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The antifibrotic effect of isolate tagitinin C from tithonia diversifolia (Hemsley) A. Gray on keloid fibroblast cell

INTRODUCTION: Keloids characterized by fibroblast hyperproliferation and depositions of collagen which similar to cancer cells. Tagitinin C is a class of sesquiterpene lactones (SLS) was isolated from the leaves of the moon flower Tithonia diversifolia (Hemsley) A. Gray. The study aim is to evaluate...

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Autores principales: Ranti, Imaniar, Wahyuningsih, Mae Sri Hartati, Wirohadidjojo, Yohannes Widodo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The African Field Epidemiology Network 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6317294/
https://www.ncbi.nlm.nih.gov/pubmed/30637049
http://dx.doi.org/10.11604/pamj.2018.30.264.9994
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author Ranti, Imaniar
Wahyuningsih, Mae Sri Hartati
Wirohadidjojo, Yohannes Widodo
author_facet Ranti, Imaniar
Wahyuningsih, Mae Sri Hartati
Wirohadidjojo, Yohannes Widodo
author_sort Ranti, Imaniar
collection PubMed
description INTRODUCTION: Keloids characterized by fibroblast hyperproliferation and depositions of collagen which similar to cancer cells. Tagitinin C is a class of sesquiterpene lactones (SLS) was isolated from the leaves of the moon flower Tithonia diversifolia (Hemsley) A. Gray. The study aim is to evaluate the effects of tagitinin C from Tithonia diversifolia to keloid fibroblasts (KF). METHODS: Monolayer cultures of keloid fibroblast (three passages) were treated with 8 serial concentration of tagitinin C (0.015 to 2) μg/mL during 72 and 120 hours. A positive control using mitomycin C. Cellular viabilities were measured by MTT assay. Collagen depositions were measured by Sirius Red assay for nonsoluble collagen. RESULTS: The reading of the result was conducted by ELISA reader. Data were analyzed by probit regression with SPSS 19 for Windows. The result showed that tagitinin C can inhibit keloid fibroblasts (KF) viability with IC(50) 0.122 μg/mL (incubation 72h) and 0.039 μg/mL (120h), whereas mitomycin C IC(50) 0.120 μg/mL (72h) and IC(50) of 0.100 μg/mL (120h). At IC(50) concentration of tagitinin C on keloid collagen deposition 53.1% (72h) and 44.3% (120h), whereas the IC(50) concentration of mitomycin C on keloid collagen deposition 60.4% (72h) and 52.1% (120h). Selectivity index tagitinin C on normal fibroblasts (NF) is 287 for 72h incubation and 791 for 120h incubation. CONCLUSION: It can be concluded that the ability of tagitinin C inhibits KF viability and decreasing keloid collagen deposition is consistent with the concentration (concentration-dependent) and incubation time (time-dependent). Tagitinin C has a low toxicity level on NF with high selectivity index.
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spelling pubmed-63172942019-01-11 The antifibrotic effect of isolate tagitinin C from tithonia diversifolia (Hemsley) A. Gray on keloid fibroblast cell Ranti, Imaniar Wahyuningsih, Mae Sri Hartati Wirohadidjojo, Yohannes Widodo Pan Afr Med J Research INTRODUCTION: Keloids characterized by fibroblast hyperproliferation and depositions of collagen which similar to cancer cells. Tagitinin C is a class of sesquiterpene lactones (SLS) was isolated from the leaves of the moon flower Tithonia diversifolia (Hemsley) A. Gray. The study aim is to evaluate the effects of tagitinin C from Tithonia diversifolia to keloid fibroblasts (KF). METHODS: Monolayer cultures of keloid fibroblast (three passages) were treated with 8 serial concentration of tagitinin C (0.015 to 2) μg/mL during 72 and 120 hours. A positive control using mitomycin C. Cellular viabilities were measured by MTT assay. Collagen depositions were measured by Sirius Red assay for nonsoluble collagen. RESULTS: The reading of the result was conducted by ELISA reader. Data were analyzed by probit regression with SPSS 19 for Windows. The result showed that tagitinin C can inhibit keloid fibroblasts (KF) viability with IC(50) 0.122 μg/mL (incubation 72h) and 0.039 μg/mL (120h), whereas mitomycin C IC(50) 0.120 μg/mL (72h) and IC(50) of 0.100 μg/mL (120h). At IC(50) concentration of tagitinin C on keloid collagen deposition 53.1% (72h) and 44.3% (120h), whereas the IC(50) concentration of mitomycin C on keloid collagen deposition 60.4% (72h) and 52.1% (120h). Selectivity index tagitinin C on normal fibroblasts (NF) is 287 for 72h incubation and 791 for 120h incubation. CONCLUSION: It can be concluded that the ability of tagitinin C inhibits KF viability and decreasing keloid collagen deposition is consistent with the concentration (concentration-dependent) and incubation time (time-dependent). Tagitinin C has a low toxicity level on NF with high selectivity index. The African Field Epidemiology Network 2018-08-08 /pmc/articles/PMC6317294/ /pubmed/30637049 http://dx.doi.org/10.11604/pamj.2018.30.264.9994 Text en © Imaniar Ranti et al. http://creativecommons.org/licenses/by/2.0/ The Pan African Medical Journal - ISSN 1937-8688. This is an Open Access article distributed under the terms of the Creative Commons Attribution License which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Ranti, Imaniar
Wahyuningsih, Mae Sri Hartati
Wirohadidjojo, Yohannes Widodo
The antifibrotic effect of isolate tagitinin C from tithonia diversifolia (Hemsley) A. Gray on keloid fibroblast cell
title The antifibrotic effect of isolate tagitinin C from tithonia diversifolia (Hemsley) A. Gray on keloid fibroblast cell
title_full The antifibrotic effect of isolate tagitinin C from tithonia diversifolia (Hemsley) A. Gray on keloid fibroblast cell
title_fullStr The antifibrotic effect of isolate tagitinin C from tithonia diversifolia (Hemsley) A. Gray on keloid fibroblast cell
title_full_unstemmed The antifibrotic effect of isolate tagitinin C from tithonia diversifolia (Hemsley) A. Gray on keloid fibroblast cell
title_short The antifibrotic effect of isolate tagitinin C from tithonia diversifolia (Hemsley) A. Gray on keloid fibroblast cell
title_sort antifibrotic effect of isolate tagitinin c from tithonia diversifolia (hemsley) a. gray on keloid fibroblast cell
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6317294/
https://www.ncbi.nlm.nih.gov/pubmed/30637049
http://dx.doi.org/10.11604/pamj.2018.30.264.9994
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