalazine Olsalazine Oral mesalamine Topical mesalamine Azathioprine or 6mercaptopurine
Placebo (n = 20) (%)
Cyclosporine (n = 20) (%)
20 40 15 25
10 40 20 30
30 15
25 20
30 45 55 10 10 40
20 65 50 I.5 10 60
5
15
NOTE. No significant differences were detected acteristics (P > 0.05). “Salicylates are sulfasalazine, olsalazine, and Therapy discontinued ~~14 days before study Therapy discontinued >I4 days before study
for any of these charoral mesalamine. entry. entry.
different in these
(Table
5). En-
in nine patients
before
was completed
Colitis
Enemas
Cyclosporine (n = 20)
O-24
225 38
Table 4. Current
Cyclosporine
21-69
2
in
Enemas
Placebo (n = 20) Median
Severity Colitis
because
of
worsening symptoms requiring initiation or increase of the dose of corticosteroids and/or hospitalization. This
included
6 of 20 patients
(30%) in the cyclosporine
and 3 of 20 (15 %) in the placebo group. No association between improvement in clinical
dis-
ease activity and colonic tissue cyclosporine concentrations was detected (P > 0.15). Among patients in the cyclosporine group, there was not a significant in the colonic tissue cyclosporine concentrations with clinical
8
group
remission
and improvement
difference for those
(median,
772
ngig; range, O-5885 “g/g) and those who failed to improve (median, 0 rig/g;; range, O-5998 “gig). Similarly,
Table 5. Response
to Treatment
in 40 Patients
0
SCOW
1
2
3
Score
Figure 1. Frequency distribution of baseline scores (O-3 points) for the individual components of the disease activity index: (A) stool frequency, (6) rectal bleeding, (C) sigmoidoscopic findings, and (D) physician global assessment. There were no significant differences in the frequency distribution of scores between the placebo and cyclosporine groups for any of the categories. ?T, ?cyclosporine (n = 20).
Disease activity index Clinical remission Clinical improvement’ Clinical failure Histological disease activity index Histological remission Histological improvement’ Histological failure
With Cyclosporine
With Left-Sided
Ulcerative
Enemas Colitis
Placebo
Cyclosporine
Pa
(n = 20) 1 9 11
(n = 20) 1 8 12
0.90 0.90 0.90
(n = 18) 1 7 11
(n = 19) 1 6 13
0.77 0.77 0.77
a/=’ based on an extension of Fisher’s Exact Test for ordered categories. bClinical improvement includes clinical remission. ‘Histological improvement includes histological remission.
CYCLOSPORINE ENEMAS FOR ULCERATIVE COLITIS
June 1994
enema
retention
time
was not significantly
associated
with improvement in the disease activity index. The median enema retention time in the placebo group was 6.3 hours (range, 2.4-8.3 group ever,
hours), whereas in the cyclosporine
it was 4.1 hours (range, there
retention
1.0-12.7
was significantly
times
greater
for the cyclosporine
Two patients
receiving
verse events during
hours).
variation group
cyclosporine
Howin (log)
(P < 0.01).
experienced
ad-
the study; both received cyclosporine.
One patient had an absolute neutrophil count of 5001 mm3 after 4 weeks in the study. The patient had started taking
sulfasalazine
8 weeks before entering
Both the cyclosporine withdrawn,
enemas
the study.
and the sulfasalazine
and the neutropenia
was later rechallenged
with
absence of sulfasalazine
therapy,
resolved.
cyclosporine
were
The patient enemas
and the neutropenia
in the did
and three patients
twice daily for 4 weeks (2.5 mg/kg 0.75 mg/kg Winter
administering the cyclosporine enemas, the patient developed severe abdominal cramping and worsening diar-
et al. used cyclosporine
cyclosporine
enemas
The present trolled
(350 mg/day
randomized,
tive colitis
was designed
uncontrolled
studies
no significant
differences
between
the
of clinical
and those who were removed
breath test performed
withafter
enema administration to assess for carbohydrate intolerance to the sorbitol in the enema vehicle was negative. Except
for the
patient
with
neutropenia
described
above, none of the patients in the study had any clinically important changes in the following parameters: systolic and diastolic blood pressure, complete blood count, serum chemistry group levels (including alkaline phosphatase, aspartate aminotransferase, total bilirubin, direct bilirubin, creatinine, and urea), and urinalysis. Trough whole blood cyclosporine
concentrations
able in all but two patients receiving receiving
(56 ng/mL
were significantly
of patients
Discussion Four uncontrolled trials have reported improvement of left-sided ulcerative colitis during treatment with cyclosporine enemas. 22,24-26 Brynskov et al. used cyclosporine enemas (250 mg/day for 2 weeks) in seven patients with refractory ulcerative proctitis and one patient with an ileostomy and colitis in the blind rectal stump and reported a response of 75%.** Ranzi et al. treated three patients with refractory proctosigmoiditis
the results
extent
and
of the
improve-
placebo-treated
was actually greater in
(30%) than the placebowere no significant who completed early with
differ-
the study
regard
to the
of disease (43 cm vs. 45 cm for
colitis involving
ing colon did not result in the selection more severe disease. The rate of histological
the descend-
of patients
with
improvement
was even lower than the rate of clinical improvement, and there was not a significant difference between the two groups.
ported
is 25 ng/mL.
There
those patients
with ulcerative
in one patient
peutic level range of 100-300 ng/mL, and the value of 30 ng/mL was near the lower limit of sensitivity for our assay, which
proximal
The negative what surprising.
below the thera-
(15%).
ulcera-
the cyclosporine group and 38 cm vs. 60 cm for the placebo group). These findings suggest that the inclusion
were undetect-
cyclosporine and 30 ng/mL in another patient placebo). The blood cyclosporine concentra-
tions in these patients
median
group
placebo-con-
from the study because
symptoms group
with with
above.2’,24-26 We found
cyclosporine-
symptoms
A hydrogen
we have
in the rate of clinical
the cyclosporine-treated
for
colitis
for left-sided
to confirm
discussed
The rate of early removal
of worsening treated
ulcerative
for 4 weeks).‘*
enemas
ences between
when the enema vehicle was administered
(250 mg/day
double-blind,
trial of cyclosporine
and
of 50%.
reported a 50% response in 10 patients ulcerative colitis after treatment
rhea that lasted for 12 hours. The symptoms recurred with two rechallenges. The patient also experienced similar out cyclosporine.
enemas
rate of 58%.26 Finally,
a response
enemas
in three patients
and reported previously left-sided
ment
after
ileosmucous
with a response
with left-sided
groups.
