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Restoring effect of oral supplementation of zinc and arginine on thymic endocrine activity and peripheral immune functions in aged mice
Arch. Gerontol. Geriatr. suppl. 3 (1992)267-276 9 1992 Elsevier Science Publishers B.V. All rights reserved. 0167-4932/92/$05.00
267
RESTORING EFFECT OF ORAL SUPPLEMENTATION OF ZINC AND ARGININE ON THYMIC ENDOCRINE ACTIVITY AND PERIPHERAL IMMUNE FUNCTIONS IN AGED MICE
E~ MOCCHEGIANI, M. MUZZlOLI, L. SANTARELLI and N. FABRIS a Immunological Center, Gerontological Research Department, Institute of National Research Centers on Aging (INRCA), Via Birarelli, 8, 1-60121 Ancona, Italy, and Chair of Immunology, University of Pavia, Piazza Botta, 10, 1-27100 Pavia, Italy SUMMARY Previous work from this laboratory has demonstrated that both a trace element, zinc, and an amino acid, arginine, are capable, when orally administered, to recover some age-related immune dysfunctions. In the present paper the effectiveness of a zinc-arginine combination versus the single nutrients in restoring age-related immunological alterations in old Balb/c mice has been investigated. The zinc-arginine combination is more effective than the treatments of single nutrients alone, in particular on the reactivation of thymic endocrine activity, as measured by the circulating level of one of the best known thymic factors, i.e. thymulin (Zn-FTS) and the natural killer (NK) cell activ i t y , particularly under boosting condition by interleukin-2 (IL-2) or interferon (IFN). On the other parameters tested the zinc-arginine combination either was not more effective than the single nutrients or a prevalence of one of them was detectable, such as of arginine on mitogen response or of zinc on basal NK act i v t i y . The findings clearly suggest that nutritional interventions and particularly combination of nutrients may represent an interesting and side-effect deprived approach for immunorestoration in elderly people. Keywords: Zinc, arginine, aging, thymulin immune function
INTRODUCTION The frequent association between malnutrition,
infective diseases and aging
has provoked a good body of experimental and clinical studies, aimed to analyze either the effect of single nutrients on the immunological in immunological
aging (Chandra,
efficiency or their role
1985, 1989). While the number of single nut-
rients relevant of immune efficiency is somewhat consistent, ranging from traceelements
(Underwood,
(Daly et al., immunological
1977) to vitamins
(Bendich,
1988) and to amino acids
1990), the studies directed to investigate their possible role in aging have remained untill now fragmentary.
Nevertheless, it has been demonstrated that a trace element, zinc and an amino acid, arginine, may exert a restorative effect of some age-related immunological alterations.
In particular,
zinc has been found capable to restore cuta-
neous hypersensitivity reactions and responses to tetanus texoid vaccination in healthy elderly (Duchateau et al., in elderly patients suffering
1981), to recover thymic endocrine function
from uremia" or hyperprolactinemia
(Travaglini et
al., 1989) and to correct both thymic function and peripheral immune efficiency
268 in subjects suffering from Down's syndrome (Franceschi et al., 1988), which is considered an early aging syndrome.
These human findings
have got f u r t h e r
support by experimental studies showing that zinc supplementation
in old mice
can recover thymic structure and function and increase mitogen responsiveness of spleen cells (Fabris et al., 1990). One of the mechanisms of zinc action has been identified in the capacity of this trace element to confer biological activity to one of the best known thymic factor,
i.e.
thymulin [ Z n - F T S ) ,
the zinc-unbound
(FTS) form of which is not
only biologically inactive but competes with the active form for the binding to the specific target (Dardenne et al., 1982; Fabris et al., 1984). The relevance of arginine for the efficiency of the immune system has been hypothesized by the observation that supplementary dietary arginine in youngadult injured rats can accelerate wound healing and prevent post-traumatic atrophy of the thymus (Barbul et al., 1983). A possible role for arginine
in
immunological
aging
has been suggested
because arginine has a secretagogue action on growth hormone (GH, al.,
Penny et
1970) and that GH is capable to modulating thymic endocrine activity and
various immune functions during development and aging (Fabris et a l . ,
1988).
It has been,
in old
in fact,
demonstrated
that oral arginine supplementation
mice causes a complete recovery of the reduced thymic endocrine activity with an improvement of peripheral immune efficiency, such as T-cell subsets, mitogen responses and NK activity [Fabris et al.,
1986b). Arginine supplementation has
been found effective in increasing thymic endocrine activity and percentage of peripheral giani,
blood T-helper
(CD4) cells in healthy elderly
1991) and in neoplastic patients
[Fabris and Mocche-
[Mocchegiani et al.,
and arginine seem to act on similar targets,
1990).
Since zinc
the question arose, whether the
combination of zinc and arginine supplementation might be more effective than the administration of the single nutrient alone. With these premises, zinc-sulphate
(Zn) and L-arginine
(Arg)
orally administered to aged mice either alone or in combination
have been
(Zn-Arg)
and
their effect on immune system evaluated in terms of thymic endocrine efficiency, peripheral T-mitogen response and NK activity. MATERIALS AND METHODS Animals. Young male (2 months) and old male (24 months) Balblc mice from our own colony were used. In both age groups mice were treated for 30 consecutive days either with arginine alone (added to the drinking water in a concentration assuring a total daily intake of 9 x 10-4 g/day/mouse, if we assume a water consumption of 5 mlldaylmouse), or with zinc sulphate alone (at the dose of 5 ]Jgldaylmouse), or with zinc-arginine combination at the same doses.
269 Thymulin T-
and
(Zn-FTS) determination.
B-lymphocytes
carry
Spleen cells from young mice including
receptors
for
sheep erythrocytes
(SRBC)
and,
therefore, form rosettes (RFC) when mixed with SRBC. T - and B-rosettes can be discriminated
by
adding
10 ug/ml
azathioprine,
which
selectively
inhibits
T-rosette formation. The azathioprine sensitivity of T-cells is strictly dependent on the thymic endocrine function: plete
disappearance
spleen
cells
(Zn-FTS).
from
of
the
in biological
fluids
azathioprine-sensitivity
thymectomized
This phenomenon
removal of the thymus in mice induces commice
are
while
incubated
it
with
reappears purified
when
thymulin
represents the basis for the bioassay of thymulin
(Bach et al.,
1975).
