Pharmaceuticals (Aug 2024)

Is There an Interplay between Environmental Factors, Microbiota Imbalance, and Cancer Chemotherapy-Associated Intestinal Mucositis?

  • Camila Fernandes,
  • Mahara Coelho Crisostomo Miranda,
  • Cássia Rodrigues Roque,
  • Ana Lizeth Padilla Paguada,
  • Carlos Adrian Rodrigues Mota,
  • Katharine Gurgel Dias Florêncio,
  • Anamaria Falcão Pereira,
  • Deysi Viviana Tenazoa Wong,
  • Reinaldo Barreto Oriá,
  • Roberto César Pereira Lima-Júnior

DOI
https://doi.org/10.3390/ph17081020
Journal volume & issue
Vol. 17, no. 8
p. 1020

Abstract

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Interindividual variation in drug efficacy and toxicity is a significant problem, potentially leading to adverse clinical and economic public health outcomes. While pharmacogenetics and pharmacogenomics have long been considered the primary causes of such heterogeneous responses, pharmacomicrobiomics has recently gained attention. The microbiome, a community of microorganisms living in or on the human body, is a critical determinant of drug response and toxicity. Factors such as diet, lifestyle, exposure to xenobiotics, antibiotics use, illness, and genetics can influence the composition of the microbiota. Changes in the intestinal microbiota are particularly influential in drug responsiveness, especially in cancer chemotherapy. The microbiota can modulate an individual’s response to a drug, affecting its bioavailability, clinical effect, and toxicity, affecting treatment outcomes and patient quality of life. For instance, the microbiota can convert drugs into active or toxic metabolites, influencing their efficacy and side effects. Alternatively, chemotherapy can also alter the microbiota, creating a bidirectional interplay. Probiotics have shown promise in modulating the microbiome and ameliorating chemotherapy side effects, highlighting the potential for microbiota-targeted interventions in improving cancer treatment outcomes. This opinion paper addresses how environmental factors and chemotherapy-induced dysbiosis impact cancer chemotherapy gastrointestinal toxicity.

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