30 minutes
in three patients)
6 weeks) in 12 patients
to the enema
Approximately
colectomy,
tomy, and colitis in a sigmoidorectal remnant fistula.*’ These patients received cyclosporine
not recur. The other adverse event seemed to be related vehicle.
with prior subtotal
1433
results of our controlled trial are someMultiple uncontrolled studies have re-
improvement
of ulcerative
colitis after treatment
with oral or intravenous cyclosporine2-” with an average response rate of 80%.20 These uncontrolled results were recently confirmed by a controlled trial of intravenous cyclosporine for severe ulcerative colitis, which reported a response of 820/o.‘” In comparison with the apparent efficacy of oral and intravenous cyclosporine for ulcerative colitis, cyclosporine enemas are not efficacious. These findings stand in contrast with other medications used to treat ulcerative colitis, such as corticosteroids and mesalamine, which are efficacious with both oral and topical administration. There are a number of potential explanations for our negative results. First, the dose of cyclosporine may have been too low or the dosing interval too infrequent. The mean oral cyclosporine dose reported to be efficacious in ulcerative colitis is 8 mg kg-’ .day-‘.I0 The cyclosporine
GASTROENTEROLOGY Vol. 106, No. 6
1434 SANDBORN ET AL.
dose
used
in
this
study
was
350
mglday
(5
mg.kg-’ .day-’ for a i’O-kg patient). However, this dose is higher than the doses used in most of the other uncontrolled trials.24-26 Second, the water-based enema vehicle that we and others used’1-26 may not provide optimal delivery of cyclosporine the treatment duration possibility
to the colonic
seems unlikely
ally reported
mucosa.
Third,
may have been too short. because cyclosporine
to act within
l-2
This
is gener-
weeks in patients
with
ulcerative colitis.*’ Fourth, the patients we selected for the study were in general refractory to standard therapy. who have not already
Patients
and salicylate cyclosporine proven
therapy
failed oral corticosteroid
may have a better
enemas than patients
to be refractory
to other medications.
tients with disease in the descending differently sigmoid
than
patients
with
colon and rectum,
disease
by cyclosporine
helper cell interleukin 2 production to stop the inflammatory reaction reported
tween colonic tissue cyclosporine tention
and a strong
time and clinical
Fifth,
pa-
confined
to the
in which case the combining
local immunosuppression
cal response
to
colon may respond
of these two groups could mask treatment
We have previously
response
who have already been
effects. Finally, of colonic
T-
may not be sufficient in ulcerative colitis. a weak association
concentration
association
between
be-
and clinienema re-
response.22 These uncontrolled
observations were not confirmed in the present controlled trial. Whether colonic tissue cyclosporine concentrations are associated
with clinical
response
in patients
treated
with oral or intravenous cyclosporine is unknown, although a preliminary report has suggested that this may be the case.‘> No toxicity clinically
directly
important
attributable
to cyclosporine
side effects were noted
during
or the
trial. Presumably, the absence of toxicity and side effects relates to the fact that the cyclosporine administered as an enema is generally not absorbed. A similar lack of toxicity during cyclosporine enema treatment has been previously reported.2’-26 In contrast, side effects occur frequently when cyclosporine is administered orally or intravenously.20 We conclude that cyclosporine enemas administered in a dose of 350 mglday for 4 weeks are not efficacious in the treatment of mildly to moderately active left-sided ulcerative colitis. Cyclosporine enemas are safe and welltolerated when administered daily for 4 weeks. Future studies should evaluate higher dosages of cyclosporine, more frequent dosing schedules, alternative enema vehicles, patients with disease extent limited to the sigmoid colon (535 cm), and patients who have not already proven refractory to other forms of therapy.
References 1. Hess AD, Tutschka PJ, Santos GW. Effect of cyclosporin A on human lymphocyte response in vitro. III. CsA inhibits the production of T lymphocyte growth factors in secondary mixed lymphocyte responses but does not inhibit the response of primed lymphocytes to TCGF. J lmmunol 1982; 128:355-359. 2. Gupta S, Keshavarzian A, Hodgson HJF. Cyclosporin in ulcerative colitis. Lancet 1984;1:1277-1278. 3. Kirschner BS, Whitington PF, Black DD, Bostwick D. Cyclosporininduced remission in severe colitis unresponsive to corticosteroid therapy (abstr). Pediatr Res 1987;21:271A. 4. Bianchi Porro G, Panza E, Petrillo M. Cyclosporin A in acute ulcerative colitis. ltal J Gastroenterol 1987; 19:40-41. 5. Shelly ED, Shelly WB. Cyclosporine therapy for pyoderma gangrenosum associated with sclerosing cholangitis and ulcerative colitis. J Am Acad Dermatol 1988; 18:1084-1088. 6. Hyams JS, Treem WR. Cyclosporine treatment of fulminant colitis. J Pediatr Gastroenterol Nutr 1989; 9:383-387. 7. Stange EF, Fleig WE, Rehklau E, Ditschuneit H. Cyclosporin A treatment in inflammatory bowel disease. Dig Dis Sci 1989; 34: 1387-1392. 8. Baker K, Jewel1 DP. Cyclosporin for the treatment of severe inflammatory bowel disease. Aliment Pharmacol Ther 1989;3: 143-149. 9. Lichtiger S, Present DH. Preliminary report: cyclosporin in treatment of severe active ulcerative colitis. Lancet 1990;336:1619. 10. Lichtiger S. Cyclosporine therapy in inflammatory bowel disease: open-label experience. Mt Sinai J Med 1990;57:315-319. 11. Bianchi Porro G, Petrillo M, Ardizzone S. Cyclosporin treatment for severe active ulcerative colitis (letter). Lancet 1990;336:439. 12. Gavaler JS, Delemos B, Belle SH, Heyl AE, Tarter RE, Starzl TE, Gavaler C, Van Thiel D. Ulcerative colitis disease activity as subjectively assessed by patient-completed questionnaires following orthotopic liver transplantation for sclerosing cholangitis. Dig Dis Sci 1991;36:321-328. 13. Shaked A, Colonna JO, Goldstein L, Busuttil RW. The interrelation between sclerosing cholangitis and ulcerative colitis in patients undergoing liver transplantation. Ann Surg 1992;215:598-603. 14. Treem WR, Davis PM, Hyams JS. Cyclosporine treatment of severe ulcerative colitis in children. J Pediatr 1991;119:994-997. 15. Sandborn WJ, Goldman DH, Lawson GM, Perrault J. Measurement of colonic tissue cyclosporine concentration in children with severe ulcerative colitis. J Pediatr Gastroenterol Nutr 1992; 15: 125-129. 16. Actis GC, Ottobrelli A, Pera A, Barletti C, Ponti V, Pinna-Pintor M, Verme G. Continuously infused cyclosporine at low dose is sufficient to avoid emergency colectomy in acute attacks of ulcerative colitis without the need for highdose steroids. J Clin Gastroenterol 1993; 17:10-13. 17. Lichtiger S, Present DH. Cyclosporin A in the treatment of severe ulcerative colitis (abstr). Gastroenterology 1992; 102:A653. 18. Sandborn WJ, Wiesner RH, Tremaine WJ, LaRusso NF. Ulcerative colitis disease activity following treatment of associated primary sclerosing cholangitis with cyclosporin. Gut 1993;34:242-246. 19. Lichtiger S, Present DH, Kornbluth A, Hanauer S. Cyclosporin A in the treatment of severe, refractory ulcerative colitis: a double blinded placebo controlled trial (abstr). Gastroenterology 1993; 104:A732. 20. Sandborn WJ, Tremaine WJ. Cyclosporine treatment of inflammatory bowel disease. Mayo Clin Proc 1992;67:981-990. 21. Sandborn WJ, Strong RM, Forland SC, Chase RE, Cutler RE. The pharmacokinetics and colonic tissue concentrations of cyclosporine after IV, oral, and enema administration. J Clin Pharmacol 1991; 31:76-80.
