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Magnesium metabolism in Huntington's chorea
Magnesium Metabolism in Huntington’s Chorea By JOHN
C. DESPER AND EDMUND B. FLINK
E. JONES, PAUL
Human magnesium deficiency states are known to be associated with tremor, choreiform and athetoid movements, delirium and convulsions. In order to assess a recent report of altered magnesium in Huntington’s metabolism chorea, 6 patients with the disease have been studied with complete balance studies, exchangeable magnesium studies, erythrocyte and ultrafiltrable magnesiums and 2 patients with spinal fluid magnesium determinations. Balance
S
referrable
YMPTOMS felderl
in a group
early report
without most Hanna
tremor,
has been
frequently
sorption,
choreiform
following losses
al.6 have
with
Since
hypomagnesemia
and athetoid
movements,
prolonged
of disorders. inadequate
gastric
the
by Hirsch-
glomerulonephritis.
and Flink,3j4
in a variety
through
reviewed
were first recognized
chronic
of Miller2
reported
seen
or excess et
to hypomagnesemia of patients
and the reports
associated
convulsions,
studies failed to suggest any abnormalities. Exchangeable magnesium28 values were within normal ranges (4.3 +- 0.7 mEq./Kg. at 24 hrs.), as were erythrocyte magnesium determinations (5.29 C 0.42 mEq./L.). Ultrafiltrable magnesiums were normal and the 2 spinal fluids evaluated had normal magnesium values. These results are not compatible with the hypothesis of altered magnesium metabolism in Huntington’s chorea.
suction
various
this
with or
delirium
and
Hypomagnesemia
is
dietary
intake,
or diarrhea.
malab-
Smith5
clinical
manifestations
finding
significant
and
of hypo-
magnesemia. In
1963,
erythrocyte of these
cations
our chance show status From
Kenyon
and
magnesium
in a group
observations
any evident
reported
of
Morgantown, West Virginia. These studies were carried 05578-AMP) and supported Received for publication EditoriaE Comment: The
abnormality,
in Huntington’s
Medicine, out
with Huntington’s
with this disease
magnesium
in
West our
elevations
in the face of normal
of 20 individuals
metabolism
Department
levels
on one patient
erythrocyte
of magnesium the
Hardy7
and calcium
Virginia
Clinical
seemed
of
(USPHS
can be made
While to
of the
worthwhile.
School
Unit
of
levels
failed
an assessment
University,
Research
chorea.
had earlier
chorea
by VSPHS Grant NB 03152. Jan. 22, 1965. diagnosis of Huntington’s chorea
serum
Medicine, Grant
with
AM
certainty
only when the family history is positive. The choreiform movements differ in no essential detail from chorea caused by other factors, the abnormal movements depending on the site of the lesion and not the pathologic process underlying it. The search for evidence of a metabolic defect in Huntington’s
chorea
has been
long
and relatively fruitless. Kenyon and Harvey (1963) estimated the serum and erythrocyte magnesium and calcium levels in a group of 20 patients with adult chorea. In 4 of those patients, the family history was negative, in 2 it was unknown, in the remaining 14 the family history was apparently typical of Huntington’s chorea. An elevation of erythrocyte magnesium levels was found in some patients with chorea, which on statistical evaluation was just short of the 5 per cent level of significance. The serum magnesium was normal. There was also a tendency for patients without famiIy history to show an over-all higher 813 METABOLISM,
VOL.
14, No. 7 (JULY ), 1965
814
JONES,
DESPER AND FLINK
The results of complete balance studies, exchangeable magnesium determinations, serum and erythrocyte magnesium levels and ultrafiltrable magnesiums in 6 patients with Huntington’s chorea are presented. METHODS Patients:
Five
females
ranging
in age
from
34 to 60 and
on our Clinical Research Unit. All had family histories more generations. All had classical associated neurologic had least ambulatory as part
impairment and had of their
spinal fluid. ~&oratory mission.
of the group normal clinical
neurologic
Methods:
Constant
as would laboratory
evaluations All patients
diets
were
and had
started
male
age
magnesium
been
eating
determinations adequate
of 3 days
determinations. studied. Stools
ad prior
30 were
known for The male
he expected from his age. results. Two of the 6 had
a minimum
balance data or exchangeable magnesium over 8 to 14 days in 5 of the 6 patients
one
of involvement manifestations.
