Influence of gut and lung dysbiosis on lung cancer progression and their modulation as promising therapeutic targets: a comprehensive review

IF 10.7 Q1 MEDICINE, RESEARCH & EXPERIMENTAL MedComm Pub Date : 2024-11-24 DOI:10.1002/mco2.70018
Rajan Thapa, Anjana Thapa Magar, Jesus Shrestha, Nisha Panth, Sobia Idrees, Tayyaba Sadaf, Saroj Bashyal, Bassma H. Elwakil, Vrashabh V. Sugandhi, Satish Rojekar, Ram Nikhate, Gaurav Gupta, Sachin Kumar Singh, Kamal Dua, Philip M Hansbro, Keshav Raj Paudel
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Abstract

Lung cancer (LC) continues to pose the highest mortality and exhibits a common prevalence among all types of cancer. The genetic interaction between human eukaryotes and microbial cells plays a vital role in orchestrating every physiological activity of the host. The dynamic crosstalk between gut and lung microbiomes and the gut–lung axis communication network has been widely accepted as promising factors influencing LC progression. The advent of the 16s rDNA sequencing technique has opened new horizons for elucidating the lung microbiome and its potential pathophysiological role in LC and other infectious lung diseases using a molecular approach. Numerous studies have reported the direct involvement of the host microbiome in lung tumorigenesis processes and their impact on current treatment strategies such as radiotherapy, chemotherapy, or immunotherapy. The genetic and metabolomic cross-interaction, microbiome-dependent host immune modulation, and the close association between microbiota composition and treatment outcomes strongly suggest that designing microbiome-based treatment strategies and investigating new molecules targeting the common holobiome could offer potential alternatives to develop effective therapeutic principles for LC treatment. This review aims to highlight the interaction between the host and microbiome in LC progression and the possibility of manipulating altered microbiome ecology as therapeutic targets.

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肠道和肺部菌群失调对肺癌进展的影响及其作为有前景的治疗靶点的调节:综述
肺癌(LC)仍然是死亡率最高的癌症,也是所有癌症类型中常见的一种。人类真核细胞与微生物细胞之间的基因相互作用在协调宿主的各种生理活动中发挥着至关重要的作用。肠道和肺部微生物群之间的动态串联以及肠道-肺轴通讯网络已被广泛认为是影响肺癌进展的有利因素。16s rDNA 测序技术的出现为利用分子方法阐明肺部微生物组及其在 LC 和其他传染性肺部疾病中的潜在病理生理作用开辟了新天地。大量研究报告表明,宿主微生物组直接参与了肺部肿瘤发生过程,并对放疗、化疗或免疫疗法等当前治疗策略产生了影响。遗传和代谢组学的交叉相互作用、微生物依赖的宿主免疫调节以及微生物群组成与治疗效果之间的密切联系都强烈表明,设计基于微生物群的治疗策略和研究针对普通全生物群的新分子可为制定有效的肺癌治疗原则提供潜在的替代方案。本综述旨在强调在 LC 进展过程中宿主与微生物组之间的相互作用,以及将改变微生物组生态作为治疗靶点的可能性。
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CiteScore
6.70
自引率
0.00%
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审稿时长
10 weeks
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