Exploring the Functional Roles of lncRNA-HOTAIR in Glioma: Unraveling its Impact on Tumor Progression

Arya Moftakhar, S. Khoshnam, D. Dayer, Maryam Farzaneh
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Abstract

Gliomas, a heterogeneous class of brain cancers, pose significant challenges as they are considered incurable. They represent the most recurrent primary intracranial cancer and exhibit distinct clinical and biological characteristics. Traditional treatment options for glioma include radiotherapy, chemotherapy, and surgery; however, the emergence of molecular-targeted therapy has provided a new avenue for improved therapeutic responses. One intriguing oncogene type of long noncoding RNAs (lncRNAs) in glioma is the HOX Transcript Antisense RNA, commonly referred to as HOTAIR. HOTAIR is characterized by its overexpression in various cancers and is situated in the intergenic region between HOXC12 and HOXC11 of the HOXC cluster on chromosome 12. Its upregulation in glioma has been found to be associated with tumor grade and plays a significant role in disease progression. HOTAIR exerts vital functions in glioma, including promoting angiogenesis, modulating glutamine catabolism, and influencing sensitivity to temozolomide (TMZ), a commonly used chemotherapy drug. Knockdown of HOTAIR has been shown to suppress cell invasion, migration, and proliferation, while inducing apoptosis, ultimately leading to tumor repression. HOTAIR achieves its biological effects, by targeting specific microRNAs (miRNAs). In this review study, we have summarized several signaling pathways that are intricately linked to HOTAIR in the context of glioma. Understanding the mechanisms and interactions involving HOTAIR and these signaling pathways may provide valuable insights for the development of targeted therapies and improved management strategies for glioma. This review provides a summary of the potential roles of HOTAIR in glioma, encompassing its effects in commercial cell lines, patient-derived cell lines, animal studies, and clinical trials.
探索lncRNA-HOTAIR在胶质瘤中的功能作用:揭示其对肿瘤进展的影响
胶质瘤是一类异质性脑癌,由于被认为是不治之症,因此带来了巨大的挑战。胶质瘤是复发率最高的颅内原发性癌症,具有独特的临床和生物学特征。胶质瘤的传统治疗方法包括放疗、化疗和手术;然而,分子靶向疗法的出现为改善治疗反应提供了新的途径。脑胶质瘤中长非编码RNA(lncRNA)的一个有趣的癌基因类型是HOX转录反义RNA,通常称为HOTAIR。HOTAIR的特点是在各种癌症中过表达,位于12号染色体HOXC簇的HOXC12和HOXC11之间的基因间区域。研究发现,它在胶质瘤中的上调与肿瘤分级有关,并在疾病进展中起着重要作用。HOTAIR 在胶质瘤中发挥着重要功能,包括促进血管生成、调节谷氨酰胺分解代谢以及影响对常用化疗药物替莫唑胺(TMZ)的敏感性。研究表明,敲除 HOTAIR 可抑制细胞的侵袭、迁移和增殖,同时诱导细胞凋亡,最终达到抑制肿瘤的目的。HOTAIR 通过靶向特定的微 RNA(miRNA)来实现其生物效应。在本综述研究中,我们总结了神经胶质瘤中与 HOTAIR 密切相关的几种信号通路。了解涉及 HOTAIR 和这些信号通路的机制和相互作用,可为开发胶质瘤靶向疗法和改进管理策略提供有价值的见解。本综述概述了 HOTAIR 在胶质瘤中的潜在作用,包括其在商业细胞系、患者衍生细胞系、动物研究和临床试验中的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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