ERX-41; Promising compound by targeting LIPA is a new Achilles heel therapeutic strategy for hard-to-treat solid tumors by induction of endoplasmic reticulum stress

Q3 Medicine Vacunas Pub Date : 2023-10-01 DOI:10.1016/j.vacun.2023.06.004
Majid Eslami , Mohammad Memarian , Bahman Yousefi
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Abstract

Recently there has been an incredible shift in cancer treatment, from broad-spectrum cytotoxic drugs to targeted drugs known as small molecules and macromolecules. Although traditional therapies have been effective in cancer treatment, they often have adverse side effects due to their nonspecific action on both normal and tumor cells. The endoplasmic reticulum (ER), is known to control a variety of vital cellular processes, including protein production, folding/misfolding, and unfolding. The ER affects cell survival and death by activating the unfolded protein response (UPR) if the balance is not preserved. Dysregulation of these pathways' homeostasis in the ER is consequently linked to the emergence and development of cancer's pathological states. Therefore, targeting ER stress and ER stress-mediated apoptosis in cancer cells by small-molecule emerged as an intriguing unconventional approach that may be an effective strategy for treating cancers. This review attempts to introduce one of the newest small molecules known as ERX-41 for cancer has a poor clinical outcome strategy for solid tumors, including breast, brain, pancreatic and ovarian cancer. ERX-41 induces ER stress resulting in cell death through specific LIPA targeting. Importantly, demonstrated that ERX-41 activity is independent of LIPA lipase function but dependent on its ER localization. Mechanistically, ERX-41 binding of LIPA decreases expression of multiple ER-resident proteins involved in protein folding and induce ER stress. This molecules targeted approach has a large therapeutic window, with no adverse effects either on normal cells and leading of new Achilles heel discovery in the therapeutics development for multiple hard-to-treat solid tumors.

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ERX-41;靶向LIPA的化合物是通过诱导内质网应激治疗难治性实体瘤的一个新的致命弱点
最近,癌症治疗发生了令人难以置信的转变,从广谱细胞毒性药物到被称为小分子和大分子的靶向药物。虽然传统疗法在癌症治疗中是有效的,但由于它们对正常细胞和肿瘤细胞的非特异性作用,往往会产生不良的副作用。众所周知,内质网(ER)控制着多种重要的细胞过程,包括蛋白质产生、折叠/错误折叠和展开。如果不保持平衡,内质网通过激活未折叠蛋白反应(UPR)来影响细胞的生存和死亡。因此,内质网中这些通路的稳态失调与癌症病理状态的出现和发展有关。因此,通过小分子靶向内质网应激和内质网应激介导的癌细胞凋亡成为一种有趣的非常规方法,可能是治疗癌症的有效策略。这篇综述试图介绍一种被称为ERX-41的最新小分子,它对包括乳腺癌、脑癌、胰腺癌和卵巢癌在内的实体肿瘤的临床疗效不佳。ERX-41通过特异性靶向LIPA诱导内质网应激导致细胞死亡。重要的是,证明了ERX-41活性独立于LIPA脂肪酶功能,但依赖于其内质网定位。在机制上,ERX-41结合LIPA降低了参与蛋白质折叠的多种内质网驻留蛋白的表达,并诱导内质网应激。这种分子靶向方法具有很大的治疗窗口,对正常细胞没有不良反应,并且在多种难以治疗的实体瘤的治疗开发中引领新的阿喀琉斯之踵的发现。
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来源期刊
Vacunas
Vacunas Medicine-Infectious Diseases
CiteScore
3.90
自引率
0.00%
发文量
138
审稿时长
62 days
期刊介绍: Sin duda una de las mejores publicaciones para conocer los avances en el campo de las vacunaciones preventivas, tanto en el ámbito de la investigación básica como aplicada y en la evaluación de programas de vacunaciones. Su alta calidad y utilidad la ha llevado a estar indexada en los prestigiosos índices IME y SCOPUS.
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