The Potential Influence of Residual or Recurrent Disease on Bevacizumab Treatment Efficacy in Ovarian Cancer: Current Evidence and Future Perspectives

Overview

Journal Cancers (Basel)

Publisher MDPI

Specialty Oncology

Date 2024 Mar 13

PMID 38473419

Authors

Klaudia Zak

Malgorzata Satora

Ilona Skrabalak

Rafal Tarkowski

Marta Ostrowska-Lesko

Marcin Bobinski

Affiliations

Soon will be listed here.

Abstract

There were high hopes for the new antiangiogenic medicament, bevacizumab, which could inhibit the creation of new blood vessels through binding to isoform A of vascular endothelial growth factor (VEGF). However, it is not only blood vessels that are responsible for tumor cell spread. During the process of tumor growth, lymphangiogenesis is mediated by other members of the VEGF family, specifically VEGF-C and VEGF-D, which act independent to bevacizumab. Therefore, based on the mechanism of bevacizumab action and the processes of angio- and lymphangiogenesis, we formed three hypotheses: (1) if the lymph nodes in primary ovarian cancers are metastatic, the outcome of bevacizumab treatment is worsened; (2) concerning the second-line treatment, bevacizumab will act in a weakened manner if recurrence occurs in lymph nodes as opposed to a local recurrence; (3) patients treated by bevacizumab are more likely to have recurrences in lymph nodes. These hypotheses raise the issue of the existing knowledge gap, which concerns the effect of bevacizumab on metastatic lymph nodes.

Citing Articles

Exploring Bevacizumab's Role in Gynecological Cancers: An Up-to-Date Narrative Review Focusing on Ovarian Cancer.

Liolis E, Mulita F, Koutras A, Makatsoris T, Sivolapenko G Mater Sociomed. 2025; 36(4):268-279.

PMID: 39963442 PMC: 11830232. DOI: 10.5455/msm.2024.36.268-279.

New hopes and promises in the treatment of ovarian cancer focusing on targeted treatment-a narrative review.

Satora M, Kulak K, Zaremba B, Grunwald A, Swiechowska-Starek P, Tarkowski R Front Pharmacol. 2024; 15:1416555.

PMID: 38948462 PMC: 11212463. DOI: 10.3389/fphar.2024.1416555.

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