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Dendritic cell engineering for selective targeting of female reproductive tract cancers

机译:树突状细胞工程技术可选择性靶向女性生殖道癌症

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摘要

Female reproductive tract cancers (FRCs) are considered as one of the most frequently occurring malignancies and a foremost cause of death among women. The late-stage diagnosis and limited clinical effectiveness of currently available mainstay therapies, primarily due to the developed drug resistance properties of tumour cells, further increase disease severity. In the past decade, dendritic cell (DC)-based immunotherapy has shown remarkable success and appeared as a feasible therapeutic alternative to treat several malignancies, including FRCs. Importantly, the clinical efficacy of this therapy is shown to be restricted by the established immunosuppressive tumour microenvironment. However, combining nanoengineered approaches can significantly assist DCs to overcome this tumour-induced immune tolerance. The prolonged release of nanoencapsulated tumour antigens helps improve the ability of DC-based therapeutics to selectively target and remove residual tumour cells. Incorporation of surface ligands and co-adjuvants may further aid DC targeting (in vivo) to overcome the issues associated with the short DC lifespan, immunosuppression and imprecise uptake. We herein briefly discuss the necessity and progress of DC-based therapeutics in FRCs. The review also sheds lights on the future challenges to design and develop clinically effective nanoparticles-DC combinations that can induce efficient anti-tumour immune responses and prolong patients’ survival.
机译:女性生殖道癌症(FRC)被认为是最常见的恶性肿瘤之一,也是女性死亡的首要原因。主要由于肿瘤细胞已形成的耐药性,导致目前可用的主流疗法的后期诊断和有限的临床有效性,进一步加剧了疾病的严重性。在过去的十年中,基于树突状细胞(DC)的免疫疗法已显示出惊人的成功,并且似乎是治疗包括FRC在内的多种恶性肿瘤的可行治疗选择。重要的是,该治疗方法的临床疗效显示受到已建立的免疫抑制肿瘤微环境的限制。但是,结合纳米工程方法可以大大帮助DC克服肿瘤诱导的免疫耐受。纳米囊封的肿瘤抗原的延长释放有助于提高基于DC的疗法选择性靶向和去除残留肿瘤细胞的能力。表面配体和辅助助剂的掺入可进一步帮助DC靶向(体内)克服与DC寿命短,免疫抑制和摄取不精确有关的问题。我们在此简要讨论FRC中基于DC的疗法的必要性和进展。审查还阐明了设计和开发临床上有效的纳米颗粒-DC组合的未来挑战,这些组合可以诱导有效的抗肿瘤免疫反应并延长患者的生存期。

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