Robust Growth Hormone (GH) secretion in aged female rats co-administered GH-releasing hexapeptide (GHRP-6) and GH-releasing hormone (GHRH)

Life Sciences, Vol. 49, pp. 1499-1504 Printed in the U.S.A.

Pergamon Press

R O B U S T GROWTH HORMONE (GH) SECRETION IN AGED FEMALE RATS C O - A D M I N I S T E R E D G H - R E L E A S I N G H E X A P E P T I D E (GHRP-6) AND G H - R E L E A S I N G H O R M O N E (GHRH)

R.F. Walker,

S-W. Yang and B.B. Bercu

D i v i s i o n of Endocrinology, Department of P e d i a t r i c s , U n i v e r s i t y of South Florida College of Medicine,Tampa, Florida 33612 and All Children's Hospital,St. Petersburg, Florida 33701 (Received in final form September 12, 1991) Summary Aging is associated with a blunted growth h o r m o n e (GH) secretory response to G H - r e l e a s i n g h o r m o n e (GHRH), in vivo. The o b j e c t i v e of the present study was to assess the effects of aging on the GH secretory response to G H - r e l e a s i n g h e x a p e p t i d e (GHRP-6), a synthetic GH secretagogue. GHRP-6 (30 Bg/kg) was a d m i n i s t e r e d alone or in c o m b i n a t i o n with GHRH (2 ~g/kg) to a n e s t h e t i z e d female Fischer 344 rats, 3 or 19 months of age. The peptides were c o - a d m i n i s t e r e d to d e t e r m i n e the effect of aging upon the p o t e n t i a t i n g effect of GHRP-6 on GHRH activity. The increase in plasma GH as a function of time following a d m i n i s t r a t i o n of GHRP-6 was lower (p < 0.001) in old rats than in young rats; w h e r e a s the increase in plasma GH secretion as a function of time following c o - a d m i n i s t r a t i o n of GHRP-6 and GHPd4was h i g h e r (p < 0.001) in old rats than in young rats (mean Cmax = 8539 ± 790.6 ~g/l vs. 2970 ± 866 ~g/l, respectively; p <0.01). since p i t u i t a r y GH concentrations in old rats were lower than in young rats (257.0 ± 59.8 ~g/mg wet wt. vs. 639.7 ± 149.2 ~g/mg wet wt., respectively; p < 0.03), the results s u g g e s t e d that GH functional reserve in old female rats was not linked to p i t u i t a r y GH concentration. The d i f f e r e n t i a l r e s p o n s e s of old rats to individually a d m i n i s t e r e d and c o - a d m i n i s t e r e d GHRP-6 are important because they d e m o n s t r a t e that robust and immediate GH secretion can occur in old rats that are a p p r o p r i a t e l y stimulated. The data further suggest that the cellular p r o c e s s e s subserving GH secretion are intact in old rats, and that a g e - r e l a t e d decrements in GH s e c r e t i o n result from inadequate stimulation, rather than to m a l a d a p t i v e changes in the m e c h a n i s m of GH release. The d e c l i n e in serum growth hormone (GH) c o n c e n t r a t i o n s during aging is a s s o c i a t e d with a p r o g r e s s i v e i n s e n s i t i v i t y of the p i t u i t a r y gland to G H - r e l e a s i n g hormone (GHRH), in vivo. GH secretion following GHRH a d m i n i s t r a t i o n was inversely c o r r e l a t e d with age in men and women between the ages of 18 and 95 years (i4), and in a n e s t h e t i z e d male rats, between the ages of 3 and 21 m o n t h s (5,6). 0024-3205/91 $3.00 + .00 Copyright © 1991 Pergamon Press plc

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GHRP-6 in Aged Rats

Vol. 49, No. 20, 1991

During the past decade, a synthetic peptide, H i s - D - T r p - A l a - T r p - D P h e - L y s - N H z (growth h o r m o n e r e l e a s i n g hexapeptide; GHRP-6) was identified as a specific GH s e c r e t a g o g u e in vivo and in vitro (see 7). GHRP-6 has d i f f e r e n t b i n d i n g c h a r a c t e r i s t i c s and employs different intracellular messengers from GHRH (8-10), and it potentiates GHRH activity (i0,ii). Since GHRP-6 can act i n d e p e n d e n t l y of GHRH, it was of interest to d e t e r m i n e whether aging also d i m i n i s h e s the hexapeptides' G H - r e l e a s i n g activity. GHRP-6 and GHRH were also co-administered, so as to e v a l u a t e ager e l a t e d changes in the functional i n t e r a c t i o n of the two GH secretagogues. M a t e r i a l s and M e t h o d s

Animal Husbandry:

Fischer 344 female rats (2 and 18 months of age) were purchased from the NIA colony at Harlan Industries (Indianapolis, Ind.) and a c c l i m a t e d to local c o n d i t i o n s of light (0600h - 1800h), t e m p e r a t u r e (72 ± 2 °F) and h u m i d i t y (60 ± 5 %) for 30 days before being used in the present study. The animal facility at All Children's Hospital is fully a p p r o v e d for use by the A A A L A C and complies with federal statues and r e g u l a t i o n s r e l a t i n g to animal use in research.

