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W2108771199 endingPage "2940" @default.
W2108771199 startingPage "2929" @default.
W2108771199 abstract "To examine the mechanisms of action, therapeutic potential, and challenges inherent in the use of incretin peptides and dipeptidyl peptidase-IV (DPP-IV) inhibitors for the treatment of type 2 diabetes.The scientific literature describing the biological importance of incretin peptides and DPP-IV inhibitors in the control of glucose homeostasis has been reviewed, with an emphasis on mechanisms of action, experimental diabetes, human physiological experiments, and short-term clinical studies in normal and diabetic human subjects.Glucagon-like peptide 1 (GLP-1) and glucose-dependent insulinotropic peptide (GIP) exert important effects on beta-cells to stimulate glucose-dependent insulin secretion. Both peptides also regulate beta-cell proliferation and cytoprotection. GLP-1, but not GIP, inhibits gastric emptying, glucagon secretion, and food intake. The glucose-lowering actions of GLP-1, but not GIP, are preserved in subjects with type 2 diabetes. However, native GLP-1 is rapidly degraded by DPP-IV after parenteral administration; hence, degradation-resistant, long-acting GLP-1 receptor (GLP-1R) agonists are preferable agents for the chronic treatment of human diabetes. Alternatively, inhibition of DPP-IV-mediated incretin degradation represents a complementary therapeutic approach, as orally available DPP-IV inhibitors have been shown to lower glucose in experimental diabetic models and human subjects with type 2 diabetes.GLP-1R agonists and DPP-IV inhibitors have shown promising results in clinical trials for the treatment of type 2 diabetes. The need for daily injections of potentially immunogenic GLP-1-derived peptides and the potential for unanticipated side effects with chronic use of DPP-IV inhibitors will require ongoing scrutiny of the risk-benefit ratio for these new therapies as they are evaluated in the clinic." @default.
W2108771199 created "2016-06-24" @default.
W2108771199 creator A5057472647 @default.
W2108771199 date "2003-10-01" @default.
W2108771199 modified "2023-10-11" @default.
W2108771199 title "Enhancing Incretin Action for the Treatment of Type 2 Diabetes" @default.
W2108771199 cites W1507814807 @default.
W2108771199 cites W1563993585 @default.
W2108771199 cites W1607232966 @default.
W2108771199 cites W1905803407 @default.
W2108771199 cites W1910418518 @default.
W2108771199 cites W1936375955 @default.
W2108771199 cites W1969628999 @default.
W2108771199 cites W1969932276 @default.
W2108771199 cites W1974270337 @default.
W2108771199 cites W1975756049 @default.
W2108771199 cites W1978490164 @default.
W2108771199 cites W1978953702 @default.
W2108771199 cites W1978959127 @default.
W2108771199 cites W1979916078 @default.
W2108771199 cites W1980130009 @default.
W2108771199 cites W1981001328 @default.
W2108771199 cites W1982018132 @default.
W2108771199 cites W1982227126 @default.
W2108771199 cites W1983441757 @default.
W2108771199 cites W1991477535 @default.
W2108771199 cites W1991737556 @default.
W2108771199 cites W1992411188 @default.
W2108771199 cites W1992452630 @default.
W2108771199 cites W1992966015 @default.
W2108771199 cites W1994141137 @default.
W2108771199 cites W1998141110 @default.
W2108771199 cites W1999413356 @default.
W2108771199 cites W2000465889 @default.
W2108771199 cites W2003141714 @default.
W2108771199 cites W2003380560 @default.
W2108771199 cites W2004507897 @default.
W2108771199 cites W2005334239 @default.
W2108771199 cites W2008411184 @default.
W2108771199 cites W2010208232 @default.
W2108771199 cites W2013055249 @default.
W2108771199 cites W2013082477 @default.
W2108771199 cites W2013336037 @default.
W2108771199 cites W2013851956 @default.
W2108771199 cites W2022101780 @default.
W2108771199 cites W2022964894 @default.
W2108771199 cites W2024058025 @default.
W2108771199 cites W2024409703 @default.
W2108771199 cites W2025162869 @default.
W2108771199 cites W2026348270 @default.
W2108771199 cites W2027593203 @default.
W2108771199 cites W2028479574 @default.
W2108771199 cites W2028515800 @default.
W2108771199 cites W2030005765 @default.
W2108771199 cites W2030347165 @default.
W2108771199 cites W2031468509 @default.
W2108771199 cites W2033600980 @default.
W2108771199 cites W2037839438 @default.
W2108771199 cites W2041442731 @default.
W2108771199 cites W2042845313 @default.
W2108771199 cites W2047594735 @default.
W2108771199 cites W2048876290 @default.
W2108771199 cites W2050046962 @default.
W2108771199 cites W2054564814 @default.
W2108771199 cites W2054590142 @default.
W2108771199 cites W2060949491 @default.
W2108771199 cites W2061202826 @default.
W2108771199 cites W2063693981 @default.
W2108771199 cites W2064492226 @default.
W2108771199 cites W2065867087 @default.
W2108771199 cites W2065869166 @default.
W2108771199 cites W2067710447 @default.
W2108771199 cites W2068183831 @default.
W2108771199 cites W2069375870 @default.
W2108771199 cites W2070027753 @default.
W2108771199 cites W2073099528 @default.
W2108771199 cites W2073996229 @default.
W2108771199 cites W2074956966 @default.
W2108771199 cites W2076880341 @default.
W2108771199 cites W2077791892 @default.
W2108771199 cites W2078387216 @default.
W2108771199 cites W2079220907 @default.
W2108771199 cites W2080128749 @default.
W2108771199 cites W2081392051 @default.
W2108771199 cites W2081666098 @default.
W2108771199 cites W2082070432 @default.
W2108771199 cites W2082604269 @default.
W2108771199 cites W2083447185 @default.
W2108771199 cites W2083684207 @default.
W2108771199 cites W2084142744 @default.
W2108771199 cites W2086238197 @default.
W2108771199 cites W2086437884 @default.
W2108771199 cites W2087063469 @default.
W2108771199 cites W2087707716 @default.
W2108771199 cites W2088773875 @default.
W2108771199 cites W2089109393 @default.
W2108771199 cites W2095959590 @default.
W2108771199 cites W2096716906 @default.