Abstract
Simple SummaryThis pilot study on the trajectory of the gut microbiota (GM) in patients with epithelial ovarian cancer undergoing neoadjuvant and adjuvant chemotherapy highlighted peculiar dynamics associated with the therapeutic outcome. In particular, platinum-resistant patients showed a marked temporal reduction in GM diversity and increased instability with loss of health-associated taxa and increased proportions of lactate-producing microorganisms compared to those sensitive to platinum. These potential GM signatures of therapeutic failure are detectable within the first half of chemotherapy cycles, suggesting that early integrated treatments also aimed at modulating GM could influence therapeutic outcome. Further studies in larger cohorts combining multiple omics and possibly animal models are urgently needed for in-depth mechanistic understanding.Epithelial ovarian cancer (EOC) is one of the most lethal and silent gynecological tumors. Despite appropriate surgery and chemotherapy, relapse occurs in over half of patients with a poor prognosis. Recently, the gut microbiota (GM) was hypothesized to influence the efficacy of anticancer therapies, but no data are available in EOC. Here, by 16S rRNA gene sequencing and inferred metagenomics, we profiled the GM of EOC patients at diagnosis and reconstructed its trajectory along the course of neoadjuvant or adjuvant chemotherapy up to follow-up. Compared to healthy subjects, the GM of EOC patients appeared unbalanced and severely affected by chemotherapy. Strikingly, discriminating patterns were identified in relation to the therapeutic response. Platinum-resistant patients showed a marked temporal reduction in GM diversity and increased instability with loss of health-associated taxa and increased proportions of Coriobacteriaceae and Bifidobacterium. Notably, most of these microorganisms are lactate producers, suggesting increased lactate production as supported by inferred metagenomics. In contrast, the GM of platinum-sensitive patients appeared overall more diverse and stable and enriched in lactate utilizers from the Veillonellaceae family. In conclusion, we identified potential GM signatures of therapeutic outcome in EOC patients, which could open up new opportunities for cancer prognosis and treatment.
Highlights
Epithelial ovarian cancer (EOC) is a relatively rare disease whose incidence rate is very high in western countries, such as Europe and North America, with eight cases out of 100,000 [1,2]
All patients received a median of six cycles of carboplatin and taxane, carcinomatosis was present in all patients except one case of stage IC, and peritoneal cancer index (PCI) showed a median of 20
No differences were found in age, body mass index (BMI), Federation of Gynecology and Obstetrics (FIGO) stage, or BRCA mutation between the neoadjuvant and the adjuvant groups, neoadjuvant-treated patients were characterized by higher PCI (Wilcoxon test, p = 0.0044), number of cycles received (9 vs. 6) (p = 0.0477), and levels of CA 125 (1040 vs. 845) (p = 0.0486)
Summary
Epithelial ovarian cancer (EOC) is a relatively rare disease whose incidence rate is very high in western countries, such as Europe and North America, with eight cases out of 100,000 [1,2]. There is no established screening test for this disease, and this cancer represents the most lethal and silent gynecological tumor with diagnosis in advanced stages (III–IV) in about 65% of cases and a 5-year relative survival of only. The standard therapeutic approach is surgical cytoreduction followed by first-line standard chemotherapy with platinum and taxane compounds. When surgery is not possible for disease extent, neoadjuvant chemotherapy is an option to reduce the burden of the disease and achieve cytoreduction in responders; in non-responders, the prognosis is poor. Despite optimal surgery and appropriate first-line chemotherapy, about
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