Vitamin D, cell death pathways, and tuberculosis

Vitamin D, cell death pathways, and tuberculosis

Background: Mycobacterium tuberculosis induces cellular necrosis that could promote spread of infection. The aim of this study is to analyze the effects of Vitamin D3 supplementation to improve the effectiveness of 2nd-line anti-tuberculosis (TB) drug therapy, especially in relation with cell death...

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Main Authors: Manik Retno Wahyunitisari, Ni Made Mertaniasih, Muhammad Amin, Wayan T. Artama, Eko Budi Koendhori
Format: Article PeerReviewed
Language:English
English
English
Published: Wolters Kluwer-Medknow Publications 2017
Subjects:
R Medicine (General)
RZ Other systems of medicine
Online Access:http://repository.unair.ac.id/93442/1/Vitamin%20D%2C%20Cell%20Death%20Pathways%20and%20Tuberculosis.pdf
http://repository.unair.ac.id/93442/2/Vitamin%20D%2C%20Cell%20Death%20Pathways.pdf
http://repository.unair.ac.id/93442/3/Vitamin%20D%2C%20Cell%20Death%20Pathways%20and%20Tuberculosis_compressed.pdf
http://repository.unair.ac.id/93442/
http://www.ijmyco.org/article.asp?issn=2212-5531;year=2017;volume=6;issue=4;spage=349;epage=355;aulast=Wahyunitisari
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spelling id-langga.934422020-01-13T07:21:13Z http://repository.unair.ac.id/93442/ Vitamin D, cell death pathways, and tuberculosis Manik Retno Wahyunitisari Ni Made Mertaniasih Muhammad Amin Wayan T. Artama Eko Budi Koendhori R Medicine (General) RZ Other systems of medicine Background: Mycobacterium tuberculosis induces cellular necrosis that could promote spread of infection. The aim of this study is to analyze the effects of Vitamin D3 supplementation to improve the effectiveness of 2nd-line anti-tuberculosis (TB) drug therapy, especially in relation with cell death pathways. Methods: Mus musculus C3HeB/FeJ was randomly divided into four groups containing eight animals each. The 1st group (G1), consisting of mice that were intratracheally infected with multidrug-resistant strain of M. tuberculosis and sacrificed on 2-week postinfection to confirm successful infection. (G2) was a group of TB mice without therapy. Then, (G3) was a group of mice with the 2nd-line anti-TB therapy. The last group (G4) was a group of mice receiving not only the 2nd-line anti-TB therapy but also daily oral Vitamin D3 supplementation. Immunohistochemistry was used to measure expression of nuclear Vitamin D receptor, apoptosis marker cleaved caspase-3, cathelin-related antimicrobial peptide (CRAMP) and LC3B autophagy markers, necrosis marker RIPK3, and collagenase matrix metalloproteinase-1 (MMP1). The number of bacteria in the lung was calculated by colony forming units. The partial least square structural equation modeling with SmartPLS 3.2.6 software was used to analyze structural models among the variables. Results: Supplementation of Vitamin D3 on the 2nd-line anti-TB therapy increases Vitamin D3 receptor, CRAMP, LC3B, caspase-3 (P = 0.026, P = 0.000, P= 0.001), presses MMP1, and the number of bacteria (P = 0.010 and P= 0.000, respectively). The structural equation modeling analysis shows that increasing autophagy pathways reduces necrosis by lowering MMP1, whereas apoptosis reduces necrosis by decreasing the number of bacteria (each with indirect effects − 0.543 and − 0.544). Conclusion: A comprehensive analysis with the partial least square structural equation modeling shows decreasing necrosis requires increasing autophagy and apoptosis. Wolters Kluwer-Medknow Publications 2017-03 Article PeerReviewed text en http://repository.unair.ac.id/93442/1/Vitamin%20D%2C%20Cell%20Death%20Pathways%20and%20Tuberculosis.pdf text en http://repository.unair.ac.id/93442/2/Vitamin%20D%2C%20Cell%20Death%20Pathways.pdf text en http://repository.unair.ac.id/93442/3/Vitamin%20D%2C%20Cell%20Death%20Pathways%20and%20Tuberculosis_compressed.pdf Manik Retno Wahyunitisari and Ni Made Mertaniasih and Muhammad Amin and Wayan T. Artama and Eko Budi Koendhori (2017) Vitamin D, cell death pathways, and tuberculosis. International Journal of Mycobacteriology, 6 (1). pp. 349-355. ISSN 2212-5531 http://www.ijmyco.org/article.asp?issn=2212-5531;year=2017;volume=6;issue=4;spage=349;epage=355;aulast=Wahyunitisari 10.4103/ijmy.ijmy_120_17