The bioassay is still
required
since
questions have been raised over the specificity of the radioimmunoassay developed till
now.
The maximum dilution
of plasma samples inducing
azathioprine
sensitivity in 50 % of RCFs from thymectomized mice was taken as the thymulin titer.
The percentage of RCFs that may become azathioprine sensitive in the
presence of excess thymulin concentration ranges between 50 ~ and 65 ~. This technique, as extensively described elsewhere (Bach et al., 1975; Fabris et al., 1984), is specific for thymulin,
since the assay is unaffected by other thymic
hormones, and the rosette-inducing
activity
plasma samples through an antithymulin
is completely removed by passing
immunoadsorbent
(Bach et al.,
1975).
The sensitivity of the bioassay allows detection of I pglml synthetic thymulin (from Serva,
Heidelberg,
Germany).
The assay is reliable,
since in two con-
secutive blind assays, no difference of more than I (expressed as 111og2) was found in various samples (Bach et a l . , 1975). Determination of inactive thymic hormone {FTS). The presence of inactive thymulin was detected by the method of Fabris et al. (1984, 1986a). The method is based on the capacity of inactive molecules to inhibit the biological activity of synthetic thymulin
in the rosette-inhibition
assay.
Sixty
~I of plasma diluted
1:50 with Hank's solution was mixed with 60 ul of different concentrations of synthetic pg/ml).
thymulin A I
(final
concentrations
= 0.1,
0.5,
I,
5,
10,
50 and
100
: 50 dilution of plasma was used to avoid interference by endo-
genous thymulin, while the lowest final concentration of synthetic thymulin used was 0.1 pglml as, in our experimental conditions, this was the lowest concentration
can inducing azathioprine sensitivity in the spleen cells from thymec-
tomized mice. The mixture was immediately filtered through a CF50 Amicon membrane
(cone size 50,000
daltons)
for 30 min at 4~
Filtrate
was tested
for
thymulin activity in the rosette assay. Inactive thymulin concentration was expressed as the highest concentration of synthetic thymulin
(pg/ml inhibited by
the plasma sample). Mitogen response. Spleen cells, obtained" by teasing the spleen through a 60-mesh
sieve, were washed twice in Hank's solution,
counted and resuspen-
270 ded,
to a final
RPMI-1640
concentration
(Gibco)
supplemented
activated male human serum. (Cook,
of 3 x
106 t r y p a n
with
glutamine,
blue excluding antibiotics
cells/ml,
in
and 5 ~ fresh
in-
Aliquots of 0.1 ml were d i s t r i b u t e d
in microwells
USA). Mitogen was then added in the amount of 10 ul/well.
bation at 37~
in a CO 2 atmosphere for 48 h r s ,
A f t e r incu-
1 ]~Ci of 3H-thymidine
(spec.
act. 2000 mCi/mM; Amersham) was added to each well. Cells were collected 20 h later by an automatic cell h a r v e s t e r determined were
using
prepared
a scintillation
for
(Skatron,
counter
each mitogen
Norway)
and
{Tricarb-Packard).
concentration.
radioactivity Triplicate
Phytohaemagglutinin
Difco) was used at final concentration of 0.0125 ~g/ml.
was
cultures M (PHA,
Concanavalin A ( C o n - A ,
Serva) was used at the final concentration of 7.5 ~ g / m l . NK
assay.
A
51Cr-cytotoxicity
assay
in
0.2
ml
Linbro
microtest
plates
(Flow Laboratories) was used. YAC-1 target cells (106/ml) were labelled for 1 h 51 with 100 lJCi (specific a c t i v i t y 386.05 mCi/mg) Cr (sodium chromate, New England Nuclear)
at 37~
washed (three times) and added to effector cell po-
pulations in a 4 hrs 51Cr-release assay. Plates were centrifuged at 800 rpm for 5 min and 100 ul of supernatant was collected and counted in a Beckman 5500 51 gamma counter. The spontaneous release was determined by c u l t u r i n g Cr-labelled target cells alone.
Total counts were determined
by counting
an aliquot
of labelled target cells after resuspension in the well. The following formula was used to calculate the percentage specific lysis. Test cpm - spontaneous release Specific lysis =
x 100 Total counts - spontaneous release
For cell
interferon
populations
were
(IFN)
and
interleukin-2
incubated
for
24 h r
(IL-2) with
boosting,
IFN
effector
(1000 U/ml)
or
spleen
IL-2
(25
U/ml) and then the c y t o t o x i c i t y a c t i v i t y was detected as described above. Zinc determination.
Plasma zinc was determined by atomic absorption spec-
trophotometry against reference standard (Evenson and Warren, 1975}. Statistical two-tailed
analysis.
Student's
The significance
t test.
Differences
between
the means was assessed by
were considered
significant
when p <
0.05.
RESULTS Effect of zinc and arginine on thymic endocrine function Table I shows that old mice have a reduced thymus weight,
a low plasma
concentration of active thymulin / Z n - F T S ) and an increased level of the inactive form ( F T S ) .
The serum zinc levels are also reduced in old mice when compared
with the values of young controls.