lib
two or patient
All patients were lumbar punctures we’re
to
studied
diets any
done
on thr
prior
to ad-
collections
Balance observations were collected in new
were gallon
for made paint
cans and homogenized by the method of Newell.8 Aliquots of the balance diets were homogenized and individually analyzed. Standard Kjeldahl digestion technics were employed in the processing of both diets and stool. Standard flame photometric determinations of sodium and potassium were done. Magnesium and calcium determinations were done on a Zeiss flame photometer by the method packed
of Mac1ntyre.a Erythrocyte cells by a modification of
a modification
of
the
method
of
magnesium the above Fiske
and
determinations were done on washed, technic. Phosphorus was determined by Subbarow,r” and nitrogen determined by
the method of Ferrari.11 Urine creatinines were done on a Technicon Autoanalyzer. Ultrafiltrable magnesium determinations were made by the method of Prasad and Flink.12 Magnesiumax
was
obtained
preparation, the isotope stool obtained. Gamma
from
was given counting
Brookhaven intravenously was done
National
Lahoratories.
and timed samples in a well scintillation
After of plasma, counter
appropriate urine, and employing
shows the results in 15 cases. In erythrocyte magnesimlr content. Table 2 of their paper 4 instances, the magnesium was markedly increased in the red cells (11.4, 19.1, 20.8 and 25.0 mEq./L.). Two of these patients had a negative family history, and one the family the family history is said to have been history was unknown, and in a further patient, positive. The only other patient without family history had a magnesium erythrocyte level of 2.5 mEq. which is the lowest result in the table. These results suggest that in these patients the magnesiunr metabolism may he abnormal and play a role in the etiology of their chorea. Jones et al. (1964) in a careful stucly of magnesium metabolism in 6 patients with chorea and a positive family history, found no evidence nesium metabolism. The conclusion that their results are not esis that Huntington’s chorea is caused by. or accompanied nesium
of any abnormality of magcompatible with the hypothby, a disturbance of mag-
metabolism, is the only possible interpretation of their work. mrrst he clearly recognized other than the hereditary type “adult chorea” Chronic and Harvey that patients diag(Bell, 1934). It appears likely, as suggested by Kenyon nosed as Huntington’s chorea are not a biochemically homogeneous group, and further studies of magnesium metabolism with particular emphasis on those patients without positive family histories may be rewarding. vol. 4. Cambridge University Huntington’s chorea. In Treasury of Human Inheritance. Press, 1934, p. 67. Kenyon, F. E., and Hardy, S. M.: A biochemical study of Huntington’s chorea. J. Neurol., Neurosurg. & Psychiat. 26123, 1963. E. B. Magnesimn metabolism in Huntington’s Jones, J. E., Desper, P. C., and Flink, Chorea.
Metabolism
14:000,
1965.
MAGNESIUM
METABOLISM
IN HUNTINGTON’S
815
CHOREA
mEq* 0 IO
0
20
0
20
Fig. L-Magnesium balances in 5 patients VaIues below the zero line represent positive balance, The scale is identical throughout.
chorea. with Huntington’s those above negative balance.
thallium activated sodium iodide crystal detector. Calculations magesiums (Mg2,8) were done with the following formulas:
a
Mgas Total =
PC. Mgas injected
E
specific activity Mg:
mEq./Kg.
=
for exchangeable
- ~c. Mg2s excreted to 24 hours (@mEq. ) of spot 24 hour urine Mgzs Total E
Weight
in Kg.
816
JONES,DESPERANDFLINK
Sodium
Potassium
Calcium
Nitrogen
Fig. 2 .-Balance data in patient P. S. are typical for the group. the zero line represent positive balance, those above negative balance.
Values below
RESULTS
The
results
of the magnesium and Wells’”
balances
Albright
from normal
was noted in any of the 5 patients.
in only one of the 5 during in sodium Typical
balance
balance
were noted
short-term
during
data for sodium,
are shown for patient Multiple
these
in figure
are presented by the methods of 1. As can be seen, no deviation
Reifenstein,
Calcium
balances,
balance and minor
the first few days balance
potassium,
calcium,
phosphorus
was attained fluctuations in 3 of the 5. and nitrogen
P. S. in figure 2.
determinations
were made of serum,
erythrocyte,
and ultrafiltrable
MAGNESIUM
METABOLISM
IN HUNTINGTON’S
817
CHOREA
TabIe 1 Patient and Age
Range of Range of Ultrafiltrahle Serum Magnesiums Magneaiums mEq./L.* mEq./L.*
Range of Elythrocyte Msgnesiums mEi&/L.*
Exchangeable bi;iq;; at 24 hours
Spinal Fluid Magnesium mEq./L.