CYCLOSPORINE ENEMAS FOR ULCERATIVE COLITIS
June 1994
22. Sandborn WJ, Tremaine WJ, Schroeder KW, Steiner BL, Batts KP, Lawson GM. Cyclosporine enemas for treatment of treatmentresistant, mildly to moderately active, left-sided ulcerative colitis. Am J Gastroenterol 1993;88:640-645. 23. Sandborn WJ, Tremaine WJ. Cyclosporin enemas for therapy-resistant ulcerative proctitis. In: Demling L, Fruhmorgen P, eds. Non-neoplastic diseases of the anorectum. Lancaster, UK: Klewer, 1992:333-339. 24. Brynskov J, Freund L, Thomsen 00, Anderson CB, Rasmussen SN, Binder V. Treatment of refractory ulcerative colitis with cyclosporine enemas. Lancet 1989; 1:721-722. 25. Ranzi T, Campanini MC, Velio P, Quart0 di Palo F, Bianchi P. Treatment of chronic proctosigmoiditis with cyclosporin enemas (letter). Lancet 1989;2:97. 26. Winter T, Dalton HR. Merrett MN, Campbell A, Jewel1 DP. Cyclosporin A retention enemas in refractory distal colitis: an open trial (abstr). Gastroenterology 1992; 102:A947. 27. Jarnerot G, LennardJones J, Bianchi-Porro G, Brynskov J, Campieri M, Present DH. Medical treatment of refractory distal ulcerative colitis. Gastroenterol Int 1991;4:93-98. 28. Truelove SC. Treatment of ulcerative colitis with local hydrocortisone hemisuccinate sodium: a report on a controlled therapeutic trial. Br Med J 1958;2:1072-1077. 29. Baron JH, Connell AM, Lennard-Jones JE. Variation between observers in describing mucosal appearances in proctocolitis. Br Med J 1964; 1:89-92. 30. Schroeder KW, Tremaine WJ, llstrup DM. Coated oral 5aminosalicylic acid therapy for mildly to moderately active ulcerative colitis: a randomized study. N Engl J Med 1987;317:1625-1629. 31. Sninsky CA, Cart DH, Shanahan F, Powers BJ, Sessions JT, Pruitt RE, Jacobs WH, Lo SK, Targan SR, Cerda JJ, Gremillion DE, Snape
32.
33.
34.
35. 36.
1435
WJ, Sabel J, Jinch H, Swinehart JM, DeMicco MP. Oral mesalamine (Asacol) for mildly to moderately active ulcerative colitis. Ann Intern Med 1991; 115:350-355. Sutherland LR, Martin F, Greer S, Robinson M, Greenberger N, Saibil F, Martin T, Sparr J, Prokipchuk E, Borgen L. 5-aminosalicylic acid enema in the treatment of distal ulcerative colitis, proctosigmoiditis, and proctitis. Gastroenterology 1987; 92: 1894-1898. Biddle WL, Greenberger NJ, Swan JT, McPhee MS. Miner PB. 5aminosalicylic acid enemas: effective agent in maintaining remission in left-sided ulcerative colitis. Gastroenterology 1988;94: 1075-1079. Venkataramanan R, Burckart GJ, Ptachcinski RJ, Blaha R, Logue LW, Bahrson A, Choo-Seng G, Brady JE. Leaching of diethylhexyl phthalate from polyvinyl chloride bags into intravenous cyclosporine solution. Am J Hosp Pharm 1986;43:2800-2802. Moyer TP, Charlson JR, Ebnet LE. Improved chromatography of cyclosporine. Ther Drug Monit 1986;8:466-468. Moyer TP, Johnson P, Faynor SM, et al. Cyclosporine: a review of drug monitoring problems and presentation of a simple, accurate liquid chromatographic procedure that solves these problems. Clin Biochem 1986; 19:83-89.
Received May 21, 1993. Accepted November 30, 1993. Address requests for reprints to: William 1. Sandborn, M.D., Mayo Clinic, 200 First Street S.W., Rochester, Minnesota 55905. Fax: (507) 284-0538. Supported by a grant from Sandoz Pharmaceutical Corporation. Presented at the annual meeting of the American Gastroenterological Association in Boston, Massachusetts, May 17-19, 1993.
Background/Aims: Uncontrolled studies suggest that cyclosporine administered as an enema may be of benefit for left-sided ulcerative colitis and safer than intravenous or oral administration. The efficacy and safety of cyclosporine enemas for left-sided ulcerative colitis in a placebo-controlled trial was assessed. Methods: Steroid and mesalamine enemas were withdrawn be fore the study. Forty patients were assigned to 1 of 4 strata: no concomitant therapy, oral steroids, oral salicylates, or oral steroids and salicylates. After stratification, patients were randomized to nightly treatment with 350 mg cyclosporine (n = 20) or placebo (n = 20) enemas. Clinical response was determined at baseline and 4 weeks by endoscopy, physician assessment, and a patient diary of daily symptoms. Trough blood cyclosporine levels were measured by high-performance liquid chromatography. Results: At 4 weeks, 8 of 20 patients (40%) who received cyclosporine showed clinical improvement compared with 9 of 20 patients (45%) who received placebo. One patient receiving cyclosporine had reversible neutropenia attrib utable to sulfasalazine, and another patient receiving cyclosporine was unable to tolerate the enema vehicle. No other toxicity was noted during the trial. Blood cyclosporine levels were detectable in only two patients. Conclusions: Cyclosporine enemas administered in a dosage of 350 mg/day for 4 weeks are not efficacious in mildly to moderately active left-sided ulcerative colitis.
