FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W3138188841> ?p ?o ?g. }

• W3138188841 endingPage "100588" @default.
• W3138188841 startingPage "100588" @default.
• W3138188841 abstract "Excess circulating human growth hormone (hGH) in vivo is linked to metabolic and growth disorders such as cancer, diabetes, and acromegaly. Consequently, there is considerable interest in developing antagonists of hGH action. Here, we present the design, synthesis, and characterization of a 16-residue peptide (site 1-binding helix [S1H]) that inhibits hGH-mediated STAT5 phosphorylation in cultured cells. S1H was designed as a direct sequence mimetic of the site 1 mini-helix (residues 36-51) of wild-type hGH and acts by inhibiting the interaction of hGH with the human growth hormone receptor (hGHR). In vitro studies indicated that S1H is stable in human serum and can adopt an α-helix in solution. Our results also show that S1H mitigates phosphorylation of STAT5 in cells co-treated with hGH, reducing intracellular STAT5 phosphorylation levels to those observed in untreated controls. Furthermore, S1H was found to attenuate the activity of the hGHR and the human prolactin receptor, suggesting that this peptide acts as an antagonist of both lactogenic and somatotrophic hGH actions. Finally, we used alanine scanning to determine how discrete amino acids within the S1H sequence contribute to its structural organization and biological activity. We observed a strong correlation between helical propensity and inhibitory effect, indicating that S1H-mediated antagonism of the hGHR is largely dependent on the ability for S1H to adopt an α-helix. Taken together, these results show that S1H not only acts as a novel peptide-based antagonist of the hGHR but can also be applied as a chemical tool to study the molecular nature of hGH-hGHR interactions." @default.
• W3138188841 created "2021-03-29" @default.
• W3138188841 creator A5006324003 @default.
• W3138188841 creator A5006509292 @default.
• W3138188841 creator A5009748504 @default.
• W3138188841 creator A5016311750 @default.
• W3138188841 creator A5016579200 @default.
• W3138188841 creator A5051496336 @default.
• W3138188841 creator A5054006122 @default.
• W3138188841 creator A5078161645 @default.
• W3138188841 creator A5079803843 @default.
• W3138188841 date "2021-01-01" @default.
• W3138188841 modified "2023-10-17" @default.
• W3138188841 title "A novel peptide antagonist of the human growth hormone receptor" @default.
• W3138188841 cites W1526003658 @default.
• W3138188841 cites W1540649941 @default.
• W3138188841 cites W1550443678 @default.
• W3138188841 cites W1578549298 @default.
• W3138188841 cites W1602803234 @default.
• W3138188841 cites W1616430665 @default.
• W3138188841 cites W1619897426 @default.
• W3138188841 cites W1624756048 @default.
• W3138188841 cites W1659717266 @default.
• W3138188841 cites W1966537913 @default.
• W3138188841 cites W1967083598 @default.
• W3138188841 cites W1967293063 @default.
• W3138188841 cites W1969541617 @default.
• W3138188841 cites W1970072631 @default.
• W3138188841 cites W1970417043 @default.
• W3138188841 cites W1974058125 @default.
• W3138188841 cites W1982685226 @default.
• W3138188841 cites W1983169511 @default.
• W3138188841 cites W1984390200 @default.
• W3138188841 cites W1985594739 @default.
• W3138188841 cites W1985832876 @default.
• W3138188841 cites W1991462498 @default.
• W3138188841 cites W1999253307 @default.
• W3138188841 cites W2000814339 @default.
• W3138188841 cites W2000909542 @default.
• W3138188841 cites W2002375890 @default.
• W3138188841 cites W2003099132 @default.
• W3138188841 cites W2007701065 @default.
• W3138188841 cites W2012711566 @default.
• W3138188841 cites W2013937244 @default.
• W3138188841 cites W2014762505 @default.
• W3138188841 cites W2016086328 @default.
• W3138188841 cites W2021293246 @default.
• W3138188841 cites W2023161917 @default.
• W3138188841 cites W2023966921 @default.
• W3138188841 cites W2024376357 @default.
• W3138188841 cites W2025206161 @default.
• W3138188841 cites W2025864476 @default.
• W3138188841 cites W2028501050 @default.
• W3138188841 cites W2034849961 @default.
• W3138188841 cites W2037226702 @default.
• W3138188841 cites W2037455416 @default.
• W3138188841 cites W2038910312 @default.
• W3138188841 cites W2039356047 @default.
• W3138188841 cites W2040051585 @default.
• W3138188841 cites W2041323282 @default.
• W3138188841 cites W2044395145 @default.
• W3138188841 cites W2049708286 @default.
• W3138188841 cites W2066303865 @default.
• W3138188841 cites W2068187158 @default.
• W3138188841 cites W2073469490 @default.
• W3138188841 cites W2079774691 @default.
• W3138188841 cites W2079952304 @default.
• W3138188841 cites W2080846291 @default.
• W3138188841 cites W2081177490 @default.
• W3138188841 cites W2085178300 @default.
• W3138188841 cites W2087945165 @default.
• W3138188841 cites W2099540110 @default.
• W3138188841 cites W2100118978 @default.
• W3138188841 cites W2100543510 @default.
• W3138188841 cites W2108401203 @default.
• W3138188841 cites W2109066322 @default.
• W3138188841 cites W2113464653 @default.
• W3138188841 cites W2114512254 @default.
• W3138188841 cites W2114836473 @default.
• W3138188841 cites W2116102682 @default.
• W3138188841 cites W2120385383 @default.
• W3138188841 cites W2128667978 @default.
• W3138188841 cites W2130617666 @default.
• W3138188841 cites W2130904570 @default.
• W3138188841 cites W2130988832 @default.
• W3138188841 cites W2140553751 @default.
• W3138188841 cites W2143010144 @default.
• W3138188841 cites W2144901932 @default.
• W3138188841 cites W2151427219 @default.
• W3138188841 cites W2155433930 @default.
• W3138188841 cites W2156136676 @default.
• W3138188841 cites W2156435407 @default.
• W3138188841 cites W2159303404 @default.
• W3138188841 cites W2161634174 @default.
• W3138188841 cites W2164270899 @default.
• W3138188841 cites W2164597119 @default.
• W3138188841 cites W2166679494 @default.
• W3138188841 cites W2168059460 @default.

• next