This study is designed as a follow up study to that performed in 2005. In the Baseline study (2005) extensive clinical whole body metabolic phenotyping was combined with in depth molecular and cellular biology analyses aimed at investigating the adipose tissue morphology as well as metabolic and inflammatory phenotypes in the adult GHD patients. Results published in (Ukropec et al., 2008) In this study identical endpoints will be investigated with the same methodology and within the same population; in order to seek relevant answers to questions on how the 6-yrs of rhGH therapy affects the * whole body insulin sensitivity * energy expenditure * body fat distribution * hepatic and skeletal muscle lipid content; as well as how it influences the adipose tissue * endocrine, * metabolic \& * inflammatory phenotypes. The strength of the planned study lies in the extensive whole body and adipose tissue phenotyping before and after the 6-year rhGH replacement therapy, that allows to determine the long-term effects of rhGH replacement therapy in GHD adults. Envisaged weakness is the limited size of the population; GHD adults (n=20); controls \[age BMI and gender matched\] (n=20). This, however, reflects \[is limited by\] the complexity of the study protocol as well as the stringency of the inclusion criteria. The clinical data obtained by methods of - integrated physiology would provide an excellent interpretation background for molecular-genetic studies at the tissue (adipose tissue) and cellular (adipocytes) level. Integration of the two could bring a new quality in the investigators understanding of metabolic derangements present in GHD, and will allow extending the investigators knowledge on the mechanisms of the long-term rhGH-therapy-induced improvement on body composition, metabolic health and the cardiovascular risk.
Study Type
OBSERVATIONAL
Enrollment
44
V th Internal Clinic, Univeristy Hospital Bratislava, Comenius University
Bratislava, Slovakia
Inst. Exp. Endocrinology Slovak Acad Sci
Bratislava, Slovakia
National Institute of Endocrinology and Diabetology
Ľubochňa, Slovakia
Effects of GH therapy to GHD adults - the whole body level
to determine the effects of a long-term (6 years) growth hormone supplementation on the whole-body metabolic phenotype in adult GHD patients (namely (i) insulin sensitivity, (ii) energy expenditure, (iii) body fat distribution and (iv) bone mineral density, (v) glucose tolerance, (vi) hepatic and skeletal muscle lipid content as well as (vii) serum lipids and (viii) inflammatory markers in circulation.
Time frame: 12 months
GH therapy effects on the endocrine, metabolic & inflammatory properties of adipose tissue
to investigate the effects of long-term (5 years) growth hormone supplementation on the subcutaneous adipose tissue (i) endocrine, (ii) metabolic and (iii) inflammatory phenotype in adult GHD patients, by extensive profiling of adipose tissue protein \& gene expression (protein antibody arrays \& real-time PCR) which could identify potential molecular mechanisms associated with abdominal obesity and insulin resistance modulated by rhGH replacement therapy.
Time frame: 2 years
comparison of GHD & control population
to compare the whole-body metabolic profile and subcutaneous adipose tissue phenotype of rhGH supplemented GHD adults with that of the healthy control group
Time frame: 2 years
Identification of the adiposity-associated parameters
to evaluate parameters associated primarily with adiposity which are largely independent on the severity of the GH deficiency
Time frame: 2 years
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