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The Role of Notch in the Cardiovascular System: Potential Adverse Effects of Investigational Notch Inhibitors

机译:Notch在心血管系统中的作用:Notch抑制剂的潜在不良反应

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摘要

Targeting the Notch pathway is a new promising therapeutic approach for cancer patients. Inhibition of Notch is effective in the oncology setting because it causes a reduction of highly proliferative tumor cells and it inhibits survival of cancer stem cells, which are considered responsible for tumor recurrence and metastasis. Additionally, since Delta-like ligand 4 (Dll4)-activated Notch signaling is a major modulator of angiogenesis, anti-Dll4 agents are being investigated to reduce vascularization of the tumor. Notch plays a major role in the heart during the development and, after birth, in response to cardiac damage. Therefore, agents used to inhibit Notch in the tumors (gamma secretase inhibitors and anti-Dll4 agents) could potentially affect myocardial repair. The past experience with trastuzumab and other tyrosine kinase inhibitors used for cancer therapy demonstrates that the possible cardiotoxicity of agents targeting shared pathways between cancer and heart and the vasculature should be considered. To date, Notch inhibition in cancer patients has resulted only in mild gastrointestinal toxicity. Little is known about the potential long-term cardiotoxicity associated to Notch inhibition in cancer patients. In this review, we will focus on mechanisms through which inhibition of Notch signaling could lead to cardiomyocytes and endothelial dysfunctions. These adverse effects could contrast with the benefits of therapeutic responses in cancer cells during times of increased cardiac stress and/or in the presence of cardiovascular risk factor.
机译:靶向Notch途径是针对癌症患者的一种新的有前途的治疗方法。 Notch的抑制作用在肿瘤学领域是有效的,因为它会导致高度增生的肿瘤细胞减少,并抑制癌干细胞的存活,而癌症干细胞被认为是造成肿瘤复发和转移的原因。另外,由于Delta样配体4(Dll4)激活的Notch信号传导是血管生成的主要调节剂,因此正在研究抗Dll4剂以减少肿瘤的血管形成。缺刻在心脏发育过程中以及出生后对心脏损伤的反应中在心脏中起主要作用。因此,用于抑制肿瘤Notch的药物(γ分泌酶抑制剂和抗Dll4药物)可能会影响心肌修复。曲妥珠单抗和其他酪氨酸激酶抑制剂用于癌症治疗的过去经验表明,应考虑靶向癌症与心脏和脉管系统之间共享途径的药物可能的心脏毒性。迄今为止,癌症患者的Notch抑制仅导致轻度的胃肠道毒性。对于癌症患者中与Notch抑制相关的潜在长期心脏毒性知之甚少。在这篇综述中,我们将重点研究抑制Notch信号传导可能导致心肌细胞和内皮功能障碍的机制。这些不良反应可能与心脏压力增加和/或存在心血管危险因素时癌细胞中治疗反应的益处形成对比。

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