271 Table I EFFECT OF ZINC AND ARGININE ADMINISTRATION ON VARIOUS PARAMETERS IN OLD MICE (mean + S . D . )
Animals
Treatment
Thymus
Thymulin
Thymulin
Plasma Zn
weight
(ZnFTS)
i n h i b , act.
level
mg
I I log 2
pglml
ugldl
Young
none
47.5 + 2.3
4.8 + 0.2
0.3 + 0.02
115 + 13
2 months
Arg
48.3 + 2.0
5.1 + 0.3
0.3 + 0.03
117 + 17
Zn
45.3 + 1.7
5.1 + 0.3
0.2 + 0.03
120 + 15
A r g + Zn
46.7 + 2.1
5.2 + 0.2
0.2 + 0.03
115 + 15
65.0 + 11.7
85 + 17
Old
none
18.5 + 2.5
1.5 + 0.3
24 months
Arg
37.3 + 2 . 7 * *
3.0 + 0.2*
2.3 + 1.0 * *
90 + 15
Zn
36.3 + 2 . 5 * *
3.8 + 0.2*
0.9 + 0.04**
98 + 12"
A r g + Zn
36.8 + 2 . 7 * *
5.0 + 0 . 3 * *
0.5 + 0.03**
100 + 11"
Notes: One and 2 a s t e r i s k s indicate p < 0.05 or 0.001, the age-matched u n t r e a t e d c o n t r o l s .
r e s p e c t i v e l y , against
All the treatments with a r g i n i n e or zinc alone or with
z i n c - a r g i n i n e com-
bination for 30 consecutive days in old mice induced a r e g r o w t h of the thymus up to 80 ~ of the weight values recorded in young mice w i t h o u t s t a t i s t i c a l l y s i g n i f i c a n t d i f f e r e n c e s between v a r i o u s treatments. c o v e r y of the mice,
reduced
plasma t h y m u l i n
the z i n c - a r g i n i n e combination
A statistically significant
level is also observed
being more e f f e c t i v e than
in
re-
old treated
the single n u t -
r i e n t s alone (p < 0.01). In all treated old g r o u p s ,
a reduction of plasma concentration
of thymic
hormone inactive molecules is observed when compared to values of old u n t r e a t ed
mice,
group
with
complete
disappearance
in
the
zinc
while in the a r g i n i n e alone treated group
and
zinc-arginine
a small residual
treated
level of the
inactive thymic hormone form is s t i l l detectable. Treatments with zinc and zinca r g i n i n e combinations increase also mean zinc plasma v a l u e s ,
(p
< 0.05);
argi-
nine treatment induces only a small increment of zinc v a l u e s . No s i g n i f i c a n t
effects
have
been
induced
by
any
of
the
treatments
in
young mice (Table I ) . Effect of zinc and a r g i n i n e on p e r i p h e r a l immune e f f i c i e n c y Table II shows that a r g i n i n e administration as well as zinc-supplementation are able to cause a s t a t i s t i c a l l y s i g n i f i c a n t increment of both PHA and Con-A (p
272 T a b l e II EFFECT
OF
ZINC
AND
ARGININE
ADMINISTRATION
ON
TH E
MITOGEN
RESPONSE OF SPLEEN CELLS OF OLD MICE (mean + S . D . )
Animals
Treatment
PHA
ConA (cpmlcult)x103
Young
none
78.7 + 13
245.6 + 13
2 months
Arg
92.4 + 15
243.1 + 15
Zn
70.2 + 13
239.7 + 15
A r g + Zn
90.4 + 15
245.7 + 12
16.1 + 16
58.5 + 11
Old
none
m
24 m o n t h s
Arg
60.2 + 15"*
124.4 + 12"*
m
Zn
46.8 + 15"*
87.0 + 15"
A r g + Zn
65.2 + 13"*
120.2 + 12"*
Notes: One and 2 a s t e r i s k s i n d i c a t e p < 0.05 the age-matched u n t r e a t e d controls.
or
0.001,
respectively,
against
Table III EFFECT OF ZINC A N D A R G I N I N E A D M I N I S T R A T I O N ON NK A C T I V I T Y IN OLD MICE (mean 96 o f l y s i s + S . D . )
Treatment
NK ( b a s a l )
None
NK ( y - I F N )
NK ( I L - 2 )
none
17.70 + 0,56
3,15 + 0.42
12.50 + 0,66
12.70 + 1.56
Arg
20.50 + 0 . 2 9 " *
7,52 + 0 , 6 8 * *
14.40 + 1,31
16.80 + 2,25
Zn
24,20 + 0 , 2 9 *
5,51 + 0 , 4 7 "
13,25 + 1,04
11,63 + 2,32
A r g + Zn
23.10 + 0 , 4 1 " *
9.90 + 1,96 ~'*
15,28 + 0 , 9 6 *
13.82 + 2.55
7.53 + 3.09
Young
Old none
2.86 + 0.19
2.63 + 2.62
3.22 + 0.43
Arg
3.02 + 0.22
2.67 + 0.22
8.34 + 1 . 2 3 " *
12.10 + 3.96
Zn
5.37 + 0.79
3.91 + 0.45
6.23 + 1 . 2 3 "
10.10 + 1.22
A r g + Zn
5.45 + 0 . 5 5 * *
5.21 + 0.54
10.83 + 1 . 0 8 " *
Notes: One and 2 a s t e r i s k s i n d i c a t e p < 0.05 the age-matched untreated controls.
or
0.001,
17.34 + 3 . 1 5 " *
respectively,
against
273 < 0.01)
response in cells from old mice,
being more active than zinc.
Consequently,
observed when zinc-arginine
combination
tivity
the
low
endogenous
NK
the arginine
treatment,
as a t r e n d ,
no f u r t h e r
significant
increment is
is used.
cytotoxicity
With regard
of old
to NK cell ac-
mice when
compared
with
young animals (p < 0.01) is s l i g h t l y modified only by zinc-arginine combination, although the increment is practically activity
induced
combination,
by
IFN and
IL-2
the single n u t r i e n t s
city (Table I I I ) .
irrelevant in respect of young values. is significantly
increased
by
NK
zinc-arginine
being effective only on IFN-induced c y t o t o x i -
A slight increase p a r t i c u l a r l y of basal NK a c t i v i t y is also p r e -
sent in young treated mice, regardless the kind of treatment applied. DISCUSSION Clinical
and
experimental
zinc (Fabris et a l . , al.,
evidences
1990) and L-arginine
have demonstrated (Fabris et a l . ,
the
relevance
of
1986b; Mocchegiani et
1990) for immunocompetence and the capacity of oral supplementation either
with zinc or with arginine to restore at least to some extent thymic endocrine a c t i v i t y and peripheral immune functions in old mice and humans (Fabris et a l . , 1990; Fabris and Mocchegiani, 1991). The findings reported in the present paper while confirming the effectiveness of zinc and arginine treatment in recovering age-related demonstrate that the zinc-arginine
immune functions,
combination is more effective that the t r e a t -
ments of single n u t r i e n t s alone in particular on the reactivation of thymic endocrine a c t i v i t y ,
as measured by the circulating
thymic factors,
i.e.,
level of one of the best known
thymulin ( Z n - F T S ) and the NK a c t i v i t y ,
p a r t i c u l a r l y under
boosting condition by IL-2 or IFN. On the other parameters tested,
the zinc-arginine
combination
either was
not more effective than the single n u t r i e n t s or a prevalence of one of them was detectable such as of arginine on mitogen response, or of zinc on basal NK activity. In all cases the effects
do not seem to be additive,
since the effect
of
zinc-arginine combination never represented the sum of the effect of the t r e a t ments with single n u t r i e n t s . Another consideration to be made is that the percentual restoration in respect of the values observed in young animals is d i f f e r e n t in dependence on the parameter
tested.
