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Tumor Cell Communications as Promising Supramolecular Targets for Cancer Chemotherapy: A Possible Strategy. | LitMetric

AI Article Synopsis

  • Despite significant investment and effort over the past 52 years in the "War on Cancer," traditional treatment methods like chemotherapy and radiation have fallen short of expectations.
  • A new approach proposes targeting cancer-stromal synapses, the connections between cancer cells and their surrounding microenvironment, which could lead to more effective treatment.
  • This method aims to disrupt these synapses using targeted chemical agents, potentially enhancing treatment safety, precision, and reducing the likelihood of drug resistance.

Article Abstract

Fifty-two years have passed since President Nixon launched the "War on Cancer". Despite unparalleled efforts and funds allocated worldwide, the outlined goals were not achieved because cancer treatment approaches such as chemotherapy, radiation therapy, hormonal and targeted therapies have not fully met the expectations. Based on the recent literature, a new direction in cancer therapy can be proposed which targets connections between cancer cells and their microenvironment by chemical means. Cancer-stromal synapses such as immunological synapses between cancer and immune cells provide an attractive target for this approach. Such synapses form ligand-receptor clusters on the interface of the interacting cells. They share a common property of involving intercellular clusters of spatially proximate and cooperatively acting proteins. Synapses provide the space for the focused intercellular signaling molecules exchange. Thus, the disassembly of cancer-stromal synapses may potentially cause the collapse of various tumors. Additionally, the clustered arrangement of synapse components offers opportunities to enhance treatment safety and precision by using targeted crosslinking chemical agents which may inactivate cancer synapses even in reduced concentrations. Furthermore, attaching a cleavable cell-permeable toxic agent(s) to a crosslinker may further enhance the anti-cancer effect of such therapeutics. The highlighted approach promises to be universal, relatively simple and cost-efficient. We also hope that, unlike chemotherapeutic and immune drugs that interact with a single target, by using supramolecular large clusters that include many different components as a target, the emergence of a resistance characteristic of chemo- and immunotherapy is extremely unlikely.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11476449PMC
http://dx.doi.org/10.3390/ijms251910454DOI Listing

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