of Laboratory Medicine and Pathology, *Section of
toxicity
cyclosporine
treatment
C
is a cyclic endecapeptide
that has revolu-
tionized solid organ transplantation because of its unique ability to selectively inhibit cellular immunity.’ Multiple uncontrolled studies have suggested that cyclosporine administered orally or intravenously is of benefit in patients with severe ulcerative colitis who are refractory to standard therapy.2-‘7 Two controlled trials of oral or intravenous cyclosporine in patients with mildly to moderately active18 and severely activer” ulcerative colitis have confirmed these observations. Serious,
oral
and
of inflammatory
intravenous
bowel disease has
been minimal,
but there is a high incidence of cyclosporexperience with side effects.20 Furthermore,
ine-related cyclosporine
in other settings,
such as organ transplanta-
tion, has shown that serious toxicity In an attempt avoiding
to reduce
can occur.
cyclosporine
small bowel absorption,
side effects by
cyclosporine
has been
administered as an enema. We have previously reported a pharmacokinetic study showing that blood concentrations are negligible
and colonic
tissue concentrations
are
quite high after enema administration of cyclosporine.21 Four uncontrolled studies of cyclosporine enema treatment
for patients
with
left-sided
ulcerative
colitis
have
reported response rates ranging from 50% - 7 5 % .22-26 No side effects attributable to cyclosporine have been reported
after enema administration.
sults of a 4-week (350 mg/day)
controlled
in patients
We report
trial of cyclosporine
with active left-sided
the reenemas
ulcerative
colitis.
Materials Study
and Methods
Design
This study was a randomized, double-blind, placebocontrolled trial using 350 mg/day ofcyclosporine administered as an enema in patients with mildly to moderately active leftsided ulcerative colitis. Patients were assigned to 1 of 4 strata based on treatment
yclosporine
during
irreversible
no treatment, olsalazine, roids,
with
oral mesalamine),
or treatment
Patients
at the time of enrollment
treatment with
were not stratified
oral salicylates treatment
oral salicylates
with
into the study: (sulfasalatine, oral corticoste-
and corticosteroids.
for topical therapy (topical cortico-
steroids or mesalamine) because these medications were discontinued before beginning the study medication for reasons discussed within
below. To maintain a balance of treatment groups each stratum, randomization was performed separately
0 1994 by the American Gastroenterological Association 00165085/94/$3.00
GASTROENTEROLOGY Vol. 106, No. 6
1430
SANDBORN ET AL.
within
each of the four strata using a randomization
developed
sequence
in the Section of Biostatistics.
Patients From September patients
with mildly
1991 to November
to moderately
colitis were referred by colleagues
1992, 40 adult
active left-sided
ulcerative
at the Mayo Clinic for enroll-
ment into the study. Active ulcerative
colitis was diagnosed
the usual symptomatic,
and endoscopic
criteria.
disease were excluded
because
Patients
radiographic,
with newly diagnosed
we wished to study patients to standard tutional
treatment.27
Review
gave informed,
who tended
The study was approved
and/or
continued
at prestudy
been changed
during doses
studying topical
(sulfasalazine,
oral corticosteroids
corticosteroid
therapies
120
the previous >20
were
Corticosteroid at least
perrectal
medications.
During
to take metronidazole, azathioprine,
to avoid
1 week
ova and parasites,
were required
evaluations
or other investiexamination
Women
to have a negative
count,
chemistry
pregnancy
tients
with renal dysfunction >2X
a trough
whole
(serum (alkaline
normal)
nine levels were measured performance
blood
panel,
test
complete
and urinalysis.
creatinine
Pa-
> 1.5X
phosphatase
nor-
or aspartate
were excluded.
Serum creati-
after 2 weeks of treatment,
cyclospotine
concentration
liquid chromatography)
and
(by high-
was determined
Throughout
the study, patients
at the 4-
kept a daily record of
the number of their stools, any rectal bleeding,
their subjective
sense of well-being,
the degree of abdominal
discomfort,
any other symptoms
coinciding
sent adverse reactions. of
during the trial. Laboratory
screening
mal) or hepatic dysfunction aminotransferase
for
capable
at the initial and 4-week visits included
blood
Disease Activity Assessment
6-
a negative stool culture for enteric pathogens,
and asked to practice contraception
Index
Stool frequency 0, Normal number of stools for this patient 1, l-2 stools more than normal 2, 3-4 stools more than normal 3, 5 or more stools more than normal Rectal bleeding 0, No blood found 1, Streaks of blood with stool less than half the time 2, Obvious blood with stool most of the time 3, Blood alone passed Sigmoidoscopic findings 0, Normal or inactive disease 1, Mild disease (etythema, decreased vascular pattern, mild friability) 2, Moderate disease (marked erythema, absent vascular pattern, friability, erosions) 3, Severe disease (spontaneous bleeding, ulceration) Physician’s global assessment 0, Normal 1, Mild disease 2, Moderate disease 3, Severe disease
the study, patients
had a negative toxin.
Activity
before
oral cyclosporine,
methotrexate,
Clostridim difiile
and a negative conception
each patient
Disease
with retention
drugs.
Before entry,
Colitis
and mesalamine
difficulties
mercaptopurine,
were
receiving
excluded
were discontinued
were not allowed
mesala-
mg/day)
2 weeks. Patients
mg/day
the study to avoid potential
of multiple
gational
olsalazine,
(dose,
doses during the trial if the doses had not
severely ill patients.
entering
by the Insti-
and all patients
consent.
Oral salicylate compounds mine)
to be more refractory
Board of the Mayo Clinic, written
by
Table1. Ulcerative
Patients
and after 4 weeks according that
measured
findings,
stool
severe) reflected
endoscopic physical
findings,
findings
rectal
and pertinent
and performance
mesalamine
ment was determined
physician
at the 4-week visit and from patient
remission
and clinical
sigmoidoscopy. marcation
Left-sided
disease extent
between endoscopically
was defined
as a de-
inflamed and endoscopically
normal colonic mucosa located not more than 60 cm from the anal verge. If the demarcation
was at exactly 60 cm (as mea-
sured by a 60-cm flexible sigmoidoscope), normal
colonic
mucosa
the tip of the endoscope. between
endoscopically
tissue was >60 the study.
then endoscopically
had to be clearly visible Patients inflamed
in which
proximal
and endoscopically
normal
cm from the anal verge were excluded
Colonic
mucosal
biopsy
during
each endoscopy
to confirm
severity
of histological
inflammation,
Ionic tissue concentration
specimens
from
were obtained
the diagnosis, and determine
of cyclosporine.
