Abstract
Development of drug resistance represents the major cause of cancer therapy failure, determines disease progression and results in poor prognosis for cancer patients. Different mechanisms are responsible for drug resistance. Intrinsic genetic modifications of cancer cells induce the alteration of expression of gene controlling specific pathways that regulate drug resistance: drug transport and metabolism; alteration of drug targets; DNA damage repair; and deregulation of apoptosis, autophagy, and pro-survival signaling. On the other hand, a complex signaling network among the entire cell component characterizes tumor microenvironment and regulates the pathways involved in the development of drug resistance. Gut microbiota represents a new player in the regulation of a patient’s response to cancer therapies, including chemotherapy and immunotherapy. In particular, commensal bacteria can regulate the efficacy of immune checkpoint inhibitor therapy by modulating the activation of immune responses to cancer. Commensal bacteria can also regulate the efficacy of chemotherapeutic drugs, such as oxaliplatin, gemcitabine, and cyclophosphamide. Recently, it has been shown that such bacteria can produce extracellular vesicles (EVs) that can mediate intercellular communication with human host cells. Indeed, bacterial EVs carry RNA molecules with gene expression regulatory ability that can be delivered to recipient cells of the host and potentially regulate the expression of genes involved in controlling the resistance to cancer therapy. On the other hand, host cells can also deliver human EVs to commensal bacteria and similarly, regulate gene expression. EV-mediated intercellular communication between commensal bacteria and host cells may thus represent a novel research area into potential mechanisms regulating the efficacy of cancer therapy.
Highlights
The development of resistance to cancer therapies represents a major challenge in the treatment of cancer patients and the main cause of poor prognosis
Some arise from intrinsic modification of cancer cells causing the alteration of genes that control specific pathways involved in treatment resistance such as drug transport and metabolism, alteration of drug targets, DNA damage repair, deregulation of apoptosis, autophagy, and prosurvival signaling[117]
After the advent of immune checkpoint inhibitor (ICI) therapy and promising evidence of its curative potential when used in combination with chemotherapy[119], it has been shown that specific species of the gut microbiota can regulate the efficacy of ICI responses
Summary
The development of resistance to cancer therapies represents a major challenge in the treatment of cancer patients and the main cause of poor prognosis. Soluble signaling factors released from specific bacterial species of the gut, which include structural components of bacteria, such as MAMPs, can induce different immune responses with opposing effects on the efficacy of cancer therapy. The acquisition of chemoresistance mediated by F. nucleatum was dependent on the activation of TLR4/ MYD88 signaling These studies provide insight into the role of soluble signaling factors released by gut microbiota on the modulation of drug resistance through the regulation of miRNA expression in host cells. In particular , hsa-miR-515-5p promotes the growth of F. nucleatus while hsa-miR-1226-5p promotes the growth of E. coli[113] These studies provide supporting evidence that a potential two-way EV-mediated communication may exist between bacteria and human host cells, resulting in reciprocal regulation of gene expression and biological cell function. In CRC patients, this equilibrium can be potentially compromised by the altered expression of miR-515-5p, that might affect F. nucleatus proliferation and consequent response to chemotherapeutic drugs, and prognosis[114]
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