The percentual
increment
around 50-70 % for mitogen responses,
is marginal
in basal NK a c t i v i t y ,
nearly 100 % for IFN and IL-2 boosting
NK c y t o t o x i c i t y , and for thymic endocrine a c t i v i t y . These findings can suggest some considerations.
F i r s t of all,
it is out of
doubt that both zinc and arginine are effective in restoring immune efficiency in old mice, although the preferential
functional target for each of these n u t r i e n t s
274 may be different
and d i f f e r e n t also the effectiveness of the combination.
cases, any of the age-related intrinsic
and i r r e v e r s i b l e ,
In all
immune defects studied should not be considered
since one or the other treatment can restore it,
at
least to a significant extent. Secondly,
the degree of restoration
is not total for all parameters.
would suggest either that other factors,
in addition
to zinc and arginine,
This are
required for completely recovering some immunological defects in old age or that the length of the treatment was not enough to affect all parameters. second hypothesis should obviously
be tested,
cluded since various microenvironmental
While this
the f i r s t one might not be e x -
factors act on the immune system and
all of them may be required to f u l l y restore it during aging. Finally, that,
the lack of an additive
to a certain e x t e n t ,
effect of zinc and arginine
may suggest
the mechanism involved belong to a common physio-
logical cascade. This interpretation may find support in the knowledge that zinc may influence the t u r n o v e r of T 3 - T 4 (Fabris et a l . , and PRL ( T r a v a g l i n i et a l . ,
1991), GH (Prasad,
1985)
1989) that are hormones promoting immune efficien-
cy, and that arginine has a secretagogue action on the same hormones. On the other hand high blood levels of GH are associated with increased plasma levels of zinc
(Travaglini
still unknown.
et a l . ,
1990),
though
the reasons for this association are
These considerations make acceptable the work hypothesis that at
least p a r t of the physiological cascade activated by zinc or by arginine may be common and therefore
an additive
effect
of the two compounds
might
not be
observable. While this hypothesis
will
be matter of f u t u r e
sented clearly suggest that nutritional
works,
the findings
pre-
interventions and p a r t i c u l a r l y combination
of n u t r i e n t s may represent an interesting and side-effect deprived approach for immunorestoration in elderly people. ACKNOWLEDGEMENTS This
work
was supported
by
CNR and
Italian
Health
Ministry.
We are
grateful to Mr, M, Marcellini and Mrs. N. Gasparini for their excellent technical assistance, We thank Mrs, C. Chesi for t y p i n g the manuscript. REFERENCES Bach, J . F . , Dardenne, M., Pleau, J.M. and Bach, M.A. (1975): Isolation, biochemical characteristics and biological a c t i v i t y of a circulating thymic h o r mone in the mouse and the human. Ann. N . Y . Acad. Sci. USA, 249, 186-210. Barbul, A . , Rettura, G . , Levenson, S.M. and Seifter, E. (1983): Wound healing and thymotropic effects of arginine: a p i t u i t a r y mechanism of action. Am. J. Clin. N u t r . , 37, 786-794. Bendich, A. (1988): A n t i o x i d a n t vitamins and immune response. In: Nutrition and Immunology, pp.125-148. Editor: R . K . Chandra. Alan Liss, New Y o r k .
275 Chandra, R.K, (1985): Trace elements regulation of immunity and infection. J. Am. Cell. N u t r . , 4, 5-16. Chandra, R.K. (1989): Nutritional regulation of immunity and risk of infection in old age. Immunology, 67, 141-147. Daly, J . M . , Reynolds, J . , Siga, R . K . , Shou, J. and Liberman, M.D. (1990): Effect of dietary protein and aminoacids on immune function. Critical Care Med., 18, 86-93. Dardenne, M., Pleau, J . , Nabama, B . , Lefancier, P., Denien, M., Choay, J. and Bach, J.F. (1982): Contribution of zinc and other metals to the biological activity of the serum thymic factor. Proc. Natl. Acad. Sci. USA, 79, 5370-5373. Duchateau, J . , Delespesse, G., Vrijen, R. and Coolet, H. (1981): Benefical effects of oral zinc supplementation on the immune response of old people. Am. J. Med., 70, 1001-1004. Evenson, M.A. and Warren, B . L . (1975): Determination of serum copper and zinc by atomic absorption with use of the graphite cuvette. Clin. Chem., 21, 619-624. Fabris, N. and Mocchegiani, E. (1992): Arginine-containing compounds and thymic endocrine a c t i v i t y . A review. Thymus, (in press) Fabris, N., Mocchegiani, E., Amadio, L . , Zannotti, M., Licastro, F. and Franceschi, C. (1984): Thymic hormone deficiency in normal aging and Down's syndrome: is there a primary failure of the thymus? Lancet, 1, 983-986. Fabris, N., Mocchegiani, E., Mariotti, S., Pacini, F. and Pinchera, A. (1986a): Thyroid function modulates thymus endocrine a c t i v i t y . J. Clin. Endocrinol. Metab., 62, 474-478. Fabris, N., Mocchegiani, E., Muzzioli, M. and Piloni, S. (1986b): Recovery of age-related decline of thymic endocrine activity and PHA response by lysine-arginine combination. Int. J. Immunopharm., 8, 677-685. Fabris, N . , Mocchegiani, E., Muzzioli, M. and Provinciali, M. (1988): Neuroendocrine-thymus interactions: perspectives for intervention in aging. Ann. New York Acad. Sci., 521, 72-87. Fabris, N., Mocchegiani, E., Muzzioli, M. and Provinciali, M. (1990): Zinc, immunity and aging. In: Biomedical Advances in Aging, pp. 271-281. Editor: A . L . Goldstein. Plenum Publ. Corp., New York. Fabris, N., Mocchegiani, E., Muzzioli, M. and Provinciali, M. (1991): The role of zinc in neuroendocrine-immune interactions during aging. Ann. New York Acad. Sci., 621, 314-326. Franceschi, C . , Chiricolo, M., Licastro, F., Zannotti, M., Masi, M., Mocchegiani, E. and Fabris, N. (1988): Oral zinc supplementation in Down's syndrome: restoration of thymic endocrine activity and of some immune defects. J. Ment. Defic. Res., 32, 169-181. Mocchegiani, E., Cacciatore, L . , Talarico, M., Lingetti, N. and Fabris, N. (1990): Recovery of low thymic hormone levels in cancer patients by lysine-arginine combination. Int. J. Immunopharmacol., 12, 365-371. Penny, R., Blizzard, R.M. and Davis, W.J. (1970): Sequential study of arginine monochloride and normal saline as stimuli to growth hormone release. Metabolism, 19, 165-173. Prasad, A.S. (1985): Clinical, endocrinological and biochemical effects of zincdeficiency. Clin. Endocrinol. Metab., 14, 567-589. Travaglini, P., Moriondo, P., Togni, E., Venegoni, P., Bocchicchio, D., Faglia, G., Ambroso, G., Ponticelli, C . , Mocchegiani, E. and Fabris, N. (1989): Effect of oral zinc administration on prolactin and thymulin c i r culating levels in uremic patients. J. Clin. Endocrinol. Metab., 68, 186-190. Travaglini, P., Mocchegiani, E., Togni, E., Muratori, M., Re, T . , Bassani, L. and Fabris, N. (1990): Thymulin and zinc circulating level in patients with GH and PRL secreting p i t u i t a r y adenomas. Int. J. Neurosci., 51, 269-271. Underwood, E.J. (1977): Trace Element,s in Human and Animal Nutrition. pp. 1-302. 4th edition, Academic Press, New York.
267
RESTORING EFFECT OF ORAL SUPPLEMENTATION OF ZINC AND ARGININE ON THYMIC ENDOCRINE ACTIVITY AND PERIPHERAL IMMUNE FUNCTIONS IN AGED MICE
E~ MOCCHEGIANI, M. MUZZlOLI, L. SANTARELLI and N. FABRIS a Immunological Center, Gerontological Research Department, Institute of National Research Centers on Aging (INRCA), Via Birarelli, 8, 1-60121 Ancona, Italy, and Chair of Immunology, University of Pavia, Piazza Botta, 10, 1-27100 Pavia, Italy SUMMARY Previous work from this laboratory has demonstrated that both a trace element, zinc, and an amino acid, arginine, are capable, when orally administered, to recover some age-related immune dysfunctions. In the present paper the effectiveness of a zinc-arginine combination versus the single nutrients in restoring age-related immunological alterations in old Balb/c mice has been investigated. The zinc-arginine combination is more effective than the treatments of single nutrients alone, in particular on the reactivation of thymic endocrine activity, as measured by the circulating level of one of the best known thymic factors, i.e. thymulin (Zn-FTS) and the natural killer (NK) cell activ i t y , particularly under boosting condition by interleukin-2 (IL-2) or interferon (IFN). On the other parameters tested the zinc-arginine combination either was not more effective than the single nutrients or a prevalence of one of them was detectable, such as of arginine on mitogen response or of zinc on basal NK act i v t i y . The findings clearly suggest that nutritional interventions and particularly combination of nutrients may represent an interesting and side-effect deprived approach for immunorestoration in elderly people. Keywords: Zinc, arginine, aging, thymulin immune function
INTRODUCTION The frequent association between malnutrition,
infective diseases and aging
has provoked a good body of experimental and clinical studies, aimed to analyze either the effect of single nutrients on the immunological in immunological
aging (Chandra,
efficiency or their role
1985, 1989). While the number of single nut-
rients relevant of immune efficiency is somewhat consistent, ranging from traceelements
(Underwood,
(Daly et al., immunological
1977) to vitamins
(Bendich,
1988) and to amino acids
1990), the studies directed to investigate their possible role in aging have remained untill now fragmentary.
Nevertheless, it has been demonstrated that a trace element, zinc and an amino acid, arginine, may exert a restorative effect of some age-related immunological alterations.
In particular,
zinc has been found capable to restore cuta-
neous hypersensitivity reactions and responses to tetanus texoid vaccination in healthy elderly (Duchateau et al., in elderly patients suffering
1981), to recover thymic endocrine function
from uremia" or hyperprolactinemia
(Travaglini et
al., 1989) and to correct both thymic function and peripheral immune efficiency
268 in subjects suffering from Down's syndrome (Franceschi et al., 1988), which is considered an early aging syndrome.
These human findings
have got f u r t h e r
support by experimental studies showing that zinc supplementation
in old mice
can recover thymic structure and function and increase mitogen responsiveness of spleen cells (Fabris et al., 1990). One of the mechanisms of zinc action has been identified in the capacity of this trace element to confer biological activity to one of the best known thymic factor,
i.e.
thymulin [ Z n - F T S ) ,
the zinc-unbound
(FTS) form of which is not
only biologically inactive but competes with the active form for the binding to the specific target (Dardenne et al., 1982; Fabris et al., 1984). The relevance of arginine for the efficiency of the immune system has been hypothesized by the observation that supplementary dietary arginine in youngadult injured rats can accelerate wound healing and prevent post-traumatic atrophy of the thymus (Barbul et al., 1983). A possible role for arginine
in
immunological
aging
has been suggested
because arginine has a secretagogue action on growth hormone (GH, al.,
Penny et
1970) and that GH is capable to modulating thymic endocrine activity and
various immune functions during development and aging (Fabris et a l . ,
1988).
