An in Vitro Study in Which New Boron Derivatives Maybe an Option for Breast Cancer Treatment

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Date

2019

Authors

Journal Title

Journal ISSN

Volume Title

Publisher

Kare Publishing

Open Access Color

GOLD

Green Open Access

No

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Publicly Funded

No
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Average
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Average
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Top 10%

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Abstract

Objectives: We aimed to investigate the distribution of immunoreactivities of vascular endothelial growth factor (VEGF), endothelial nitric oxide synthase (eNOS), and inducible NOS (iNOS) on breast cancer cells in response to treatment with boron derivatives. Methods: We initially analyzed the cytotoxic effect and IC50 value of boron by MTT assay. For the evaluation of the angiogenesis, expression level of antibodies was detected to following boron derivatives such as boric acid, boron penta (BP), and T-Boron (DPD) in the absence of boron treatment using the indirect immunohistochemical method. The evaluation of these staining was done using the H-scoring system. Results: It was found that immunoreactivities of VEGF, eNOS, and iNOS increased on control compared to those of the cells of MDA-MB231 human breast cancer cell line. Following boron derivatives treatment, it was observed that they were inhibited the VEGF/NOS labeling in MDA-MB-231 breast cancer cells. Conclusion: The present data suggest that BP, especially DPD, inhibits the angiogenesis of breast cancer cells through VEGF pathway. From this point, these boron derivatives may provide a novel therapeutic approach for breast cancer treatment. © 2019, by Eurasian Journal of Medicine and Oncology.

Description

Keywords

Boron penta, DPD, Immunohistochemistry, iNOS, MDA-MB-231

Fields of Science

03 medical and health sciences, 0302 clinical medicine

Citation

WoS Q

Q3

Scopus Q

Q3
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OpenCitations Citation Count
8

Source

Eurasian Journal of Medicine and Oncology

Volume

3

Issue

1

Start Page

22

End Page

27
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CrossRef : 7

Scopus : 6

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Mendeley Readers : 21

SCOPUS™ Citations

6

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4

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Downloads

7

checked on Feb 13, 2026

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