4.3 *
2.4 + 0.14
Normal 1.86 z!I 0.14
values
1.18 r+ 0.1
5.29 -+ 0.42
0.7
N. W., 34 H. E., 51 D. M., 37 P. s. 60
1.8-2.0 1.6-2.05 1.9-2.0 1.8-2.0
1.15-1.3 -
5.2-5.5 4.9-5.3 4.8-5.7 4.9-5.0
4.4 3.6 4.6 3.8
2.56 -
M. L., 43
1.7-1.85
1.17-1.3
4.8-5.7
5.4
-
1.7-2.0
1.19-1.3
4.8-5.1
3.8
2.35
D. S., 30 (male) ‘Ranges
represent
magnesiums magnesiums (table 1).
a minimum of 6 determinations
per category.
in each patient and were entirely normal (table 1). Spinal fluid in the 2 patients who had lumbar punctures were normal
DISCUSSION
Our balance studies were designed primarily to test magnesium handling and were terminated in each case after normal magnesium balance was evident. The failure to develop calcium balance during short-term studies such as these is expected. Further, varying degrees of neurologic impairment and dementia made a standard level of activity impossible. Aside from minor fluctuations in sodium balances during the first few days in 3 of the 5 patients, the remaining balance data were entirely within normal limits. Exchangeable magnesiums in these patients fell within our normal ranges with the exception of minimal, unimpressive elevation in patient M. L. (table 1). MacIntyre et a1.,14 quoting the unpublished observations of Caesar and coworkers, and Petersen,l” found normal 24 hour values for exchangeable magnesium in the range of 4.5 mEq./Kg. This is also the same general order of values pubhshed by Silver et al. lo The availability of high specific activity Mgzs affords a means of attempting to assess body magnesium pools, but its short half-life (21.3 hours) virtually insures the inability to determine total body magnesium levels. Certainly, equilibrium between bone, soft tissue, and extracellular space has not occurred at 24 hours. Our limited observations in other patients do not suggest the attainment of equilibrium by 48 hours. Nonetheless, it appears meaningful that patients with Huntington’s chorea have values within normal ranges at 24 hours. As can be seen in table 1, we were unable to find any evident abnormalities in erythrocyte, serum or uhrafiltrable magnesiums. While the patients of Kenyon and Hardy7 tended to have been both older and to have had the disease longer, 2 of our patients were over age 50 and had values within the same ranges as our younger patients. It does not appear likely that the age of patients or duration of symptoms explain the differences in results.
818
JONES, DESPER AND FLINK
REFERENCES 1. Hirschfelder,
A. D.:
Clinical
manifesta-
tions of high and low plasma magnesium: Dangers of epsom salt purgation in nephritis. J. A. M. A. 102: 1138, 1934. 2. Miller, J. F.: Tetany of magnesium. 67: 117, 1944. 3. Flink,
due
Amer.
to deficiency J. Dis
Child.
McCollister, R., Prasad, A. S., Melby, J. C.. and Doe, R. P.: Evidences clinical magnesium deficiency. for Ann. Int. Med. 47:956. 1957. W.
O.,
Hammarsten,
Eliel, L. P.: of magnesium 174: 159, 6. Hanna, and
J. F.,
M.. of
magnesium deficiency in man. Lancet 2: 172, 1960. 7. Kenyon. F. E., and Hardy, S. M.: A biochemical study of Huntington’s chorea. J. Neurol. Neurosurg. Psychiat. 26: 123, 1963. 8. Newell. J. E.: Quantitative chemical assay
of feces,
sampling.
collecting,
Techn.
Bull.
mixing, Regist.
and Med.