to
the demarcation
assess the the co-
improvement
indices
such
as
criteria
and Baron et a12’
appearance, has been used
in other studies of oral mesalamine
week visit. The extent and severity of colonic mucosal involveat the initial and 4-week visits by flexible
mild,
symptoms,
ofTtuelove’s28
the degree of clinical activity
enemas.32-33 Adverse
(quiescent,
recorded
clinical
criteria for grading the sigmoidoscopic previously
endoscopic
(Table 1). The phy-
status. This disease activity
index, which was based on modifications for classifying
bleeding,
of disease activity the patient’s
at study entry
disease activity index
global assessment
sician’s global assessment moderate,
were evaluated
to a 12-point
frequency,
and physician’s
and
with therapy that might repre-
therapy3”-3’ and
events were evaluated
by a
diaries. Clinical
were defined
as a disease
activity index score of zero and a decrease in the disease activity index of at least three points, respectively. Histological disease activity was also assessed at study entry and after 4 weeks according to a four-point histological disease activity index (Table 2).22 Assessed features included the nature (polymorphonuclear vs. entirely mononuclear) and distribution (lamina propria vs. cryptal) of the inflammatory cell infiltrate as well as the degree of glandular destruction and/or ulceration. Endoscopic biopsy specimens were obtained from the site in the distal colon that appeared to have the most severe inflammatory change. The histological disease activity index score was determined by a single pathologist (K.P.B.) who was
CYCLOSPORINE ENEMAS FOR ULCERATIVE COLITIS
June 1994
Table 2. Histological
Disease
Activity Index
0, Normal (normocellular lamina propria, PMNs absent) 1, inactive chronic colitis (hypercellular lamina propria, PMNs absent) 2, Mild active chronic colitis (scant PMNs in lamina propria, occasional cryptitis but few crypt abscesses, minimal glandular destruction or ulceration) 3, Moderately active chronic colitis (moderate numbers of PMNs in lamina propria with ct-yptitis and crypt abscesses prominent, some glandular destruction) 4. Severely active chronic colitis (numerous PMNs with abundant cryptitis, crypt abscesses, extensive glandular destruction, ulceration may be prominent) PMN, polymorphonuclear
cyclosporine as previously described.‘s.2’-23 The last enema was taken approximately 15 hours before the biopsies were performed. The tissue samples from each patient were frozen at -20°C in a drop of Tissue Tek (Miles Inc., Diagnostic Division,
Elkhart,
thawed, stool,
rinsed
IN). At the time of assay, the samples were
in 0.9%
or cyclosporine
and weighed.
saline
(to remove
adherent
Cyclosporine
minutes.
any Tissue
was extracted
by placing
the tissue
and homogenizing
The samples were then assayed for cyclosporine
the same methodology
that
Tek,
to the surface of the tissue),
in 2 mL of 9:l acetonitrile/methanol
for 2 using
we use for the measurement
whole blood cyclosporine.3’-‘6 tions were expressed
leukocyte.
1431
Tissue cyclosporine
in nanograms
of
concentra-
per gram wet tissue.
Statistical Methods blinded
to patient
identification,
point
in time (entry
week), and clinical status. The slides were reviewed sitting
in a randomized
histological activity
fashion.
improvement
Histological
disease activity
remission
and
disease
in the histological
index of at least one point,
The treatment
at a single
were defined as a histological
index score of zero and a decrease
vs. 4-
respectively.
baseline
demographic
and histological
Treatment Patients
consisted
were instructed
to add 3.5 mL of blinded-study
cation to the enema vehicle and retain
retention
were recorded
Each enema vehicle was composed
(Ruger Chemical Co., Irvington, methylcellulose
(Spectrum
isoosmolar
and the carboxymethylcellulose
added
to suspend
The vehicle,
into individual
This
g of sorbitol described
Corp.,
dose of sorbitol
reported
(Sandimmune East Hanover,
oral solution;
olive oil, were each dispensed
that the cremophors
castor oil for intravenous
oxyethylated
oleic glycerides
to extract
Sandoz Phar-
NJ), and the placebo
oxyethylated potential
was dispensed
The active study medi-
in llO-mL
glass bottles. The blinded-study medications cebo) were not mixed with the vehicle until because of concern
brown
in cyclosporine concentrate
phthlate
study
(active vs. plajust before use
for the oral solution)
diethylhexyl
(poly-
and polyhave the
from the polyvinyl
chloride enema bottles into the solution. s* Compliance determined by review of the patient diaries.
was
Measurement of Colonic Tissue Cyclosporine Concentration We obtained four mucosal pinch biopsy specimens from the rectosigmoid colon during flexible sigmoidoscopy performed
at the
4-week
visit
group between
treatment
group
change
a difference,
for assay of colonic
tissue
time
in the disease tissue
was considered
activity
index
vs.
concentra-
significant. group
and 20 in
there was 75% power for de-
corresponding
group
vs.
and were used
cyclosporine
in the placebo-treated group,
change in
vs. not improved)
retention
P <0.05
20 patients
the cyclosporine-treated tecting
(improved
and colonic
tions. A two-tailed With
index
and enema
separately
to 80%
compared
improvement
in
with 40% improvement
in
test at a type I error rate
of 5%.
Results
is well
to cause a cathartic
previously,*i~**
100-mL enema bottles.
cation, cyclosporine medication,
Corp.,
the vehicle
cyclosporine.
activity
NJ), and 500 mg carboxyto make
improvement,
rank tests or extensions Logistic regression
the placebo group using a two-sided
Manufacturing
to
between
of 60 mL water, 5 g sorbitol
was added
below the 20-30
maceutical
and the
on a daily basis.
clinical
using
the cyclosporine
Chemical
CA). The sorbitol
the hydrophobic effect.
of 1 hour or overnight
The time that the enema was administered of enema
Gardena,
medi-
just before use, shake vigorously,
the enema for a minimum
if possible. duration
for 4 weeks.
characteristics,
improvement
with regard
models were used to assess the relationship treatment
of one enema nightly
were compared
of Fisher’s Exact Test for ordered categories. the disease
Cyclosporine Enema Treatment
groups
There were no significant cyclosporine
and placebo
comparisons
of demographic
severity (Table 3), initial and current or previous
groups
differences
between
the
with regard to baseline
characteristics
and disease
disease assessment (Figure l), drug therapy (Table 4). The
duration of symptoms can be classified as follows for the cyclosporineand placebo-treated patients, respectively: recent flare (< 30 days), 0 of 20 and 1 of 20; intermediate duration (30-90 days), 5 of 20 and 4 of 20; and chronically active (>90 days), 15 of 20 and 15 of 20. The median
duration
of symptoms
in the cyclosporine
and
placebo groups was 210 and 225 days, respectively (Table 3). Only six patients (two receiving cyclosporine and four receiving placebo) were not receiving concomitant oral corticosteroids and/or salicylates during the study; of these, four had topical corticosteroids or mesalamine therapy withdrawn 2 weeks before the study. Thus, the majority of patients in both groups had chronically active and refractory disease as evidenced by a long duration of
1432 SANDBORN ET AL.
Table 3. Patient
Demographic
40 Patients Treated
GASTROENTEROLOGY Vol. 106, No. 6
Data and Disease
With Left-Sided
Ulcerative
With Cyclosporine
43
Age at entry (yf) Duration of ulcerative colitis (yr) Duration of current symptoms (days) Extent of disease (cm) Initial DAI score (range, O-12) Initial HDAI score (range, O-4)
Median
Range
38
l-4
26-68 o-21
5 210 43
5-11
3 IO/IO
Sex (M/F)
Range
14-6570 lo-60
8
42-3650 12-60
8
4-10
3 13/7
l-4
NOTE. No significant differences were detected for any of these characteristics (P > 0.05). DAI. clinical disease activity index; HDAI, histological disease activity index.
