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Article Abstract

Cervical adenocarcinoma (AC), a subtype of uterine cervical cancer (CC), poses a challenge due to its resistance to therapy and poor prognosis compared with squamous cervical carcinoma. [group B (GBS)], a Gram-positive coccus, has been associated with cervical intraepithelial neoplasia in CC. However, the underlying mechanism interaction between GBS and CC, particularly AC, remains elusive. Leveraging The Cancer Genome Atlas public data and time-series transcriptomic data, the present study investigated the interaction between GBS and AC, revealing activation of two pivotal pathways: 'MAPK signaling pathway' and 'mTORC1 signaling'. Western blotting, reverse transcription-quantitative PCR and cell viability assays were performed to validate the activation of these pathways and their role in promoting cancer cell proliferation. Subsequently, the present study evaluated the efficacy of two anticancer drugs targeting these pathways (binimetinib and ridaforolimus) in AC cell treatment. Binimetinib demonstrated a cytostatic effect, while ridaforolimus had a modest impact on HeLa cells after 48 h of treatment, as observed in both cell viability and cytotoxicity assays. The combination of binimetinib and ridaforolimus resulted in a significantly greater cytotoxic effect compared to binimetinib or ridaforolimus monotherapy, although the synergy score indicated an additive effect. In general, the MAPK and mTORC1 signaling pathways were identified as the main pathways associated with GBS and AC cells. The combination of binimetinib and ridaforolimus could be a potential AC treatment.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11474141PMC
http://dx.doi.org/10.3892/ol.2024.14720DOI Listing

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Article Synopsis
  • Cervical adenocarcinoma (AC) is a challenging subtype of cervical cancer that is more resistant to treatment and has a worse prognosis than squamous cervical carcinoma, and its connection to bacteria like group B Streptococcus (GBS) is not fully understood.
  • This study used genomic and transcriptomic data to explore the interaction between GBS and AC, discovering that GBS activates important pathways in cancer development, specifically the MAPK and mTORC1 signaling pathways.
  • The researchers tested two anticancer drugs, binimetinib and ridaforolimus, finding that their combination had a more effective cytotoxic response against AC cells compared to using either drug alone, suggesting a potential strategy for treating this
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