institution Universitas Airlangga
building Universitas Airlangga Library
country Indonesia
collection UNAIR Repository
language English
English
English
topic R Medicine (General)
RZ Other systems of medicine
spellingShingle R Medicine (General)
RZ Other systems of medicine
Manik Retno Wahyunitisari
Ni Made Mertaniasih
Muhammad Amin
Wayan T. Artama
Eko Budi Koendhori
Vitamin D, cell death pathways, and tuberculosis
description Background: Mycobacterium tuberculosis induces cellular necrosis that could promote spread of infection. The aim of this study is to analyze the effects of Vitamin D3 supplementation to improve the effectiveness of 2nd-line anti-tuberculosis (TB) drug therapy, especially in relation with cell death pathways. Methods: Mus musculus C3HeB/FeJ was randomly divided into four groups containing eight animals each. The 1st group (G1), consisting of mice that were intratracheally infected with multidrug-resistant strain of M. tuberculosis and sacrificed on 2-week postinfection to confirm successful infection. (G2) was a group of TB mice without therapy. Then, (G3) was a group of mice with the 2nd-line anti-TB therapy. The last group (G4) was a group of mice receiving not only the 2nd-line anti-TB therapy but also daily oral Vitamin D3 supplementation. Immunohistochemistry was used to measure expression of nuclear Vitamin D receptor, apoptosis marker cleaved caspase-3, cathelin-related antimicrobial peptide (CRAMP) and LC3B autophagy markers, necrosis marker RIPK3, and collagenase matrix metalloproteinase-1 (MMP1). The number of bacteria in the lung was calculated by colony forming units. The partial least square structural equation modeling with SmartPLS 3.2.6 software was used to analyze structural models among the variables. Results: Supplementation of Vitamin D3 on the 2nd-line anti-TB therapy increases Vitamin D3 receptor, CRAMP, LC3B, caspase-3 (P = 0.026, P = 0.000, P= 0.001), presses MMP1, and the number of bacteria (P = 0.010 and P= 0.000, respectively). The structural equation modeling analysis shows that increasing autophagy pathways reduces necrosis by lowering MMP1, whereas apoptosis reduces necrosis by decreasing the number of bacteria (each with indirect effects − 0.543 and − 0.544). Conclusion: A comprehensive analysis with the partial least square structural equation modeling shows decreasing necrosis requires increasing autophagy and apoptosis.
format Article
PeerReviewed
author Manik Retno Wahyunitisari
Ni Made Mertaniasih
Muhammad Amin
Wayan T. Artama
Eko Budi Koendhori
author_facet Manik Retno Wahyunitisari
Ni Made Mertaniasih
Muhammad Amin
Wayan T. Artama
Eko Budi Koendhori
author_sort Manik Retno Wahyunitisari
title Vitamin D, cell death pathways, and tuberculosis
title_short Vitamin D, cell death pathways, and tuberculosis
title_full Vitamin D, cell death pathways, and tuberculosis
title_fullStr Vitamin D, cell death pathways, and tuberculosis
title_full_unstemmed Vitamin D, cell death pathways, and tuberculosis
title_sort vitamin d, cell death pathways, and tuberculosis
publisher Wolters Kluwer-Medknow Publications
publishDate 2017
url http://repository.unair.ac.id/93442/1/Vitamin%20D%2C%20Cell%20Death%20Pathways%20and%20Tuberculosis.pdf
http://repository.unair.ac.id/93442/2/Vitamin%20D%2C%20Cell%20Death%20Pathways.pdf
http://repository.unair.ac.id/93442/3/Vitamin%20D%2C%20Cell%20Death%20Pathways%20and%20Tuberculosis_compressed.pdf
http://repository.unair.ac.id/93442/
http://www.ijmyco.org/article.asp?issn=2212-5531;year=2017;volume=6;issue=4;spage=349;epage=355;aulast=Wahyunitisari
_version_ 1681153293832683520

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