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W2794172851 endingPage "686" @default.
W2794172851 startingPage "686" @default.
W2794172851 abstract "Human islet amyloid peptide (hIAPP1–37) aggregation is an early step in Diabetes Mellitus. We aimed to evaluate a family of pharmaco-chaperones to act as modulators that provide dynamic interventions and the multi-target capacity (native state, cytotoxic oligomers, protofilaments and fibrils of hIAPP1–37) required to meet the treatment challenges of diabetes. We used a cross-functional approach that combines in silico and in vitro biochemical and biophysical methods to study the hIAPP1–37 aggregation-oligomerization process as to reveal novel potential anti-diabetic drugs. The family of pharmaco-chaperones are modulators of the oligomerization and fibre formation of hIAPP1–37. When they interact with the amino acid in the amyloid-like steric zipper zone, they inhibit and/or delay the aggregation-oligomerization pathway by binding and stabilizing several amyloid structures of hIAPP1–37. Moreover, they can protect cerebellar granule cells (CGC) from the cytotoxicity produced by the hIAPP1–37 oligomers. The modulation of proteostasis by the family of pharmaco-chaperones A–F is a promising potential approach to limit the onset and progression of diabetes and its comorbidities." @default.
W2794172851 created "2018-03-29" @default.
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W2794172851 date "2018-03-19" @default.
W2794172851 modified "2023-10-18" @default.
W2794172851 title "Diabetes Drug Discovery: hIAPP1–37 Polymorphic Amyloid Structures as Novel Therapeutic Targets" @default.
W2794172851 cites W1592702941 @default.
W2794172851 cites W1608054934 @default.
W2794172851 cites W1608388154 @default.
W2794172851 cites W1963764130 @default.
W2794172851 cites W1971108880 @default.
W2794172851 cites W1981458288 @default.
W2794172851 cites W1987066756 @default.
W2794172851 cites W1987112434 @default.
W2794172851 cites W1988745994 @default.
W2794172851 cites W1989018026 @default.
W2794172851 cites W1990634143 @default.
W2794172851 cites W2005279391 @default.
W2794172851 cites W2007031655 @default.
W2794172851 cites W2015243877 @default.
W2794172851 cites W2016333334 @default.
W2794172851 cites W2023035838 @default.
W2794172851 cites W2026516238 @default.
W2794172851 cites W2032605307 @default.
W2794172851 cites W2050891813 @default.
W2794172851 cites W2053095574 @default.
W2794172851 cites W2059490702 @default.
W2794172851 cites W2061111679 @default.
W2794172851 cites W2064367582 @default.
W2794172851 cites W2066777346 @default.
W2794172851 cites W2075784917 @default.
W2794172851 cites W2084981109 @default.
W2794172851 cites W2092797538 @default.
W2794172851 cites W2098651156 @default.
W2794172851 cites W2098953186 @default.
W2794172851 cites W2099999454 @default.
W2794172851 cites W2109803055 @default.
W2794172851 cites W2115168896 @default.
W2794172851 cites W2121963977 @default.
W2794172851 cites W2121977115 @default.
W2794172851 cites W2124745408 @default.
W2794172851 cites W2126160318 @default.
W2794172851 cites W2132629607 @default.
W2794172851 cites W2133762037 @default.
W2794172851 cites W2134688994 @default.
W2794172851 cites W2134967712 @default.
W2794172851 cites W2135706939 @default.
W2794172851 cites W2136885518 @default.
W2794172851 cites W2143546709 @default.
W2794172851 cites W2143599576 @default.
W2794172851 cites W2144481414 @default.
W2794172851 cites W2148869006 @default.
W2794172851 cites W2149084010 @default.
W2794172851 cites W2152446161 @default.
W2794172851 cites W2152696868 @default.
W2794172851 cites W2156135176 @default.
W2794172851 cites W2157104650 @default.
W2794172851 cites W2157733093 @default.
W2794172851 cites W2157767457 @default.
W2794172851 cites W2159879659 @default.
W2794172851 cites W2163210644 @default.
W2794172851 cites W2165186407 @default.
W2794172851 cites W2166138110 @default.
W2794172851 cites W2265775199 @default.
W2794172851 cites W2313725855 @default.
W2794172851 cites W2376076274 @default.
W2794172851 cites W2412921526 @default.
W2794172851 cites W2544936306 @default.
W2794172851 cites W2555151293 @default.
W2794172851 cites W2560598375 @default.
W2794172851 cites W2570218327 @default.
W2794172851 cites W2606042337 @default.
W2794172851 cites W2614053601 @default.
W2794172851 cites W2619698442 @default.
W2794172851 cites W2754610788 @default.
W2794172851 cites W2778757226 @default.
W2794172851 cites W4240929891 @default.
W2794172851 cites W746491878 @default.
W2794172851 cites W97810949 @default.
W2794172851 cites W98713150 @default.
W2794172851 doi "https://doi.org/10.3390/molecules23030686" @default.
W2794172851 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6017868" @default.