Dakal Tikam Chand, Bhushan Ravi, Xu Caiming, Gadi Bhana Ram, Cameotra Swaranjit Singh, Yadav Vikas, Maciaczyk Jarek, Schmidt-Wolf Ingo G H, Kumar Abhishek, Sharma Amit
Genome and Computational Biology Lab Department of Biotechnology Mohanlal Sukhadia University Udaipur Rajasthan India.
Department of Zoology M.S. College Motihari Bihar India.
MedComm (2020). 2024 Sep 21;5(10):e710. doi: 10.1002/mco2.710. eCollection 2024 Oct.
Cancer stem cells (CSCs) are widely acknowledged as the drivers of tumor initiation, epithelial-mesenchymal transition (EMT) progression, and metastasis. Originating from both hematologic and solid malignancies, CSCs exhibit quiescence, pluripotency, and self-renewal akin to normal stem cells, thus orchestrating tumor heterogeneity and growth. Through a dynamic interplay with the tumor microenvironment (TME) and intricate signaling cascades, CSCs undergo transitions from differentiated cancer cells, culminating in therapy resistance and disease recurrence. This review undertakes an in-depth analysis of the multifaceted mechanisms underlying cancer stemness and CSC-mediated resistance to therapy. Intrinsic factors encompassing the TME, hypoxic conditions, and oxidative stress, alongside extrinsic processes such as drug efflux mechanisms, collectively contribute to therapeutic resistance. An exploration into key signaling pathways, including JAK/STAT, WNT, NOTCH, and HEDGEHOG, sheds light on their pivotal roles in sustaining CSCs phenotypes. Insights gleaned from preclinical and clinical studies hold promise in refining drug discovery efforts and optimizing therapeutic interventions, especially chimeric antigen receptor (CAR)-T cell therapy, cytokine-induced killer (CIK) cell therapy, natural killer (NK) cell-mediated CSC-targeting and others. Ultimately use of cell sorting and single cell sequencing approaches for elucidating the fundamental characteristics and resistance mechanisms inherent in CSCs will enhance our comprehension of CSC and intratumor heterogeneity, which ultimately would inform about tailored and personalized interventions.
癌症干细胞(CSCs)被广泛认为是肿瘤起始、上皮-间质转化(EMT)进展和转移的驱动因素。CSCs起源于血液系统恶性肿瘤和实体恶性肿瘤,具有类似于正常干细胞的静止、多能性和自我更新能力,从而导致肿瘤异质性和生长。通过与肿瘤微环境(TME)的动态相互作用和复杂的信号级联反应,CSCs从分化的癌细胞转变而来,最终导致治疗耐药性和疾病复发。本综述对癌症干性和CSC介导的治疗耐药性的多方面机制进行了深入分析。包括TME、缺氧条件和氧化应激在内的内在因素,以及药物外排机制等外在过程,共同导致了治疗耐药性。对关键信号通路的探索,包括JAK/STAT、WNT、NOTCH和HEDGEHOG,揭示了它们在维持CSCs表型中的关键作用。从临床前和临床研究中获得的见解有望改进药物发现工作并优化治疗干预措施,特别是嵌合抗原受体(CAR)-T细胞疗法、细胞因子诱导的杀伤(CIK)细胞疗法、自然杀伤(NK)细胞介导的CSC靶向治疗等。最终,使用细胞分选和单细胞测序方法来阐明CSCs固有的基本特征和耐药机制,将增强我们对CSC和肿瘤内异质性的理解,这最终将为定制化和个性化干预提供依据。