symptoms
and the need
with corticosteroids The
for concomitant
and/or
rates of clinical
oral therapy
salicylates.
and
histological
improvement
after 4 weeks of therapy were not significantly between the placebo and cyclosporine groups patients
with left-sided
ema treatment the 4-week
ulcerative
was discontinued
treatment
period
and Previous
With Left-Sided
Drug Therapy
Ulcerative
colitis
in 40 Patients
Treated
With
Current drug therapy No current treatment Salicylatesa Steroids Salicylates” and steroids Recently discontinued drug therapyb Topical steroids Topical mesalamine Previous drug therapyC Oral steroids Topical steroids Sulfasalazine Olsalazine Oral mesalamine Topical mesalamine Azathioprine or 6mercaptopurine
Placebo (n = 20) (%)
Cyclosporine (n = 20) (%)
20 40 15 25
10 40 20 30
30 15
25 20
30 45 55 10 10 40
20 65 50 I.5 10 60
5
15
NOTE. No significant differences were detected acteristics (P > 0.05). “Salicylates are sulfasalazine, olsalazine, and Therapy discontinued ~~14 days before study Therapy discontinued >I4 days before study
for any of these charoral mesalamine. entry. entry.
different in these
(Table
5). En-
in nine patients
before
was completed
Colitis
Enemas
Cyclosporine (n = 20)
O-24
225 38
Table 4. Current
Cyclosporine
21-69
2
in
Enemas
Placebo (n = 20) Median
Severity Colitis
because
of
worsening symptoms requiring initiation or increase of the dose of corticosteroids and/or hospitalization. This
included
6 of 20 patients
(30%) in the cyclosporine
and 3 of 20 (15 %) in the placebo group. No association between improvement in clinical
dis-
ease activity and colonic tissue cyclosporine concentrations was detected (P > 0.15). Among patients in the cyclosporine group, there was not a significant in the colonic tissue cyclosporine concentrations with clinical
8
group
remission
and improvement
difference for those
(median,
772
ngig; range, O-5885 “g/g) and those who failed to improve (median, 0 rig/g;; range, O-5998 “gig). Similarly,
Table 5. Response
to Treatment
in 40 Patients
0
SCOW
1
2
3
Score
Figure 1. Frequency distribution of baseline scores (O-3 points) for the individual components of the disease activity index: (A) stool frequency, (6) rectal bleeding, (C) sigmoidoscopic findings, and (D) physician global assessment. There were no significant differences in the frequency distribution of scores between the placebo and cyclosporine groups for any of the categories. ?T, ?cyclosporine (n = 20).
Disease activity index Clinical remission Clinical improvement’ Clinical failure Histological disease activity index Histological remission Histological improvement’ Histological failure
With Cyclosporine
With Left-Sided
Ulcerative
Enemas Colitis
Placebo
Cyclosporine
Pa
(n = 20) 1 9 11
(n = 20) 1 8 12
0.90 0.90 0.90
(n = 18) 1 7 11
(n = 19) 1 6 13
0.77 0.77 0.77
a/=’ based on an extension of Fisher’s Exact Test for ordered categories. bClinical improvement includes clinical remission. ‘Histological improvement includes histological remission.
CYCLOSPORINE ENEMAS FOR ULCERATIVE COLITIS
June 1994
enema
retention
time
was not significantly
associated
with improvement in the disease activity index. The median enema retention time in the placebo group was 6.3 hours (range, 2.4-8.3 group ever,
hours), whereas in the cyclosporine
it was 4.1 hours (range, there
retention
1.0-12.7
was significantly
times
greater
for the cyclosporine
Two patients
receiving
verse events during
hours).
variation group
cyclosporine
Howin (log)
(P < 0.01).
experienced
ad-
the study; both received cyclosporine.
One patient had an absolute neutrophil count of 5001 mm3 after 4 weeks in the study. The patient had started taking
sulfasalazine
8 weeks before entering
Both the cyclosporine withdrawn,
enemas
the study.
and the sulfasalazine
and the neutropenia
was later rechallenged
with
absence of sulfasalazine
therapy,
resolved.
cyclosporine
were
The patient enemas
and the neutropenia
in the did
and three patients
twice daily for 4 weeks (2.5 mg/kg 0.75 mg/kg Winter
administering the cyclosporine enemas, the patient developed severe abdominal cramping and worsening diar-
et al. used cyclosporine
cyclosporine
enemas
The present trolled
(350 mg/day
randomized,
tive colitis
was designed
uncontrolled
studies
no significant
differences
between
the
of clinical
and those who were removed
breath test performed
withafter
enema administration to assess for carbohydrate intolerance to the sorbitol in the enema vehicle was negative. Except
for the
patient
with
neutropenia
described
above, none of the patients in the study had any clinically important changes in the following parameters: systolic and diastolic blood pressure, complete blood count, serum chemistry group levels (including alkaline phosphatase, aspartate aminotransferase, total bilirubin, direct bilirubin, creatinine, and urea), and urinalysis. Trough whole blood cyclosporine
concentrations
able in all but two patients receiving receiving
(56 ng/mL
were significantly
of patients
Discussion Four uncontrolled trials have reported improvement of left-sided ulcerative colitis during treatment with cyclosporine enemas. 22,24-26 Brynskov et al. used cyclosporine enemas (250 mg/day for 2 weeks) in seven patients with refractory ulcerative proctitis and one patient with an ileostomy and colitis in the blind rectal stump and reported a response of 75%.** Ranzi et al. treated three patients with refractory proctosigmoiditis
the results
extent
and
of the
improve-
placebo-treated
was actually greater in
(30%) than the placebowere no significant who completed early with
differ-
the study
regard
to the
of disease (43 cm vs. 45 cm for
colitis involving
ing colon did not result in the selection more severe disease. The rate of histological
the descend-
of patients
with
improvement
was even lower than the rate of clinical improvement, and there was not a significant difference between the two groups.
ported
is 25 ng/mL.