Y.: The of phos-
digestion
4nn.
and
N. Y. Acad.
1925. by
analysis
Sci. 87:792,
1960. 12. Prasad. A. S., and Flink. E. 13.: Effect of carbon dioxide on concentration of calcium in an ultrafiltrate of serum obtained Psysiol.
by centrifugation. 10: 103. 1957.
J.
Appl.
13. Reifrnstein, E:. C., Jr.. Albright, F., and Wells. S. L.: The accumulation, interpretation and presentation of data pertaining
to
notably those and nitrogen.
The clinical expression deficiency. J. A. h4. A.
S., MacIntyre, I., Harrison, Fraser, R.: The syndrome
continuous
system.
and
1960.
and Subbarow, determination
Adv.
phorus. J. Biol. Chem. 66:375. 11. Ferrari. A.: Nitrogen determination
F. L., Anderson,
parenteral fluid administration and after chronic alcoholism complicated by delirium tremens. J. Lab. Clin. Med. 43:169, 1954.
5. Smith,
10. Fiske. C. H., calorimetric
a
E. B., Stutzman,
A. R., Konig. T., and Fraser, R.: Magnesium deficiency after prolonged
4. -,
Techn. 30: 125, 1960. 9. MacIntyre, I.: Flame photometry. Clin. Chem. 4:1, 1961.
367,
metabolic
balances.
of calcium. phosphorus. J. Clin. Endocrinol. 5:
1945.
14. MacIntyre. I., Hanna. S.. Booth, C. C.. and Read. A. E.: Intracellular magnesium deficiency in man. Clin. Sci. lij.
20:297, Petersen, nesimli ficiency.
1961. V. I’.: Potassium and turnover in magnesium Acta Med. Scandinav.
595, 1963. 16. Silver. I,.. Robertson. I,. K: Magnesium human Invest.
studied 39:420,
J. S.. and Dahl, turnover in the
with 1960.
Mgs*.
John E. Jones, M.D., Assistant Professor of Medicine, Dept. of Medicine, West Virginia University, School of Medicine, Morgantown, W. Va. Paul C. Desyer, M.D., Trainee of the USPHS (5Tl-AM-538143). Edmund B. Flink, M.D., Professor ,of Medicine, Medicine, West Virginia University, School of Morgantown, W. Va.
magde174:
Dept. of Medicine,
J.
Clin.
C. DESPER AND EDMUND B. FLINK
E. JONES, PAUL
Human magnesium deficiency states are known to be associated with tremor, choreiform and athetoid movements, delirium and convulsions. In order to assess a recent report of altered magnesium in Huntington’s metabolism chorea, 6 patients with the disease have been studied with complete balance studies, exchangeable magnesium studies, erythrocyte and ultrafiltrable magnesiums and 2 patients with spinal fluid magnesium determinations. Balance
S
referrable
YMPTOMS felderl
in a group
early report
without most Hanna
tremor,
has been
frequently
sorption,
choreiform
following losses
al.6 have
with
Since
hypomagnesemia
and athetoid
movements,
prolonged
of disorders. inadequate
gastric
the
by Hirsch-
glomerulonephritis.
and Flink,3j4
in a variety
through
reviewed
were first recognized
chronic
of Miller2
reported
seen
or excess et
to hypomagnesemia of patients
and the reports
associated
convulsions,
studies failed to suggest any abnormalities. Exchangeable magnesium28 values were within normal ranges (4.3 +- 0.7 mEq./Kg. at 24 hrs.), as were erythrocyte magnesium determinations (5.29 C 0.42 mEq./L.). Ultrafiltrable magnesiums were normal and the 2 spinal fluids evaluated had normal magnesium values. These results are not compatible with the hypothesis of altered magnesium metabolism in Huntington’s chorea.
suction
various
this
with or
delirium
and
Hypomagnesemia
is
dietary
intake,
or diarrhea.
malab-
Smith5
clinical
manifestations
finding
significant
and
of hypo-
magnesemia. In
1963,
erythrocyte of these
cations
our chance show status From
Kenyon
and
magnesium
in a group
observations
any evident
reported
of
Morgantown, West Virginia. These studies were carried 05578-AMP) and supported Received for publication EditoriaE Comment: The
abnormality,
in Huntington’s
Medicine, out
with Huntington’s
with this disease
magnesium
in
West our
elevations
in the face of normal
of 20 individuals
metabolism
Department
levels
on one patient
erythrocyte
of magnesium the
Hardy7
and calcium
Virginia
Clinical
seemed
of
(USPHS
can be made
While to
of the
worthwhile.
