Therapeutic Targeting of NOTCH1 Signaling in T-Cell Acute Lymphoblastic Leukemia

Teresa Palomero , Adolfo Ferrando
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引用次数: 66

Abstract

The recent identification of activating mutations in NOTCH1 in the majority of T-cell acute lymphoblastic leukemias (T-ALLs) has brought major interest toward targeting the NOTCH signaling pathway in this disease. Small-molecule γ-secretase inhibitors (GSIs), which block a critical proteolytic step required for NOTCH1 activation, can effectively block the activity of NOTCH1 mutant alleles. However, the clinical development of GSIs has been hampered by their low cytotoxicity against human T-ALL and the development of significant gastrointestinal toxicity derived from the inhibition of NOTCH signaling in the gut. Improved understanding of the oncogenic mechanisms of NOTCH1 and the effects of NOTCH inhibition in leukemic cells and the intestinal epithelium are required for the design of effective anti-NOTCH1 therapies in T-ALL.

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NOTCH1信号在t细胞急性淋巴细胞白血病中的靶向治疗
最近在大多数t细胞急性淋巴细胞白血病(t - all)中发现NOTCH1激活突变,这使人们对靶向NOTCH信号通路在该疾病中的作用产生了重大兴趣。小分子γ-分泌酶抑制剂(GSIs)阻断NOTCH1激活所需的关键蛋白水解步骤,可以有效阻断NOTCH1突变等位基因的活性。然而,gsi的临床发展一直受到其对人类T-ALL的低细胞毒性和肠道中NOTCH信号抑制引起的显著胃肠道毒性的阻碍。更好地了解NOTCH1的致癌机制以及NOTCH抑制在白血病细胞和肠上皮中的作用,是设计T-ALL有效的抗NOTCH1疗法的必要条件。
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