Proteomic profiling of growth hormone-responsive proteins in human peripheral blood leukocytes

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Abstract

Context: GH is a known modulator of the immune system, but the effect of exogenous GH administration on white blood cell proteins has not been investigated. Surface-enhanced laser desorption/ionization time-of-flight mass spectrometry (SELDI-TOF MS) is a powerful platform for the study of GH effects on immune system proteins. Objective: Our objective was to explore a novel approach for the detection of GH-responsive proteins in human leukocytes by proteomic analysis using SELDI-TOF MS. Design: We conducted a randomized double-blind, placebo-controlled GH administration study of 8 wk treatment followed by 6 wk washout. Pre- and posttreatment samples from 30 subjects were used for biomarker discovery. Setting: The study was performed at a clinical research facility. Participants: We studied 30 recreationally trained healthy athletes. Intervention: Subjects received either recombinant human GH (2 mg/d sc; n = 22) or placebo (n = 8) for 8 wk. Main Outcome Measures: Proteomic profiles were determined using CM10 weak cation-exchange protein chips, and some GH-regulated proteins were purified and identified by mass spectrometry and/or immunoblotting. Results: SELDI-TOF analysis revealed a number of GH-regulated peptides/proteins in the 3- to 22-kDa range that are either up- or down-regulated by GH. Several of these may be useful as biomarkers of GH action. The calcium-binding, proinflammatory calgranulins S100A8, S100A9, and S100A12 were all significantly down-regulated in response to GH treatment. Conclusion: This study illustrates the novel use of human leukocyte proteomic profiling by SELDI-TOF MS and reveals the negative regulation of proinflammatory S100 proteins by GH in human white blood cells. Copyright © 2009 by The Endocrine Society.

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Chung, L., Nelson, A. E., Ho, K. K. Y., & Baxter, R. C. (2009). Proteomic profiling of growth hormone-responsive proteins in human peripheral blood leukocytes. Journal of Clinical Endocrinology and Metabolism, 94(8), 3038–3043. https://doi.org/10.1210/jc.2009-0778

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