School
Unit
of
levels
failed
an assessment
University,
Research
chorea.
had earlier
chorea
by VSPHS Grant NB 03152. Jan. 22, 1965. diagnosis of Huntington’s chorea
serum
Medicine, Grant
with
AM
certainty
only when the family history is positive. The choreiform movements differ in no essential detail from chorea caused by other factors, the abnormal movements depending on the site of the lesion and not the pathologic process underlying it. The search for evidence of a metabolic defect in Huntington’s
chorea
has been
long
and relatively fruitless. Kenyon and Harvey (1963) estimated the serum and erythrocyte magnesium and calcium levels in a group of 20 patients with adult chorea. In 4 of those patients, the family history was negative, in 2 it was unknown, in the remaining 14 the family history was apparently typical of Huntington’s chorea. An elevation of erythrocyte magnesium levels was found in some patients with chorea, which on statistical evaluation was just short of the 5 per cent level of significance. The serum magnesium was normal. There was also a tendency for patients without famiIy history to show an over-all higher 813 METABOLISM,
VOL.
14, No. 7 (JULY ), 1965
814
JONES,
DESPER AND FLINK
The results of complete balance studies, exchangeable magnesium determinations, serum and erythrocyte magnesium levels and ultrafiltrable magnesiums in 6 patients with Huntington’s chorea are presented. METHODS Patients:
Five
females
ranging
in age
from
34 to 60 and
on our Clinical Research Unit. All had family histories more generations. All had classical associated neurologic had least ambulatory as part
impairment and had of their
spinal fluid. ~&oratory mission.
of the group normal clinical
neurologic
Methods:
Constant
as would laboratory
evaluations All patients
diets
were
and had
started
male
age
magnesium
been
eating
determinations adequate
of 3 days
determinations. studied. Stools
ad prior
30 were
known for The male
he expected from his age. results. Two of the 6 had
a minimum
balance data or exchangeable magnesium over 8 to 14 days in 5 of the 6 patients
one
of involvement manifestations.
lib
two or patient
All patients were lumbar punctures we’re
to
studied
diets any
done
on thr
prior
to ad-
collections
Balance observations were collected in new
were gallon
for made paint
cans and homogenized by the method of Newell.8 Aliquots of the balance diets were homogenized and individually analyzed. Standard Kjeldahl digestion technics were employed in the processing of both diets and stool. Standard flame photometric determinations of sodium and potassium were done. Magnesium and calcium determinations were done on a Zeiss flame photometer by the method packed
of Mac1ntyre.a Erythrocyte cells by a modification of
a modification
of
the
method
of
magnesium the above Fiske
and
determinations were done on washed, technic. Phosphorus was determined by Subbarow,r” and nitrogen determined by
the method of Ferrari.11 Urine creatinines were done on a Technicon Autoanalyzer. Ultrafiltrable magnesium determinations were made by the method of Prasad and Flink.12 Magnesiumax
was
obtained
preparation, the isotope stool obtained. Gamma
from
was given counting
Brookhaven intravenously was done
National
Lahoratories.
and timed samples in a well scintillation
After of plasma, counter
appropriate urine, and employing
shows the results in 15 cases. In erythrocyte magnesimlr content. Table 2 of their paper 4 instances, the magnesium was markedly increased in the red cells (11.4, 19.1, 20.8 and 25.0 mEq./L.). Two of these patients had a negative family history, and one the family the family history is said to have been history was unknown, and in a further patient, positive. The only other patient without family history had a magnesium erythrocyte level of 2.5 mEq. which is the lowest result in the table. These results suggest that in these patients the magnesiunr metabolism may he abnormal and play a role in the etiology of their chorea. Jones et al. (1964) in a careful stucly of magnesium metabolism in 6 patients with chorea and a positive family history, found no evidence nesium metabolism. The conclusion that their results are not esis that Huntington’s chorea is caused by. or accompanied nesium
of any abnormality of magcompatible with the hypothby, a disturbance of mag-
metabolism, is the only possible interpretation of their work. mrrst he clearly recognized other than the hereditary type “adult chorea” Chronic and Harvey that patients diag(Bell, 1934). It appears likely, as suggested by Kenyon nosed as Huntington’s chorea are not a biochemically homogeneous group, and further studies of magnesium metabolism with particular emphasis on those patients without positive family histories may be rewarding. vol. 4. Cambridge University Huntington’s chorea. In Treasury of Human Inheritance. Press, 1934, p. 67. Kenyon, F. E., and Hardy, S. M.: A biochemical study of Huntington’s chorea. J. Neurol., Neurosurg. & Psychiat. 26123, 1963. E. B. Magnesimn metabolism in Huntington’s Jones, J. E., Desper, P. C., and Flink, Chorea.
