1999
DOI: 10.1139/z99-162
|View full text |Cite
|
Sign up to set email alerts
|

The growth hormone axis, feeding, and central allocative regulation: lessons from giant transgenic growth hormone mice

Abstract: Lifetime consumption rates of male transgenic growth hormone (GH) mice and normal controls were measured on either a 38% protein diet (HP), the standard rodent diet (STD) (23.5% protein), or the standard diet supplemented with a free choice of sucrose (CARB). On STD, daily intake of normal mice increased little at sizes greater than 20 g, but larger transgenic mice ate progressively more. Both kinds of mice showed declining daily mass-specific consumption with increasing age. Transgenic mice consistently ate 1… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
1
1

Citation Types

0
2
0

Year Published

2008
2008
2020
2020

Publication Types

Select...
5
1

Relationship

0
6

Authors

Journals

citations
Cited by 11 publications
(2 citation statements)
references
References 139 publications
(206 reference statements)
0
2
0
Order By: Relevance
“…Further support for a relationship between small body size and longevity is derived from reports showing that mice selected for reduced body sizes live longer (Roberts, 1961). In contrast to GH or IGF-1 deficiencies, animals overexpressing GH are significantly larger (30–60%) than wild-type controls (Shea et al, 1987; Wanke et al, 1992; Rollo et al, 1999). de Magalhães et al (2005) used Gompertz analysis to show that GH and the GH receptor statistically influence aging, while IGF1R and the insulin receptor (IR) do not.…”
Section: Gh Growth and Body Sizementioning
confidence: 90%
See 1 more Smart Citation
“…Further support for a relationship between small body size and longevity is derived from reports showing that mice selected for reduced body sizes live longer (Roberts, 1961). In contrast to GH or IGF-1 deficiencies, animals overexpressing GH are significantly larger (30–60%) than wild-type controls (Shea et al, 1987; Wanke et al, 1992; Rollo et al, 1999). de Magalhães et al (2005) used Gompertz analysis to show that GH and the GH receptor statistically influence aging, while IGF1R and the insulin receptor (IR) do not.…”
Section: Gh Growth and Body Sizementioning
confidence: 90%
“…As mentioned previously, reproductive senescence occurs earlier in transgenic mice with infertility appearing at 5–7 months of age (Bartke et al, 1994). Declines in cognitive function have also been observed at much younger ages in GH transgenic mice (Meliska et al, 1997; Rollo et al, 1999). Finally, evidence that cells from GH transgenic mice exhibit a reduced capacity to replicate is also consistent with accelerated aging (Pendergrass et al, 1993).…”
Section: Delayed and Premature Agingmentioning
confidence: 95%