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靶向蛋白激酶C家族的新型药物的临床前和临床开发。

Preclinical and clinical development of novel agents that target the protein kinase C family.

作者信息

Serova Maria, Ghoul Aïda, Benhadji Karim A, Cvitkovic Esteban, Faivre Sandrine, Calvo Fabien, Lokiec François, Raymond Eric

机构信息

U716, Hopital Saint-Louis, Paris, France

出版信息

Semin Oncol. 2006 Aug;33(4):466-78. doi: 10.1053/j.seminoncol.2006.04.009.

Abstract

Protein kinase C (PKC) family comprises more than 12 serine-/threonine-specific isoenzymes. PKC isoenzymes play a complex role in the transduction of signal from tyrosine kinase receptor modulating proliferation, cell cycle, apoptosis, invasion, differentiation, and senescence in both cancer cells and endothelial cells. Thereby, inhibition and/or activation of specific PKCs is thought to control tumor growth by interacting directly with cancer cells and indirectly by blocking tumor angiogenesis. Furthermore, PKCs are known to modulate multi-drug resistance, providing a rational for the combination of PKCs modulators with classical cytotoxic drugs. During the past few years, preclinical and clinical data with first-generation PKC inhibitors/activators provided insight that PKCs may indeed represent attractive targets for the discovery of small molecules with new anticancer properties. In this review, we will provide an overview on the current understanding of PKC participation in chemotherapeutic resistance, the possible implications in cancer treatment, and the potential of most recent PKC inhibitors in molecular cancer therapeutics.

摘要

蛋白激酶C(PKC)家族由12种以上的丝氨酸/苏氨酸特异性同工酶组成。PKC同工酶在酪氨酸激酶受体信号转导中发挥复杂作用,调节癌细胞和内皮细胞的增殖、细胞周期、凋亡、侵袭、分化和衰老。因此,抑制和/或激活特定的PKC被认为可通过直接与癌细胞相互作用以及间接阻断肿瘤血管生成来控制肿瘤生长。此外,已知PKC可调节多药耐药性,这为PKC调节剂与经典细胞毒性药物联合使用提供了理论依据。在过去几年中,第一代PKC抑制剂/激活剂的临床前和临床数据表明,PKC确实可能是发现具有新抗癌特性小分子的有吸引力的靶点。在本综述中,我们将概述目前对PKC参与化疗耐药性的理解、其在癌症治疗中的可能影响以及最新PKC抑制剂在分子癌症治疗中的潜力。

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