Peptides

and Experimental Design: GHRP-6 and rat GHRH were purchased from Peninsula Laboratories (Belmont, CA) and a d m i n i s t e r e d as saline solutions in doses of 30 Bg/kg and 2 ~g/kg, respectively. In a p r e l i m i n a r y d o s e - r a n g e study, 30 ~g/kg GHRP-6 was the EDs^ in anesthetized, 3 month old female rats. The dose of GHRH (2 ~g/~g) was selected from p u b l i s h e d data showing d i f f e r e n c e s in GH s e c r e t o r y responses in 3 and 18 month old rats (5). On the day of testing, rats were a n e s t h e t i z e d w i t h k e t a m i n e (60 mg/kg i.m.) and p e n t o b a r b i t a l (35 mg/kg i.p.) and the right femoral artery was cannulated. Peptides were administered with c o n s i d e r a t i o n of time from surgery so that all animals were tested under the same duration of anesthesia. Blood samples (approximately 250 ~i) were c o l l e c t e d in h e p a r i n i z e d tubes before and at selected intervals after administration of the GH secretagogues. The rats were e x s a n g u i n a t e d at the last blood sample and their p i t u i t a r y glands were rapidly removed, w e i g h e d and frozen on dry ice. No adenomas were evident upon m a c r o s c o p i c e x a m i n a t i o n of the pituitaries. Radioimmunoassay:

Blood samples were c e n t r i f u g e d and plasma was c o l l e c t e d for r a d i o i m m u n o a s s a y (RIA) analysis of GH concentrations. P i t u i t a r i e s were h o m o g e n i z e d in 0.1 N NaOH/saline, d i l u t e d and aliquots were analyzed by RIA for GH concentrations. RIA reagents were s u p p l i e d by Dr. A. Parlow (Harbor-UCLA M e d i c a l Center, Torrence, CA) and the NIADD. GH was e x p r e s s e d in terms of rGH-RP2. I n t r a a s s a y and interassay c o e f f i c i e n t s of v a r i a t i o n were <5 % and <8 %, respectively.

Data Analysis:

P i t u i t a r y GH c o n c e n t r a t i o n s and peak plasma GH c o n c e n t r a t i o n s (Cm ) were compared among the groups of y o u n g and old rats using Student's t test. Changes in p l a s m a GH s e c r e t i o n over time w e r e c o m p a r e d using two way A N O V A w i t h r e p e a t e d m e a s u r e s analysis. R e s u l t s were e x p r e s s e d as means ± S.E.M. Plasma and p i t u i t a r y GH c o n c e n t r a t i o n s were e x p r e s s e d as ~g/l and ~g/mg wet weight, respectively.

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GHRP-6 in Aged Rats

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Results The data p r e s e n t e d in Figure 1 show that the increase in GH s e c r e t i o n as a function of time following GHRP-6 a d m i n i s t r a t i o n was lower (p <0.001) in old rats than in young rats. M e a n peak plasma GH values were lower in old rats than in young rats (179.8 ± 64.9 ~g/l vs. 356.4 ± 85.0 ~g/l, respectively); h o w e v e r the d i f f e r e n c e s were not s t a t i s t i c a l l y significant. P o t e n t i a t e d GH secretion occurred in rats of both ages following c o - a d m i n i s t r a t i o n of GHRP-6 and GHRH. However, the increase in plasma GH c o n c e n t r a t i o n s as a function of time (p <0.001), and peak plasma GH c o n c e n t r a t i o n s (p < 0.01) were s i g n i f i c a n t l y greater in old rats than in y o u n g rats (Cmx = 8539 ± 790.6 ~g/l vs. 2970 ± 866 ~g/l, respectively). 60O

............ OLD RATS •

Y O U N G RATS

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MINUTES Fiq. 1

GH s e c r e t i o n in young (3 months old) and old (19 m o n t h s old) female, Fischer 344 rats following a d m i n i s t r a t i o n of GHRP-6 (30 ~g/kg). Values are expressed as means + SEM; N = 4 r a t s / a g e group.