It has been,
in old
in fact,
demonstrated
that oral arginine supplementation
mice causes a complete recovery of the reduced thymic endocrine activity with an improvement of peripheral immune efficiency, such as T-cell subsets, mitogen responses and NK activity [Fabris et al.,
1986b). Arginine supplementation has
been found effective in increasing thymic endocrine activity and percentage of peripheral giani,
blood T-helper
(CD4) cells in healthy elderly
1991) and in neoplastic patients
[Fabris and Mocche-
[Mocchegiani et al.,
and arginine seem to act on similar targets,
1990).
Since zinc
the question arose, whether the
combination of zinc and arginine supplementation might be more effective than the administration of the single nutrient alone. With these premises, zinc-sulphate
(Zn) and L-arginine
(Arg)
orally administered to aged mice either alone or in combination
have been
(Zn-Arg)
and
their effect on immune system evaluated in terms of thymic endocrine efficiency, peripheral T-mitogen response and NK activity. MATERIALS AND METHODS Animals. Young male (2 months) and old male (24 months) Balblc mice from our own colony were used. In both age groups mice were treated for 30 consecutive days either with arginine alone (added to the drinking water in a concentration assuring a total daily intake of 9 x 10-4 g/day/mouse, if we assume a water consumption of 5 mlldaylmouse), or with zinc sulphate alone (at the dose of 5 ]Jgldaylmouse), or with zinc-arginine combination at the same doses.
269 Thymulin T-
and
(Zn-FTS) determination.
B-lymphocytes
carry
Spleen cells from young mice including
receptors
for
sheep erythrocytes
(SRBC)
and,
therefore, form rosettes (RFC) when mixed with SRBC. T - and B-rosettes can be discriminated
by
adding
10 ug/ml
azathioprine,
which
selectively
inhibits
T-rosette formation. The azathioprine sensitivity of T-cells is strictly dependent on the thymic endocrine function: plete
disappearance
spleen
cells
(Zn-FTS).
from
of
the
in biological
fluids
azathioprine-sensitivity
thymectomized
This phenomenon
removal of the thymus in mice induces commice
are
while
incubated
it
with
reappears purified
when
thymulin
represents the basis for the bioassay of thymulin
(Bach et al.,
1975).
The bioassay is still
required
since
questions have been raised over the specificity of the radioimmunoassay developed till
now.
The maximum dilution
of plasma samples inducing
azathioprine
sensitivity in 50 % of RCFs from thymectomized mice was taken as the thymulin titer.
The percentage of RCFs that may become azathioprine sensitive in the
presence of excess thymulin concentration ranges between 50 ~ and 65 ~. This technique, as extensively described elsewhere (Bach et al., 1975; Fabris et al., 1984), is specific for thymulin,
since the assay is unaffected by other thymic
hormones, and the rosette-inducing
activity
plasma samples through an antithymulin
is completely removed by passing
immunoadsorbent
(Bach et al.,
1975).
The sensitivity of the bioassay allows detection of I pglml synthetic thymulin (from Serva,
Heidelberg,
Germany).
The assay is reliable,
since in two con-
secutive blind assays, no difference of more than I (expressed as 111og2) was found in various samples (Bach et a l . , 1975). Determination of inactive thymic hormone {FTS). The presence of inactive thymulin was detected by the method of Fabris et al. (1984, 1986a). The method is based on the capacity of inactive molecules to inhibit the biological activity of synthetic thymulin
in the rosette-inhibition
assay.
Sixty
~I of plasma diluted
1:50 with Hank's solution was mixed with 60 ul of different concentrations of synthetic pg/ml).
thymulin A I
(final
concentrations
= 0.1,
0.5,
I,
5,
10,
50 and
100
: 50 dilution of plasma was used to avoid interference by endo-
genous thymulin, while the lowest final concentration of synthetic thymulin used was 0.1 pglml as, in our experimental conditions, this was the lowest concentration
can inducing azathioprine sensitivity in the spleen cells from thymec-
tomized mice. The mixture was immediately filtered through a CF50 Amicon membrane
(cone size 50,000
daltons)
for 30 min at 4~
Filtrate
was tested
for
thymulin activity in the rosette assay. Inactive thymulin concentration was expressed as the highest concentration of synthetic thymulin
(pg/ml inhibited by
the plasma sample). Mitogen response. Spleen cells, obtained" by teasing the spleen through a 60-mesh
sieve, were washed twice in Hank's solution,
counted and resuspen-
270 ded,
to a final
RPMI-1640
concentration
(Gibco)
supplemented
activated male human serum. (Cook,
of 3 x
106 t r y p a n
with
glutamine,
blue excluding antibiotics
cells/ml,
in
and 5 ~ fresh
in-
Aliquots of 0.1 ml were d i s t r i b u t e d
in microwells
USA). Mitogen was then added in the amount of 10 ul/well.
bation at 37~
in a CO 2 atmosphere for 48 h r s ,
A f t e r incu-
1 ]~Ci of 3H-thymidine
(spec.
act. 2000 mCi/mM; Amersham) was added to each well. Cells were collected 20 h later by an automatic cell h a r v e s t e r determined were
using
prepared
a scintillation
for
(Skatron,
counter
each mitogen
Norway)
and
{Tricarb-Packard).
concentration.
radioactivity Triplicate
Phytohaemagglutinin
Difco) was used at final concentration of 0.0125 ~g/ml.
was
cultures M (PHA,
Concanavalin A ( C o n - A ,
Serva) was used at the final concentration of 7.5 ~ g / m l . NK
assay.
A
51Cr-cytotoxicity
assay
in
0.2
ml
Linbro
microtest
plates
(Flow Laboratories) was used. YAC-1 target cells (106/ml) were labelled for 1 h 51 with 100 lJCi (specific a c t i v i t y 386.05 mCi/mg) Cr (sodium chromate, New England Nuclear)
at 37~
washed (three times) and added to effector cell po-
pulations in a 4 hrs 51Cr-release assay. Plates were centrifuged at 800 rpm for 5 min and 100 ul of supernatant was collected and counted in a Beckman 5500 51 gamma counter. The spontaneous release was determined by c u l t u r i n g Cr-labelled target cells alone.