Metabolism
14:000,
1965.
MAGNESIUM
METABOLISM
IN HUNTINGTON’S
815
CHOREA
mEq* 0 IO
0
20
0
20
Fig. L-Magnesium balances in 5 patients VaIues below the zero line represent positive balance, The scale is identical throughout.
chorea. with Huntington’s those above negative balance.
thallium activated sodium iodide crystal detector. Calculations magesiums (Mg2,8) were done with the following formulas:
a
Mgas Total =
PC. Mgas injected
E
specific activity Mg:
mEq./Kg.
=
for exchangeable
- ~c. Mg2s excreted to 24 hours (@mEq. ) of spot 24 hour urine Mgzs Total E
Weight
in Kg.
816
JONES,DESPERANDFLINK
Sodium
Potassium
Calcium
Nitrogen
Fig. 2 .-Balance data in patient P. S. are typical for the group. the zero line represent positive balance, those above negative balance.
Values below
RESULTS
The
results
of the magnesium and Wells’”
balances
Albright
from normal
was noted in any of the 5 patients.
in only one of the 5 during in sodium Typical
balance
balance
were noted
short-term
during
data for sodium,
are shown for patient Multiple
these
in figure
are presented by the methods of 1. As can be seen, no deviation
Reifenstein,
Calcium
balances,
balance and minor
the first few days balance
potassium,
calcium,
phosphorus
was attained fluctuations in 3 of the 5. and nitrogen
P. S. in figure 2.
determinations
were made of serum,
erythrocyte,
and ultrafiltrable
MAGNESIUM
METABOLISM
IN HUNTINGTON’S
817
CHOREA
TabIe 1 Patient and Age
Range of Range of Ultrafiltrahle Serum Magnesiums Magneaiums mEq./L.* mEq./L.*
Range of Elythrocyte Msgnesiums mEi&/L.*
Exchangeable bi;iq;; at 24 hours
Spinal Fluid Magnesium mEq./L.
4.3 *
2.4 + 0.14
Normal 1.86 z!I 0.14
values
1.18 r+ 0.1
5.29 -+ 0.42
0.7
N. W., 34 H. E., 51 D. M., 37 P. s. 60
1.8-2.0 1.6-2.05 1.9-2.0 1.8-2.0
1.15-1.3 -
5.2-5.5 4.9-5.3 4.8-5.7 4.9-5.0
4.4 3.6 4.6 3.8
2.56 -
M. L., 43
1.7-1.85
1.17-1.3
4.8-5.7
5.4
-
1.7-2.0
1.19-1.3
4.8-5.1
3.8
2.35
D. S., 30 (male) ‘Ranges
represent
magnesiums magnesiums (table 1).
a minimum of 6 determinations
per category.
in each patient and were entirely normal (table 1). Spinal fluid in the 2 patients who had lumbar punctures were normal
DISCUSSION
Our balance studies were designed primarily to test magnesium handling and were terminated in each case after normal magnesium balance was evident. The failure to develop calcium balance during short-term studies such as these is expected. Further, varying degrees of neurologic impairment and dementia made a standard level of activity impossible. Aside from minor fluctuations in sodium balances during the first few days in 3 of the 5 patients, the remaining balance data were entirely within normal limits. Exchangeable magnesiums in these patients fell within our normal ranges with the exception of minimal, unimpressive elevation in patient M. L. (table 1). MacIntyre et a1.,14 quoting the unpublished observations of Caesar and coworkers, and Petersen,l” found normal 24 hour values for exchangeable magnesium in the range of 4.5 mEq./Kg. This is also the same general order of values pubhshed by Silver et al. lo The availability of high specific activity Mgzs affords a means of attempting to assess body magnesium pools, but its short half-life (21.3 hours) virtually insures the inability to determine total body magnesium levels. Certainly, equilibrium between bone, soft tissue, and extracellular space has not occurred at 24 hours. Our limited observations in other patients do not suggest the attainment of equilibrium by 48 hours. Nonetheless, it appears meaningful that patients with Huntington’s chorea have values within normal ranges at 24 hours. As can be seen in table 1, we were unable to find any evident abnormalities in erythrocyte, serum or uhrafiltrable magnesiums. While the patients of Kenyon and Hardy7 tended to have been both older and to have had the disease longer, 2 of our patients were over age 50 and had values within the same ranges as our younger patients. It does not appear likely that the age of patients or duration of symptoms explain the differences in results.
