SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2108803513> ?p ?o ?g. }

Showing items 1 to 100 of ±186 with 100 items per page.

W2108803513 endingPage "1271" @default.
W2108803513 startingPage "1263" @default.
W2108803513 abstract "Many patients with diabetes mellitus (both type 1 and type 2) require therapy to maintain normal fasting glucose levels. To develop a novel treatment for these individuals, we used phage display technology to target the insulin receptor (INSR) complexed with insulin and identified a high affinity, allosteric, human monoclonal antibody, XMetA, which mimicked the glucoregulatory, but not the mitogenic, actions of insulin. Biophysical studies with cultured cells expressing human INSR demonstrated that XMetA acted allosterically and did not compete with insulin for binding to its receptor. XMetA was found to function as a specific partial agonist of INSR, eliciting tyrosine phosphorylation of INSR but not the IGF-IR. Although this antibody activated metabolic signaling, leading to enhanced glucose uptake, it neither activated Erk nor induced proliferation of cancer cells. In an insulin resistant, insulinopenic model of diabetes, XMetA markedly reduced elevated fasting blood glucose and normalized glucose tolerance. After 6 weeks, significant improvements in HbA(1c), dyslipidemia, and other manifestations of diabetes were observed. It is noteworthy that hypoglycemia and weight gain were not observed during these studies. These studies indicate, therefore, that allosteric monoclonal antibodies have the potential to be novel, ultra-long acting, agents for the regulation of hyperglycemia in diabetes." @default.
W2108803513 created "2016-06-24" @default.
W2108803513 creator A5010219228 @default.
W2108803513 creator A5011106965 @default.
W2108803513 creator A5014336410 @default.
W2108803513 creator A5017532271 @default.
W2108803513 creator A5024581015 @default.
W2108803513 creator A5024753004 @default.
W2108803513 creator A5025383668 @default.
W2108803513 creator A5028875663 @default.
W2108803513 creator A5029161401 @default.
W2108803513 creator A5031837060 @default.
W2108803513 creator A5032412677 @default.
W2108803513 creator A5033422964 @default.
W2108803513 creator A5036443339 @default.
W2108803513 creator A5040935030 @default.
W2108803513 creator A5042476590 @default.
W2108803513 creator A5060943418 @default.
W2108803513 creator A5063619714 @default.
W2108803513 creator A5078072251 @default.
W2108803513 creator A5082701819 @default.
W2108803513 creator A5085817398 @default.
W2108803513 creator A5089579825 @default.
W2108803513 creator A5090235621 @default.
W2108803513 creator A5091189105 @default.
W2108803513 date "2012-04-13" @default.
W2108803513 modified "2023-10-18" @default.
W2108803513 title "A Fully Human, Allosteric Monoclonal Antibody That Activates the Insulin Receptor and Improves Glycemic Control" @default.
W2108803513 cites W124828924 @default.
W2108803513 cites W1535069478 @default.
W2108803513 cites W1652063548 @default.
W2108803513 cites W1827566752 @default.
W2108803513 cites W1953369200 @default.
W2108803513 cites W1963637633 @default.
W2108803513 cites W1977448657 @default.
W2108803513 cites W1985190943 @default.
W2108803513 cites W1985469212 @default.
W2108803513 cites W1994890616 @default.
W2108803513 cites W1998493448 @default.
W2108803513 cites W2001751915 @default.
W2108803513 cites W2003590414 @default.
W2108803513 cites W2006661094 @default.
W2108803513 cites W2009033372 @default.
W2108803513 cites W2017504609 @default.
W2108803513 cites W2021010709 @default.
W2108803513 cites W2022749561 @default.
W2108803513 cites W2047906693 @default.
W2108803513 cites W2050573411 @default.
W2108803513 cites W2051313176 @default.
W2108803513 cites W2058431467 @default.
W2108803513 cites W2059082073 @default.
W2108803513 cites W2062078854 @default.
W2108803513 cites W2063345836 @default.
W2108803513 cites W2066578460 @default.
W2108803513 cites W2075197583 @default.
W2108803513 cites W2084559524 @default.
W2108803513 cites W2087454504 @default.
W2108803513 cites W2091235742 @default.
W2108803513 cites W2093862846 @default.
W2108803513 cites W2096773810 @default.
W2108803513 cites W2100554558 @default.
W2108803513 cites W2109728760 @default.
W2108803513 cites W2112447641 @default.
W2108803513 cites W2119625160 @default.
W2108803513 cites W2121879147 @default.
W2108803513 cites W2126113812 @default.
W2108803513 cites W2130859056 @default.
W2108803513 cites W2132554143 @default.
W2108803513 cites W2150037154 @default.
W2108803513 cites W2153881169 @default.
W2108803513 cites W2163098588 @default.
W2108803513 cites W2306142335 @default.
W2108803513 cites W2334309509 @default.
W2108803513 cites W2340100375 @default.
W2108803513 doi "https://doi.org/10.2337/db11-1578" @default.
W2108803513 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/3331746" @default.
W2108803513 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/22403294" @default.
W2108803513 hasPublicationYear "2012" @default.
W2108803513 type Work @default.
W2108803513 sameAs 2108803513 @default.
W2108803513 citedByCount "61" @default.
W2108803513 countsByYear W21088035132012 @default.
W2108803513 countsByYear W21088035132013 @default.
W2108803513 countsByYear W21088035132014 @default.
W2108803513 countsByYear W21088035132015 @default.
W2108803513 countsByYear W21088035132016 @default.
W2108803513 countsByYear W21088035132017 @default.
W2108803513 countsByYear W21088035132018 @default.
W2108803513 countsByYear W21088035132019 @default.
W2108803513 countsByYear W21088035132020 @default.
W2108803513 countsByYear W21088035132021 @default.
W2108803513 countsByYear W21088035132022 @default.
W2108803513 countsByYear W21088035132023 @default.
W2108803513 crossrefType "journal-article" @default.
W2108803513 hasAuthorship W2108803513A5010219228 @default.
W2108803513 hasAuthorship W2108803513A5011106965 @default.
W2108803513 hasAuthorship W2108803513A5014336410 @default.
W2108803513 hasAuthorship W2108803513A5017532271 @default.