Total counts were determined
by counting
an aliquot
of labelled target cells after resuspension in the well. The following formula was used to calculate the percentage specific lysis. Test cpm - spontaneous release Specific lysis =
x 100 Total counts - spontaneous release
For cell
interferon
populations
were
(IFN)
and
interleukin-2
incubated
for
24 h r
(IL-2) with
boosting,
IFN
effector
(1000 U/ml)
or
spleen
IL-2
(25
U/ml) and then the c y t o t o x i c i t y a c t i v i t y was detected as described above. Zinc determination.
Plasma zinc was determined by atomic absorption spec-
trophotometry against reference standard (Evenson and Warren, 1975}. Statistical two-tailed
analysis.
Student's
The significance
t test.
Differences
between
the means was assessed by
were considered
significant
when p <
0.05.
RESULTS Effect of zinc and arginine on thymic endocrine function Table I shows that old mice have a reduced thymus weight,
a low plasma
concentration of active thymulin / Z n - F T S ) and an increased level of the inactive form ( F T S ) .
The serum zinc levels are also reduced in old mice when compared
with the values of young controls.
271 Table I EFFECT OF ZINC AND ARGININE ADMINISTRATION ON VARIOUS PARAMETERS IN OLD MICE (mean + S . D . )
Animals
Treatment
Thymus
Thymulin
Thymulin
Plasma Zn
weight
(ZnFTS)
i n h i b , act.
level
mg
I I log 2
pglml
ugldl
Young
none
47.5 + 2.3
4.8 + 0.2
0.3 + 0.02
115 + 13
2 months
Arg
48.3 + 2.0
5.1 + 0.3
0.3 + 0.03
117 + 17
Zn
45.3 + 1.7
5.1 + 0.3
0.2 + 0.03
120 + 15
A r g + Zn
46.7 + 2.1
5.2 + 0.2
0.2 + 0.03
115 + 15
65.0 + 11.7
85 + 17
Old
none
18.5 + 2.5
1.5 + 0.3
24 months
Arg
37.3 + 2 . 7 * *
3.0 + 0.2*
2.3 + 1.0 * *
90 + 15
Zn
36.3 + 2 . 5 * *
3.8 + 0.2*
0.9 + 0.04**
98 + 12"
A r g + Zn
36.8 + 2 . 7 * *
5.0 + 0 . 3 * *
0.5 + 0.03**
100 + 11"
Notes: One and 2 a s t e r i s k s indicate p < 0.05 or 0.001, the age-matched u n t r e a t e d c o n t r o l s .
r e s p e c t i v e l y , against
All the treatments with a r g i n i n e or zinc alone or with
z i n c - a r g i n i n e com-
bination for 30 consecutive days in old mice induced a r e g r o w t h of the thymus up to 80 ~ of the weight values recorded in young mice w i t h o u t s t a t i s t i c a l l y s i g n i f i c a n t d i f f e r e n c e s between v a r i o u s treatments. c o v e r y of the mice,
reduced
plasma t h y m u l i n
the z i n c - a r g i n i n e combination
A statistically significant
level is also observed
being more e f f e c t i v e than
in
re-
old treated
the single n u t -
r i e n t s alone (p < 0.01). In all treated old g r o u p s ,
a reduction of plasma concentration
of thymic
hormone inactive molecules is observed when compared to values of old u n t r e a t ed
mice,
group
with
complete
disappearance
in
the
zinc
while in the a r g i n i n e alone treated group
and
zinc-arginine
a small residual
treated
level of the
inactive thymic hormone form is s t i l l detectable. Treatments with zinc and zinca r g i n i n e combinations increase also mean zinc plasma v a l u e s ,
(p
< 0.05);
argi-
nine treatment induces only a small increment of zinc v a l u e s . No s i g n i f i c a n t
effects
have
been
induced
by
any
of
the
treatments
in
young mice (Table I ) . Effect of zinc and a r g i n i n e on p e r i p h e r a l immune e f f i c i e n c y Table II shows that a r g i n i n e administration as well as zinc-supplementation are able to cause a s t a t i s t i c a l l y s i g n i f i c a n t increment of both PHA and Con-A (p
272 T a b l e II EFFECT
OF
ZINC
AND
ARGININE
ADMINISTRATION
ON
TH E
MITOGEN
RESPONSE OF SPLEEN CELLS OF OLD MICE (mean + S . D . )
Animals
Treatment
PHA
ConA (cpmlcult)x103
Young
none
78.7 + 13
245.6 + 13
2 months
Arg
92.4 + 15
243.1 + 15
Zn
70.2 + 13
239.7 + 15
A r g + Zn
90.4 + 15
245.7 + 12
16.1 + 16
58.5 + 11
Old
none
m
24 m o n t h s
Arg
60.2 + 15"*
124.4 + 12"*
m
Zn
46.8 + 15"*
87.0 + 15"
A r g + Zn
65.2 + 13"*
120.2 + 12"*
Notes: One and 2 a s t e r i s k s i n d i c a t e p < 0.05 the age-matched u n t r e a t e d controls.
or
0.001,
respectively,
against
Table III EFFECT OF ZINC A N D A R G I N I N E A D M I N I S T R A T I O N ON NK A C T I V I T Y IN OLD MICE (mean 96 o f l y s i s + S . D . )
Treatment
NK ( b a s a l )
None
NK ( y - I F N )
NK ( I L - 2 )
none
17.70 + 0,56
3,15 + 0.42
12.50 + 0,66
12.70 + 1.56
Arg
20.50 + 0 . 2 9 " *
7,52 + 0 , 6 8 * *
14.40 + 1,31
16.80 + 2,25
Zn
24,20 + 0 , 2 9 *
5,51 + 0 , 4 7 "
13,25 + 1,04
11,63 + 2,32
A r g + Zn
23.10 + 0 , 4 1 " *
9.90 + 1,96 ~'*
15,28 + 0 , 9 6 *
13.82 + 2.55
7.53 + 3.09
Young
Old none
2.86 + 0.19
2.63 + 2.62
3.22 + 0.43
Arg
3.02 + 0.22
2.67 + 0.22
8.34 + 1 . 2 3 " *
12.10 + 3.96
Zn
5.37 + 0.79
3.91 + 0.45
6.23 + 1 . 2 3 "
10.10 + 1.22
A r g + Zn
5.45 + 0 . 5 5 * *
5.21 + 0.54
10.83 + 1 . 0 8 " *
Notes: One and 2 a s t e r i s k s i n d i c a t e p < 0.05 the age-matched untreated controls.
or
0.001,
17.34 + 3 . 1 5 " *
respectively,
against
273 < 0.01)
response in cells from old mice,
being more active than zinc.
