| Literature DB >> 36253486 |
Yu-Yi Chu1, Mei-Kuang Chen1,2, Yongkun Wei1, Heng-Huan Lee1, Weiya Xia1,3, Ying-Nai Wang1, Clinton Yam1,2,4, Jennifer L Hsu1, Hung-Ling Wang3, Wei-Chao Chang3, Hirohito Yamaguchi1,3, Zhou Jiang1, Chunxiao Liu1, Ching-Fei Li1, Lei Nie1, Li-Chuan Chan1, Yuan Gao1,5, Shao-Chun Wang3, Jinsong Liu6, Shannon N Westin7, Sanghoon Lee8, Anil K Sood7,9, Liuqing Yang1, Gabriel N Hortobagyi4, Dihua Yu10, Mien-Chie Hung11,12,13.
Abstract
Poly(ADP-ribose) polymerase (PARP) inhibitors have demonstrated promising clinical activity in multiple cancers. However, resistance to PARP inhibitors remains a substantial clinical challenge. In the present study, we report that anaplastic lymphoma kinase (ALK) directly phosphorylates CDK9 at tyrosine-19 to promote homologous recombination (HR) repair and PARP inhibitor resistance. Phospho-CDK9-Tyr19 increases its kinase activity and nuclear localization to stabilize positive transcriptional elongation factor b and activate polymerase II-dependent transcription of HR-repair genes. Conversely, ALK inhibition increases ubiquitination and degradation of CDK9 by Skp2, an E3 ligase. Notably, combination of US Food and Drug Administration-approved ALK and PARP inhibitors markedly reduce tumor growth and improve survival of mice in PARP inhibitor-/platinum-resistant tumor xenograft models. Using human tumor biospecimens, we further demonstrate that phosphorylated ALK (p-ALK) expression is associated with resistance to PARP inhibitors and positively correlated with p-Tyr19-CDK9 expression. Together, our findings support a biomarker-driven, combinatorial treatment strategy involving ALK and PARP inhibitors to induce synthetic lethality in PARP inhibitor-/platinum-resistant tumors with high p-ALK-p-Tyr19-CDK9 expression.Entities:
Year: 2022 PMID: 36253486 PMCID: PMC9586872 DOI: 10.1038/s43018-022-00438-2
Source DB: PubMed Journal: Nat Cancer ISSN: 2662-1347