There
those patients
with ulcerative
in one patient
peutic level range of 100-300 ng/mL, and the value of 30 ng/mL was near the lower limit of sensitivity for our assay, which
proximal
The negative what surprising.
below the thera-
(15%).
ulcera-
the cyclosporine group and 38 cm vs. 60 cm for the placebo group). These findings suggest that the inclusion
were undetect-
cyclosporine and 30 ng/mL in another patient placebo). The blood cyclosporine concentra-
tions in these patients
median
group
placebo-con-
from the study because
symptoms group
with with
above.2’,24-26 We found
cyclosporine-
symptoms
A hydrogen
we have
in the rate of clinical
the cyclosporine-treated
for
colitis
for left-sided
to confirm
discussed
The rate of early removal
of worsening treated
ulcerative
for 4 weeks).‘*
enemas
ences between
when the enema vehicle was administered
(250 mg/day
double-blind,
trial of cyclosporine
and
of 50%.
reported a 50% response in 10 patients ulcerative colitis after treatment
rhea that lasted for 12 hours. The symptoms recurred with two rechallenges. The patient also experienced similar out cyclosporine.
enemas
rate of 58%.26 Finally,
a response
enemas
in three patients
and reported previously left-sided
ment
after
ileosmucous
with a response
with left-sided
groups.
30 minutes
in three patients)
6 weeks) in 12 patients
to the enema
Approximately
colectomy,
tomy, and colitis in a sigmoidorectal remnant fistula.*’ These patients received cyclosporine
not recur. The other adverse event seemed to be related vehicle.
with prior subtotal
1433
results of our controlled trial are someMultiple uncontrolled studies have re-
improvement
of ulcerative
colitis after treatment
with oral or intravenous cyclosporine2-” with an average response rate of 80%.20 These uncontrolled results were recently confirmed by a controlled trial of intravenous cyclosporine for severe ulcerative colitis, which reported a response of 820/o.‘” In comparison with the apparent efficacy of oral and intravenous cyclosporine for ulcerative colitis, cyclosporine enemas are not efficacious. These findings stand in contrast with other medications used to treat ulcerative colitis, such as corticosteroids and mesalamine, which are efficacious with both oral and topical administration. There are a number of potential explanations for our negative results. First, the dose of cyclosporine may have been too low or the dosing interval too infrequent. The mean oral cyclosporine dose reported to be efficacious in ulcerative colitis is 8 mg kg-’ .day-‘.I0 The cyclosporine
GASTROENTEROLOGY Vol. 106, No. 6
1434 SANDBORN ET AL.
dose
used
in
this
study
was
350
mglday
(5
mg.kg-’ .day-’ for a i’O-kg patient). However, this dose is higher than the doses used in most of the other uncontrolled trials.24-26 Second, the water-based enema vehicle that we and others used’1-26 may not provide optimal delivery of cyclosporine the treatment duration possibility
to the colonic
seems unlikely
ally reported
mucosa.
Third,
may have been too short. because cyclosporine
to act within
l-2
This
is gener-
weeks in patients
with
ulcerative colitis.*’ Fourth, the patients we selected for the study were in general refractory to standard therapy. who have not already
Patients
and salicylate cyclosporine proven
therapy
failed oral corticosteroid
may have a better
enemas than patients
to be refractory
to other medications.
tients with disease in the descending differently sigmoid
than
patients
with
colon and rectum,
disease
by cyclosporine
helper cell interleukin 2 production to stop the inflammatory reaction reported
tween colonic tissue cyclosporine tention
and a strong
time and clinical
Fifth,
pa-
confined
to the
in which case the combining
local immunosuppression
cal response
to
colon may respond
of these two groups could mask treatment
We have previously
response
who have already been
effects. Finally, of colonic
T-
may not be sufficient in ulcerative colitis. a weak association
concentration
association
between
be-
and clinienema re-
response.22 These uncontrolled
observations were not confirmed in the present controlled trial. Whether colonic tissue cyclosporine concentrations are associated
with clinical
response
in patients
treated
with oral or intravenous cyclosporine is unknown, although a preliminary report has suggested that this may be the case.‘> No toxicity clinically
directly
important
attributable
to cyclosporine
side effects were noted
during
or the
trial. Presumably, the absence of toxicity and side effects relates to the fact that the cyclosporine administered as an enema is generally not absorbed. A similar lack of toxicity during cyclosporine enema treatment has been previously reported.2’-26 In contrast, side effects occur frequently when cyclosporine is administered orally or intravenously.20 We conclude that cyclosporine enemas administered in a dose of 350 mglday for 4 weeks are not efficacious in the treatment of mildly to moderately active left-sided ulcerative colitis. Cyclosporine enemas are safe and welltolerated when administered daily for 4 weeks. Future studies should evaluate higher dosages of cyclosporine, more frequent dosing schedules, alternative enema vehicles, patients with disease extent limited to the sigmoid colon (535 cm), and patients who have not already proven refractory to other forms of therapy.
