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一种受体酪氨酸激酶 ROR1 抑制剂(KAN0439834)可诱导胰腺细胞发生显著的凋亡,厄洛替尼和伊布替尼可增强这种作用。

A receptor tyrosine kinase ROR1 inhibitor (KAN0439834) induced significant apoptosis of pancreatic cells which was enhanced by erlotinib and ibrutinib.

机构信息

Department of Oncology-Pathology, Immune and Gene therapy Lab, Cancer Center Karolinska (CCK), Karolinska University Hospital Solna, Stockholm, Sweden.

Karolinska Institutet, Stockholm, Sweden.

出版信息

PLoS One. 2018 Jun 1;13(6):e0198038. doi: 10.1371/journal.pone.0198038. eCollection 2018.

DOI:10.1371/journal.pone.0198038
PMID:29856777
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5983484/
Abstract

There is a great unmet medical need in pancreatic carcinoma (PC) for novel drugs with other mechanisms of action than existing. PC cells express the onco-fetal RTK ROR1, absent on most normal post-partem cells. ROR1 is involved in proliferation, survival, EMT and metastasis of tumor cells in various malignancies. A small molecule inhibitor (KAN0439834) (530 Da) targeting the TK domain of ROR1 was developed and the activity in ROR1 expressing human PC cell lines (n = 8) evaluated. The effects were compared to a murine mAb against the external part of ROR1, gemcitabine, erlotinib and ibrutinib. KAN0439834 induced significant apoptosis of the tumor cells. EC50 values for KAN0439834 varied between 250-650 nM depending on the cell line. The corresponding values for erlotinib and ibrutinib were 10-40 folds higher. KAN0439834 was much more effective in inducing tumor cell death than the ROR1 mAb although both inhibited ROR1 phosphorylation and downstream non-canonical Wnt pathway molecules. Combination of KAN0439834 with erlotinib or ibrutinib had significant additive effects on tumor cell death. A first-in-class small molecule ROR1 inhibitor (KAN0439834) showed promising in vitro activity against a number of human PC cell lines. Interesting is the additive effects of erlotinib and ibrutinib which warrants further studies as both these agents are in clinical trials for pancreatic carcinoma.

摘要

在胰腺癌(PC)中,存在着对具有不同于现有药物作用机制的新型药物的巨大未满足的医学需求。PC 细胞表达肿瘤发生的 RTK ROR1,而大多数正常产后细胞都不表达。ROR1 参与多种恶性肿瘤中肿瘤细胞的增殖、存活、上皮间质转化和转移。开发了一种针对 ROR1 TK 结构域的小分子抑制剂(KAN0439834)(530 Da),并评估了其在表达 ROR1 的人 PC 细胞系(n = 8)中的活性。将其与针对 ROR1 外部部分的鼠单克隆抗体、吉西他滨、厄洛替尼和伊布替尼进行了比较。KAN0439834 可诱导肿瘤细胞发生显著凋亡。KAN0439834 的 EC50 值因细胞系而异,范围为 250-650 nM。厄洛替尼和伊布替尼的相应值高 10-40 倍。虽然 KAN0439834 和 ROR1 单克隆抗体均能抑制 ROR1 磷酸化和下游非经典 Wnt 途径分子,但 KAN0439834 诱导肿瘤细胞死亡的效果要比 ROR1 单克隆抗体好得多。KAN0439834 与厄洛替尼或伊布替尼联合使用对肿瘤细胞死亡具有显著的相加作用。一种新型的 ROR1 小分子抑制剂(KAN0439834)在体外对多种人 PC 细胞系表现出有前景的活性。有趣的是,厄洛替尼和伊布替尼具有相加作用,这值得进一步研究,因为这两种药物都在胰腺癌的临床试验中。

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