Consequently,
observed when zinc-arginine
combination
tivity
the
low
endogenous
NK
the arginine
treatment,
as a t r e n d ,
no f u r t h e r
significant
increment is
is used.
cytotoxicity
With regard
of old
to NK cell ac-
mice when
compared
with
young animals (p < 0.01) is s l i g h t l y modified only by zinc-arginine combination, although the increment is practically activity
induced
combination,
by
IFN and
IL-2
the single n u t r i e n t s
city (Table I I I ) .
irrelevant in respect of young values. is significantly
increased
by
NK
zinc-arginine
being effective only on IFN-induced c y t o t o x i -
A slight increase p a r t i c u l a r l y of basal NK a c t i v i t y is also p r e -
sent in young treated mice, regardless the kind of treatment applied. DISCUSSION Clinical
and
experimental
zinc (Fabris et a l . , al.,
evidences
1990) and L-arginine
have demonstrated (Fabris et a l . ,
the
relevance
of
1986b; Mocchegiani et
1990) for immunocompetence and the capacity of oral supplementation either
with zinc or with arginine to restore at least to some extent thymic endocrine a c t i v i t y and peripheral immune functions in old mice and humans (Fabris et a l . , 1990; Fabris and Mocchegiani, 1991). The findings reported in the present paper while confirming the effectiveness of zinc and arginine treatment in recovering age-related demonstrate that the zinc-arginine
immune functions,
combination is more effective that the t r e a t -
ments of single n u t r i e n t s alone in particular on the reactivation of thymic endocrine a c t i v i t y ,
as measured by the circulating
thymic factors,
i.e.,
level of one of the best known
thymulin ( Z n - F T S ) and the NK a c t i v i t y ,
p a r t i c u l a r l y under
boosting condition by IL-2 or IFN. On the other parameters tested,
the zinc-arginine
combination
either was
not more effective than the single n u t r i e n t s or a prevalence of one of them was detectable such as of arginine on mitogen response, or of zinc on basal NK activity. In all cases the effects
do not seem to be additive,
since the effect
of
zinc-arginine combination never represented the sum of the effect of the t r e a t ments with single n u t r i e n t s . Another consideration to be made is that the percentual restoration in respect of the values observed in young animals is d i f f e r e n t in dependence on the parameter
tested.
The percentual
increment
around 50-70 % for mitogen responses,
is marginal
in basal NK a c t i v i t y ,
nearly 100 % for IFN and IL-2 boosting
NK c y t o t o x i c i t y , and for thymic endocrine a c t i v i t y . These findings can suggest some considerations.
F i r s t of all,
it is out of
doubt that both zinc and arginine are effective in restoring immune efficiency in old mice, although the preferential
functional target for each of these n u t r i e n t s
274 may be different
and d i f f e r e n t also the effectiveness of the combination.
cases, any of the age-related intrinsic
and i r r e v e r s i b l e ,
In all
immune defects studied should not be considered
since one or the other treatment can restore it,
at
least to a significant extent. Secondly,
the degree of restoration
is not total for all parameters.
would suggest either that other factors,
in addition
to zinc and arginine,
This are
required for completely recovering some immunological defects in old age or that the length of the treatment was not enough to affect all parameters. second hypothesis should obviously
be tested,
cluded since various microenvironmental
While this
the f i r s t one might not be e x -
factors act on the immune system and
all of them may be required to f u l l y restore it during aging. Finally, that,
the lack of an additive
to a certain e x t e n t ,
effect of zinc and arginine
may suggest
the mechanism involved belong to a common physio-
logical cascade. This interpretation may find support in the knowledge that zinc may influence the t u r n o v e r of T 3 - T 4 (Fabris et a l . , and PRL ( T r a v a g l i n i et a l . ,
1991), GH (Prasad,
1985)
1989) that are hormones promoting immune efficien-
cy, and that arginine has a secretagogue action on the same hormones. On the other hand high blood levels of GH are associated with increased plasma levels of zinc
(Travaglini
still unknown.
et a l . ,
1990),
though
the reasons for this association are
These considerations make acceptable the work hypothesis that at
least p a r t of the physiological cascade activated by zinc or by arginine may be common and therefore
an additive
effect
of the two compounds
might
not be
observable. While this hypothesis
will
be matter of f u t u r e
sented clearly suggest that nutritional
works,
the findings
pre-
interventions and p a r t i c u l a r l y combination
of n u t r i e n t s may represent an interesting and side-effect deprived approach for immunorestoration in elderly people. ACKNOWLEDGEMENTS This
work
was supported
by
CNR and
Italian
Health
Ministry.
We are
grateful to Mr, M, Marcellini and Mrs. N. Gasparini for their excellent technical assistance, We thank Mrs, C. Chesi for t y p i n g the manuscript. REFERENCES Bach, J . F . , Dardenne, M., Pleau, J.M. and Bach, M.A. (1975): Isolation, biochemical characteristics and biological a c t i v i t y of a circulating thymic h o r mone in the mouse and the human. Ann. N . Y . Acad. Sci. USA, 249, 186-210. Barbul, A . , Rettura, G . , Levenson, S.M. and Seifter, E. (1983): Wound healing and thymotropic effects of arginine: a p i t u i t a r y mechanism of action. Am. J. Clin. N u t r . , 37, 786-794. Bendich, A. (1988): A n t i o x i d a n t vitamins and immune response. In: Nutrition and Immunology, pp.125-148. Editor: R . K . Chandra. Alan Liss, New Y o r k .
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