818
JONES, DESPER AND FLINK
REFERENCES 1. Hirschfelder,
A. D.:
Clinical
manifesta-
tions of high and low plasma magnesium: Dangers of epsom salt purgation in nephritis. J. A. M. A. 102: 1138, 1934. 2. Miller, J. F.: Tetany of magnesium. 67: 117, 1944. 3. Flink,
due
Amer.
to deficiency J. Dis
Child.
McCollister, R., Prasad, A. S., Melby, J. C.. and Doe, R. P.: Evidences clinical magnesium deficiency. for Ann. Int. Med. 47:956. 1957. W.
O.,
Hammarsten,
Eliel, L. P.: of magnesium 174: 159, 6. Hanna, and
J. F.,
M.. of
magnesium deficiency in man. Lancet 2: 172, 1960. 7. Kenyon. F. E., and Hardy, S. M.: A biochemical study of Huntington’s chorea. J. Neurol. Neurosurg. Psychiat. 26: 123, 1963. 8. Newell. J. E.: Quantitative chemical assay
of feces,
sampling.
collecting,
Techn.
Bull.
mixing, Regist.
and Med.
Y.: The of phos-
digestion
4nn.
and
N. Y. Acad.
1925. by
analysis
Sci. 87:792,
1960. 12. Prasad. A. S., and Flink. E. 13.: Effect of carbon dioxide on concentration of calcium in an ultrafiltrate of serum obtained Psysiol.
by centrifugation. 10: 103. 1957.
J.
Appl.
13. Reifrnstein, E:. C., Jr.. Albright, F., and Wells. S. L.: The accumulation, interpretation and presentation of data pertaining
to
notably those and nitrogen.
The clinical expression deficiency. J. A. h4. A.
S., MacIntyre, I., Harrison, Fraser, R.: The syndrome
continuous
system.
and
1960.
and Subbarow, determination
Adv.
phorus. J. Biol. Chem. 66:375. 11. Ferrari. A.: Nitrogen determination
F. L., Anderson,
parenteral fluid administration and after chronic alcoholism complicated by delirium tremens. J. Lab. Clin. Med. 43:169, 1954.
5. Smith,
10. Fiske. C. H., calorimetric
a
E. B., Stutzman,
A. R., Konig. T., and Fraser, R.: Magnesium deficiency after prolonged
4. -,
Techn. 30: 125, 1960. 9. MacIntyre, I.: Flame photometry. Clin. Chem. 4:1, 1961.
367,
metabolic
balances.
of calcium. phosphorus. J. Clin. Endocrinol. 5:
1945.
14. MacIntyre. I., Hanna. S.. Booth, C. C.. and Read. A. E.: Intracellular magnesium deficiency in man. Clin. Sci. lij.
20:297, Petersen, nesimli ficiency.
1961. V. I’.: Potassium and turnover in magnesium Acta Med. Scandinav.
595, 1963. 16. Silver. I,.. Robertson. I,. K: Magnesium human Invest.
studied 39:420,
J. S.. and Dahl, turnover in the
with 1960.
Mgs*.
John E. Jones, M.D., Assistant Professor of Medicine, Dept. of Medicine, West Virginia University, School of Medicine, Morgantown, W. Va. Paul C. Desyer, M.D., Trainee of the USPHS (5Tl-AM-538143). Edmund B. Flink, M.D., Professor ,of Medicine, Medicine, West Virginia University, School of Morgantown, W. Va.
magde174:
Dept. of Medicine,
J.
Clin.