References 1. Hess AD, Tutschka PJ, Santos GW. Effect of cyclosporin A on human lymphocyte response in vitro. III. CsA inhibits the production of T lymphocyte growth factors in secondary mixed lymphocyte responses but does not inhibit the response of primed lymphocytes to TCGF. J lmmunol 1982; 128:355-359. 2. Gupta S, Keshavarzian A, Hodgson HJF. Cyclosporin in ulcerative colitis. Lancet 1984;1:1277-1278. 3. Kirschner BS, Whitington PF, Black DD, Bostwick D. Cyclosporininduced remission in severe colitis unresponsive to corticosteroid therapy (abstr). Pediatr Res 1987;21:271A. 4. Bianchi Porro G, Panza E, Petrillo M. Cyclosporin A in acute ulcerative colitis. ltal J Gastroenterol 1987; 19:40-41. 5. Shelly ED, Shelly WB. Cyclosporine therapy for pyoderma gangrenosum associated with sclerosing cholangitis and ulcerative colitis. J Am Acad Dermatol 1988; 18:1084-1088. 6. Hyams JS, Treem WR. Cyclosporine treatment of fulminant colitis. J Pediatr Gastroenterol Nutr 1989; 9:383-387. 7. Stange EF, Fleig WE, Rehklau E, Ditschuneit H. Cyclosporin A treatment in inflammatory bowel disease. Dig Dis Sci 1989; 34: 1387-1392. 8. Baker K, Jewel1 DP. Cyclosporin for the treatment of severe inflammatory bowel disease. Aliment Pharmacol Ther 1989;3: 143-149. 9. Lichtiger S, Present DH. Preliminary report: cyclosporin in treatment of severe active ulcerative colitis. Lancet 1990;336:1619. 10. Lichtiger S. Cyclosporine therapy in inflammatory bowel disease: open-label experience. Mt Sinai J Med 1990;57:315-319. 11. Bianchi Porro G, Petrillo M, Ardizzone S. Cyclosporin treatment for severe active ulcerative colitis (letter). Lancet 1990;336:439. 12. Gavaler JS, Delemos B, Belle SH, Heyl AE, Tarter RE, Starzl TE, Gavaler C, Van Thiel D. Ulcerative colitis disease activity as subjectively assessed by patient-completed questionnaires following orthotopic liver transplantation for sclerosing cholangitis. Dig Dis Sci 1991;36:321-328. 13. Shaked A, Colonna JO, Goldstein L, Busuttil RW. The interrelation between sclerosing cholangitis and ulcerative colitis in patients undergoing liver transplantation. Ann Surg 1992;215:598-603. 14. Treem WR, Davis PM, Hyams JS. Cyclosporine treatment of severe ulcerative colitis in children. J Pediatr 1991;119:994-997. 15. Sandborn WJ, Goldman DH, Lawson GM, Perrault J. Measurement of colonic tissue cyclosporine concentration in children with severe ulcerative colitis. J Pediatr Gastroenterol Nutr 1992; 15: 125-129. 16. Actis GC, Ottobrelli A, Pera A, Barletti C, Ponti V, Pinna-Pintor M, Verme G. Continuously infused cyclosporine at low dose is sufficient to avoid emergency colectomy in acute attacks of ulcerative colitis without the need for highdose steroids. J Clin Gastroenterol 1993; 17:10-13. 17. Lichtiger S, Present DH. Cyclosporin A in the treatment of severe ulcerative colitis (abstr). Gastroenterology 1992; 102:A653. 18. Sandborn WJ, Wiesner RH, Tremaine WJ, LaRusso NF. Ulcerative colitis disease activity following treatment of associated primary sclerosing cholangitis with cyclosporin. Gut 1993;34:242-246. 19. Lichtiger S, Present DH, Kornbluth A, Hanauer S. Cyclosporin A in the treatment of severe, refractory ulcerative colitis: a double blinded placebo controlled trial (abstr). Gastroenterology 1993; 104:A732. 20. Sandborn WJ, Tremaine WJ. Cyclosporine treatment of inflammatory bowel disease. Mayo Clin Proc 1992;67:981-990. 21. Sandborn WJ, Strong RM, Forland SC, Chase RE, Cutler RE. The pharmacokinetics and colonic tissue concentrations of cyclosporine after IV, oral, and enema administration. J Clin Pharmacol 1991; 31:76-80.
CYCLOSPORINE ENEMAS FOR ULCERATIVE COLITIS
June 1994
22. Sandborn WJ, Tremaine WJ, Schroeder KW, Steiner BL, Batts KP, Lawson GM. Cyclosporine enemas for treatment of treatmentresistant, mildly to moderately active, left-sided ulcerative colitis. Am J Gastroenterol 1993;88:640-645. 23. Sandborn WJ, Tremaine WJ. Cyclosporin enemas for therapy-resistant ulcerative proctitis. In: Demling L, Fruhmorgen P, eds. Non-neoplastic diseases of the anorectum. Lancaster, UK: Klewer, 1992:333-339. 24. Brynskov J, Freund L, Thomsen 00, Anderson CB, Rasmussen SN, Binder V. Treatment of refractory ulcerative colitis with cyclosporine enemas. Lancet 1989; 1:721-722. 25. Ranzi T, Campanini MC, Velio P, Quart0 di Palo F, Bianchi P. Treatment of chronic proctosigmoiditis with cyclosporin enemas (letter). Lancet 1989;2:97. 26. Winter T, Dalton HR. Merrett MN, Campbell A, Jewel1 DP. Cyclosporin A retention enemas in refractory distal colitis: an open trial (abstr). Gastroenterology 1992; 102:A947. 27. Jarnerot G, LennardJones J, Bianchi-Porro G, Brynskov J, Campieri M, Present DH. Medical treatment of refractory distal ulcerative colitis. Gastroenterol Int 1991;4:93-98. 28. Truelove SC. Treatment of ulcerative colitis with local hydrocortisone hemisuccinate sodium: a report on a controlled therapeutic trial. Br Med J 1958;2:1072-1077. 29. Baron JH, Connell AM, Lennard-Jones JE. Variation between observers in describing mucosal appearances in proctocolitis. Br Med J 1964; 1:89-92. 30. Schroeder KW, Tremaine WJ, llstrup DM. Coated oral 5aminosalicylic acid therapy for mildly to moderately active ulcerative colitis: a randomized study. N Engl J Med 1987;317:1625-1629. 31. Sninsky CA, Cart DH, Shanahan F, Powers BJ, Sessions JT, Pruitt RE, Jacobs WH, Lo SK, Targan SR, Cerda JJ, Gremillion DE, Snape
32.
33.
34.
35. 36.
1435
WJ, Sabel J, Jinch H, Swinehart JM, DeMicco MP. Oral mesalamine (Asacol) for mildly to moderately active ulcerative colitis. Ann Intern Med 1991; 115:350-355. Sutherland LR, Martin F, Greer S, Robinson M, Greenberger N, Saibil F, Martin T, Sparr J, Prokipchuk E, Borgen L. 5-aminosalicylic acid enema in the treatment of distal ulcerative colitis, proctosigmoiditis, and proctitis. Gastroenterology 1987; 92: 1894-1898. Biddle WL, Greenberger NJ, Swan JT, McPhee MS. Miner PB. 5aminosalicylic acid enemas: effective agent in maintaining remission in left-sided ulcerative colitis. Gastroenterology 1988;94: 1075-1079. Venkataramanan R, Burckart GJ, Ptachcinski RJ, Blaha R, Logue LW, Bahrson A, Choo-Seng G, Brady JE. Leaching of diethylhexyl phthalate from polyvinyl chloride bags into intravenous cyclosporine solution. Am J Hosp Pharm 1986;43:2800-2802. Moyer TP, Charlson JR, Ebnet LE. Improved chromatography of cyclosporine. Ther Drug Monit 1986;8:466-468. Moyer TP, Johnson P, Faynor SM, et al. Cyclosporine: a review of drug monitoring problems and presentation of a simple, accurate liquid chromatographic procedure that solves these problems. Clin Biochem 1986; 19:83-89.
Received May 21, 1993. Accepted November 30, 1993. Address requests for reprints to: William 1. Sandborn, M.D., Mayo Clinic, 200 First Street S.W., Rochester, Minnesota 55905. Fax: (507) 284-0538. Supported by a grant from Sandoz Pharmaceutical Corporation. Presented at the annual meeting of the American Gastroenterological Association in Boston, Massachusetts, May 17-19, 1993.