Impact and potential value of immunosenescence on solid gastrointestinal tumors

Jul 15, 2024Frontiers in immunology

How aging of the immune system may affect solid digestive system tumors

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Abstract

may lead to decreased immune recognition and efficacy of antitumor therapies in solid tumors.

  • Immunosenescence involves increased diversity of immune genes due to aging, resulting in reduced immune system function.
  • DNA damage is a fundamental change associated with immunosenescence, contributing to remodeling.
  • Worsening inflammation and increased production of immunosuppressive factors are observed in the immunosenescent tumor microenvironment.
  • The accumulation of tumor-associated fibroblasts and myeloid-derived suppressor cells may further hinder antitumor immune responses.
  • Senotherapy strategies could enhance treatment effectiveness by removing senescent cells and blocking processes related to senescence.

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Full Text

What this is

  • refers to the aging-related decline in immune function, impacting tumor progression and treatment efficacy.
  • This review examines how alters the () in solid gastrointestinal tumors, particularly colorectal cancer.
  • It discusses the interplay between immune aging processes and the , emphasizing the need for targeted therapies to counteract these effects.

Essence

  • negatively affects immune responses in solid gastrointestinal tumors, leading to poor treatment outcomes. Targeting may enhance antitumor therapies.

Key takeaways

  • contributes to a pro- by altering immune cell function and promoting inflammation. This change can lead to increased tumor progression and decreased efficacy of immunotherapies.
  • Senotherapy strategies, which aim to eliminate senescent cells or mitigate their effects, have potential as adjunct therapies to enhance the effectiveness of existing cancer treatments.

Caveats

  • The interaction between and tumor progression is complex and not fully understood, necessitating further research to clarify these relationships.
  • Current therapeutic strategies targeting require more extensive validation in clinical settings to assess their long-term efficacy and safety.

Definitions

  • immunosenescence: Aging-related decline in immune system function, characterized by reduced recognition and response to pathogens and tumors.
  • tumor microenvironment (TME): The environment surrounding a tumor, including immune cells, fibroblasts, and signaling molecules, which influences tumor growth and response to therapy.
  • senescence-associated secretory phenotype (SASP): A collection of factors secreted by senescent cells that can promote inflammation and alter immune responses.

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