As seen in Figure 2, the temporal profiles for GH secretion following c o - a d m i n i s t r a t i o n of GHRP-6 and GHRH were the same in the two age groups, except that plasma GH c o n c e n t r a t i o n s were up to three times higher in the old rats. P i t u i t a r y c o n c e n t r a t i o n s of GH in all y o u n g rats (639.7 ± 149.2 ~g/mg) were s i g n i f i c a n t l y higher (p < 0.03) than in all old rats (257.5 ± 59.8 ~g/mg). However, the data p r e s e n t e d in Table 1 show that the individual t r e a t m e n t s were a s s o c i a t e d w i t h d i f f e r e n t c o n c e n t r a t i o n s of p i t u i t a r y GH, p r o b a b l y reflecting the GH releasing efficacy of the individually a d m i n i s t e r e d or c o - a d m i n i s t e r e d peptides. C o - a d m i n i s t r a t i o n of GHRP-6 and GHRH was a s s o c i a t e d with the g r e a t e s t r e d u c t i o n in p i t u i t a r y GH c o n c e n t r a t i o n s in both age groups.

1502

GHRP-6

in A g e d R a t s

Vol.

49, No.

20,

1991

9,OOO T

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OLD RATS YOUNG

RATS

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Fig.

2

GH secretion in young and old female rats following coadministration of GHRP-6 and GHRH (30 ~g/kg and 2 ~g/kg, respectively). V a l u e s a r e e x p r e s s e d as m e a n ± SEM; N = 4 rats/age group. N o t e s c a l e d i f f e r e n c e o n t h e o r d i n a t e of t h i s g r a p h a n d t h a t in F i g u r e i.

TABLE

PITUITARY RATS AFTER

1

G H C O N C E N T R A T I O N S IN Y O U N G A N D O L D ADMINISTRATION OF GHRP-6 AND/OR GHRH PITUITARY GH CONCENTRATIONS Young Old

(~g/mg)

TREATMENT

N

GHRP-6

4

899

± 321

255

± 113"

GHRH

4

735

± 275

434

± 115"

GHRP-6 + GHRH

4

363 ± 122

170

±

p < 0.03;

o l d vs.

young

33*

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GHRP-6 in Aged Rats

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Discussion The results of this study show that GH s e c r e t i o n following a d m i n i s t r a t i o n of GHRP-6 declines during aging in female rats. Similar r e s p o n s e s following a d m i n i s t r a t i o n of GHRH have been r e p o r t e d in rats and humans (i - 6). Despite these a g e - r e l a t e d d e c r e m e n t s in response to GHRP-6 or GHRH, the r e s p o n s e to coa d m i n i s t e r e d GHRP-6 and GHRH was higher in old rats than in young rats. This effect was inversely related to p i t u i t a r y GH concentrations, which were higher in the y o u n g rats. Thus, even t h o u g h p i t u i t a r y GH c o n c e n t r a t i o n s were reduced, the old rats e x p r e s s e d a g r e a t e r functional GH reserve than the young rats when GHRP-6 and G H R H w e r e co-administered. The d i f f e r e n t i a l effects of GHRP-6 on GH secretion when a d m i n i s t e r e d alone or in c o m b i n a t i o n with GHRH are very important because they suggest that a g e - r e l a t e d d e c r e m e n t s in GH secretion are not due to intrinsic p i t u i t a r y defects. A p p a r e n t l y the cellular processes s u b s e r v i n g GH secretion were intact in old rats used in this study, since they were capable of i m m e d i a t e l y releasing as much or more GH as y o u n g rats when a p p r o p r i a t e l y stimulated. These findings are c o n s i s t e n t with data from in vitro studies showing that GH secretion from p i t u i t a r y slices is not d i m i n i s h e d with advancing age (6). The p a r a d o x i c a l response of old rats to c o - a d m i n i s t e r e d GHRH and GHRP-6 is quite interesting. An attenuated r e s p o n s e to the coa d m i n i s t e r e d peptides would be consistent with blunted r e s p o n s e s to individually administered GHRH or GHRP-6. Instead, coa d m i n i s t r a t i o n of GHRP-6 and GHRH stimulated more GH secretion in old rats than in young rats, as if the former group were h y p e r s e n s i t i v e rather than h y p o s e n s i t i v e to the GH secretagogues. One p o s s i b l e i n t e r p r e t a t i o n of these data is that in addition to r e d u c e d GHRH secretion in old rats (12, 13), c o n c e n t r a t i o n s of an a n c i l l a r y factor that facilitates G H R H a c t i v i t y are also d i m i n i s h e d during aging. With a progressive decrease in this p u t a t i v e a n c i l l a r y factor during aging, GHRH activity w o u l d become blunted. A l t h o u g h hypothetical, the existence of a yet unidentified, endogenous analog of GHRP-6 as proposed by Bowers et al. (7), is supported by the consistent, potent and specific GH r e l e a s i n g a c t i v i t y of the hexapeptide. The reduced s e n s i t i v i t y of old rats to i n d i v i d u a l l y but not c o - a d m i n i s t e r e d GHRH and GHRP-6 suggests that the concentrations of both functionally interdependent m o l e c u l e s are d e p l e t e d during aging. REFERENCES i.

2. 3. 4.

5.

E.

GHIGO,

S. GOFFI,

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