CCL2 and IL18 expressions may associate with the anti-proliferative effect of noncontact electro capacitive cancer therapy in vivo

Hindana Fatmasari,Rarastoeti Pratiwi,Sunarti Sunarti,Lalu Gunawan Fadliansyah,Eti Nurwening Sholikhah,Ahmad Ghitha Fadhlurrahman,Richard Luke Daniels,Sofia Mubarika Haryana,Yoram Palti,Woro Anindito Sri Tunjung,Sitarina Widyarini,Agung Putra,Syamsul Arif Ardiansyah,Luthfi Nurhidayat,Firman Alamsyah,Rarastoeti Pratiwi,Nyoman Yudi Antara,Warsito Purwo Taruno

doi:10.5256/f1000research.22795.r55336

Hindana Fatmasari, Rarastoeti Pratiwi + Show 16 more

https://doi.org/10.5256/f1000research.22795.r55336

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Journal: F1000Research	Publication Date: Jul 14, 2020
Citations: 3	License type: CC BY 4.0

Affiliation: College of Idaho, Sultan Agung Islamic University

Abstract

Background: Noncontact Electro Capacitive Cancer Therapy (ECCT) is a novel treatment modality in cancer. Chemokine (C-C motif) ligand 2 (CCL2) has a major role in the outgrowth of metastatic breast cancer. Interleukin 18 (IL18) plays a role in macrophage alteration, which leads to excessive angiogenesis. This study aims to elaborate on the association of CCL2, IL18, IL23α, and TNF-α (tumor necrosis factor-alpha) expression with the anti-proliferative effect of ECCT in rat breast tumor tissue. Methods: Low intensity (18 Vpp) and intermediate frequency (150 kHz) alternating current-electric field (AC-EF) between two capacitive electrodes were exposed as external EF to a rat cage. Twenty-four rats were divided into four groups of six replicates. Breast tumor tissues were collected from 7, 12-dimethylbenz[a]anthracene (DMBA)-induced rats. Two groups were non DMBA-induced rats without ECCT exposure (NINT) and with (NIT). The other two groups were DMBA-induced rats without ECCT exposure (INT) and with (IT). Mammary glands and breast tumor tissues were collected from each group and preserved. Hematoxylin-eosin and immunohistochemistry staining were performed on paraffin sections of tissues using anti-PCNA, anti-ErbB2, anti-Caspase3, and anti-CD68. CCL2, IL18, IL23α, and TNF-α mRNA relative expressions were analyzed using qRT-PCR. Results: ECCT exposure may cause the reduction of PCNA protein expression as well as ErbB2 on breast tumor tissues, but it causes the increase of Caspase3 and macrophage CD68 protein. In rat breast tumor tissues of IT groups, the mRNA expression of CCL2 and IL18 are significantly down-regulated, in contrast with the up-regulated expression of these cytokines in tumor tissues of the INT group. IL23α and TNF- α expression remained similar in both groups. Conclusion: CCL2 and IL18 expressions have an association with the inhibition of breast tumor cell proliferation affected by ECCT exposure

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