A Different Approach to Cancer and Drug Resistance in Cancer: Parasites

A Different Approach to Cancer and Drug Resistance in Cancer: Parasites

Encephalitozoon intestinalis (E. intestinalis) is a parasite that causes opportunistic infections that can cause death in immune compromised patients. The aim of this study was to determine the effect of parasite on genes involved in host cell apoptosis. The CaCo cells were infected with E. intestin...

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Bibliographic Details
Published in:Proceedings Vol. 40; no. 1; p. 30
Main Authors: Armağan Caner, Ülfet Çetinkaya, Meryem Şentürk, Arzuv Charyyeva, Meryem Eren
Format: Journal Article
Language:English
Published: MDPI AG 01-12-2019
Subjects:
anticancer drug resistance
cancer
encephalitozoon intestinalis
parasite
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Summary:Encephalitozoon intestinalis (E. intestinalis) is a parasite that causes opportunistic infections that can cause death in immune compromised patients. The aim of this study was to determine the effect of parasite on genes involved in host cell apoptosis. The CaCo cells were infected with E. intestinalis 50506 (ATCC) strain. Apoptosis was induced in both control and parasite-infected groups after infection. RNA isolation and cDNA extraction were then performed. Changes in the expression of genes involved in apoptotic pathways were evaluated quantitatively (qPCR) by Real-Time PCR. The obtained data were analyzed by 2-ΔΔCt method. E. intestinalis inhibits the CASP6, DR4, DR5, DCR2 genes that regulate the transcription of the genes known as the death gene of cells in CaCo cells. TP53 regulates the transcription of certain genes involved in cell death. DR4, DR5 and DCR2 are inhibited by the introduction of E. intestinalis into the cell. Caspase 6 is one of the caspases that induces apoptosis. As can be seen from the activation of these genes, E. intestinalis inhibits transcription genes in the pro-apoptotic pathway of the cell. We think that this parasite, which is commonly found in cancer patients, should be investigated for the effect of drug resistance in cancer treatment. This study was supported by Erciyes University. Project ID: TCD-2016-7042.
ISSN:2504-3900
DOI:10.3390/proceedings2019040030