SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2892573863> ?p ?o ?g. }

Showing items 1 to 100 of ±193 with 100 items per page.

W2892573863 endingPage "1597" @default.
W2892573863 startingPage "1582" @default.
W2892573863 abstract "Abstract The prosurvival BCL2 family member MCL1 is frequently dysregulated in cancer. To overcome the significant challenges associated with inhibition of MCL1 protein–protein interactions, we rigorously applied small-molecule conformational restriction, which culminated in the discovery of AMG 176, the first selective MCL1 inhibitor to be studied in humans. We demonstrate that MCL1 inhibition induces a rapid and committed step toward apoptosis in subsets of hematologic cancer cell lines, tumor xenograft models, and primary patient samples. With the use of a human MCL1 knock-in mouse, we demonstrate that MCL1 inhibition at active doses of AMG 176 is tolerated and correlates with clear pharmacodynamic effects, demonstrated by reductions in B cells, monocytes, and neutrophils. Furthermore, the combination of AMG 176 and venetoclax is synergistic in acute myeloid leukemia (AML) tumor models and in primary patient samples at tolerated doses. These results highlight the therapeutic promise of AMG 176 and the potential for combinations with other BH3 mimetics. Significance: AMG 176 is a potent, selective, and orally bioavailable MCL1 inhibitor that induces a rapid commitment to apoptosis in models of hematologic malignancies. The synergistic combination of AMG 176 and venetoclax demonstrates robust activity in models of AML at tolerated doses, highlighting the promise of BH3-mimetic combinations in hematologic cancers. See related commentary by Leber et al., p. 1511. This article is highlighted in the In This Issue feature, p. 1494" @default.
W2892573863 created "2018-10-05" @default.
W2892573863 creator A5001120662 @default.
W2892573863 creator A5005591514 @default.
W2892573863 creator A5009328861 @default.
W2892573863 creator A5011418864 @default.
W2892573863 creator A5014815366 @default.
W2892573863 creator A5015725755 @default.
W2892573863 creator A5016057308 @default.
W2892573863 creator A5017385944 @default.
W2892573863 creator A5017725600 @default.
W2892573863 creator A5021521707 @default.
W2892573863 creator A5021750238 @default.
W2892573863 creator A5023347212 @default.
W2892573863 creator A5023496303 @default.
W2892573863 creator A5032290146 @default.
W2892573863 creator A5033407869 @default.
W2892573863 creator A5040208750 @default.
W2892573863 creator A5041017678 @default.
W2892573863 creator A5043076936 @default.
W2892573863 creator A5043617790 @default.
W2892573863 creator A5043958558 @default.
W2892573863 creator A5045261805 @default.
W2892573863 creator A5048852631 @default.
W2892573863 creator A5049185198 @default.
W2892573863 creator A5053060128 @default.
W2892573863 creator A5053316941 @default.
W2892573863 creator A5055501408 @default.
W2892573863 creator A5056883468 @default.
W2892573863 creator A5060699951 @default.
W2892573863 creator A5060909099 @default.
W2892573863 creator A5062139061 @default.
W2892573863 creator A5064932456 @default.
W2892573863 creator A5069659291 @default.
W2892573863 creator A5082957455 @default.
W2892573863 creator A5083026456 @default.
W2892573863 creator A5085149483 @default.
W2892573863 creator A5088889740 @default.
W2892573863 creator A5091087182 @default.
W2892573863 creator A5091908601 @default.
W2892573863 date "2018-12-01" @default.
W2892573863 modified "2023-10-15" @default.
W2892573863 title "AMG 176, a Selective MCL1 Inhibitor, Is Effective in Hematologic Cancer Models Alone and in Combination with Established Therapies" @default.
W2892573863 cites W141181845 @default.
W2892573863 cites W1554671812 @default.
W2892573863 cites W1979248048 @default.
W2892573863 cites W1986615462 @default.
W2892573863 cites W1990983360 @default.
W2892573863 cites W1999549312 @default.
W2892573863 cites W2011588098 @default.
W2892573863 cites W2024216850 @default.
W2892573863 cites W2027395744 @default.
W2892573863 cites W2035296409 @default.
W2892573863 cites W2043398720 @default.
W2892573863 cites W2059416155 @default.
W2892573863 cites W2064759291 @default.
W2892573863 cites W2070375075 @default.
W2892573863 cites W2070878170 @default.
W2892573863 cites W2088883749 @default.
W2892573863 cites W2095026430 @default.
W2892573863 cites W2095095520 @default.
W2892573863 cites W2098910097 @default.
W2892573863 cites W2117692326 @default.
W2892573863 cites W2125789330 @default.
W2892573863 cites W2127287358 @default.
W2892573863 cites W2132740145 @default.
W2892573863 cites W2137240394 @default.
W2892573863 cites W2147590336 @default.
W2892573863 cites W2150048195 @default.
W2892573863 cites W2168166668 @default.
W2892573863 cites W2171224722 @default.
W2892573863 cites W2192121806 @default.
W2892573863 cites W2252711380 @default.
W2892573863 cites W2289539591 @default.
W2892573863 cites W2461928138 @default.
W2892573863 cites W2467779447 @default.
W2892573863 cites W2485824342 @default.
W2892573863 cites W2515842163 @default.
W2892573863 cites W2517675534 @default.
W2892573863 cites W2533641274 @default.
W2892573863 cites W2534349779 @default.
W2892573863 cites W2589060305 @default.
W2892573863 cites W2743418290 @default.
W2892573863 cites W2761234508 @default.
W2892573863 doi "https://doi.org/10.1158/2159-8290.cd-18-0387" @default.
W2892573863 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30254093" @default.
W2892573863 hasPublicationYear "2018" @default.
W2892573863 type Work @default.
W2892573863 sameAs 2892573863 @default.
W2892573863 citedByCount "279" @default.
W2892573863 countsByYear W28925738632018 @default.
W2892573863 countsByYear W28925738632019 @default.
W2892573863 countsByYear W28925738632020 @default.
W2892573863 countsByYear W28925738632021 @default.
W2892573863 countsByYear W28925738632022 @default.
W2892573863 countsByYear W28925738632023 @default.
W2892573863 crossrefType "journal-article" @default.
W2892573863 hasAuthorship W2892573863A5001120662 @default.