Bivalent chromatin as a therapeutic target in cancer: An in silico predictive approach for combining epigenetic drugs.
Tumour cell heterogeneity is a major barrier for efficient design of targeted anti-cancer therapies. A diverse distribution of phenotypically distinct tumour-cell subpopulations prior to drug treatment predisposes to non-uniform responses, leading to the elimination of sensitive cancer cells whilst...
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doaj-c6170dc9763e4c5ab5c1b3c8c85023502021-07-13T04:30:37ZengPublic Library of Science (PLoS)PLoS Computational Biology1553-734X1553-73582021-06-01176e100840810.1371/journal.pcbi.1008408Bivalent chromatin as a therapeutic target in cancer: An in silico predictive approach for combining epigenetic drugs.Tomás AlarcónJosep SardanyésAntoni GuillamonJavier A MenendezTumour cell heterogeneity is a major barrier for efficient design of targeted anti-cancer therapies. A diverse distribution of phenotypically distinct tumour-cell subpopulations prior to drug treatment predisposes to non-uniform responses, leading to the elimination of sensitive cancer cells whilst leaving resistant subpopulations unharmed. Few strategies have been proposed for quantifying the variability associated to individual cancer-cell heterogeneity and minimizing its undesirable impact on clinical outcomes. Here, we report a computational approach that allows the rational design of combinatorial therapies involving epigenetic drugs against chromatin modifiers. We have formulated a stochastic model of a bivalent transcription factor that allows us to characterise three different qualitative behaviours, namely: bistable, high- and low-gene expression. Comparison between analytical results and experimental data determined that the so-called bistable and high-gene expression behaviours can be identified with undifferentiated and differentiated cell types, respectively. Since undifferentiated cells with an aberrant self-renewing potential might exhibit a cancer/metastasis-initiating phenotype, we analysed the efficiency of combining epigenetic drugs against the background of heterogeneity within the bistable sub-ensemble. Whereas single-targeted approaches mostly failed to circumvent the therapeutic problems represented by tumour heterogeneity, combinatorial strategies fared much better. Specifically, the more successful combinations were predicted to involve modulators of the histone H3K4 and H3K27 demethylases KDM5 and KDM6A/UTX. Those strategies involving the H3K4 and H3K27 methyltransferases MLL2 and EZH2, however, were predicted to be less effective. Our theoretical framework provides a coherent basis for the development of an in silico platform capable of identifying the epigenetic drugs combinations best-suited to therapeutically manage non-uniform responses of heterogenous cancer cell populations.https://doi.org/10.1371/journal.pcbi.1008408 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Tomás Alarcón Josep Sardanyés Antoni Guillamon Javier A Menendez |
spellingShingle |
Tomás Alarcón Josep Sardanyés Antoni Guillamon Javier A Menendez Bivalent chromatin as a therapeutic target in cancer: An in silico predictive approach for combining epigenetic drugs. PLoS Computational Biology |
author_facet |
Tomás Alarcón Josep Sardanyés Antoni Guillamon Javier A Menendez |
author_sort |
Tomás Alarcón |
title |
Bivalent chromatin as a therapeutic target in cancer: An in silico predictive approach for combining epigenetic drugs. |
title_short |
Bivalent chromatin as a therapeutic target in cancer: An in silico predictive approach for combining epigenetic drugs. |
title_full |
Bivalent chromatin as a therapeutic target in cancer: An in silico predictive approach for combining epigenetic drugs. |
title_fullStr |
Bivalent chromatin as a therapeutic target in cancer: An in silico predictive approach for combining epigenetic drugs. |
title_full_unstemmed |
Bivalent chromatin as a therapeutic target in cancer: An in silico predictive approach for combining epigenetic drugs. |
title_sort |
bivalent chromatin as a therapeutic target in cancer: an in silico predictive approach for combining epigenetic drugs. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS Computational Biology |
issn |
1553-734X 1553-7358 |
publishDate |
2021-06-01 |
description |
Tumour cell heterogeneity is a major barrier for efficient design of targeted anti-cancer therapies. A diverse distribution of phenotypically distinct tumour-cell subpopulations prior to drug treatment predisposes to non-uniform responses, leading to the elimination of sensitive cancer cells whilst leaving resistant subpopulations unharmed. Few strategies have been proposed for quantifying the variability associated to individual cancer-cell heterogeneity and minimizing its undesirable impact on clinical outcomes. Here, we report a computational approach that allows the rational design of combinatorial therapies involving epigenetic drugs against chromatin modifiers. We have formulated a stochastic model of a bivalent transcription factor that allows us to characterise three different qualitative behaviours, namely: bistable, high- and low-gene expression. Comparison between analytical results and experimental data determined that the so-called bistable and high-gene expression behaviours can be identified with undifferentiated and differentiated cell types, respectively. Since undifferentiated cells with an aberrant self-renewing potential might exhibit a cancer/metastasis-initiating phenotype, we analysed the efficiency of combining epigenetic drugs against the background of heterogeneity within the bistable sub-ensemble. Whereas single-targeted approaches mostly failed to circumvent the therapeutic problems represented by tumour heterogeneity, combinatorial strategies fared much better. Specifically, the more successful combinations were predicted to involve modulators of the histone H3K4 and H3K27 demethylases KDM5 and KDM6A/UTX. Those strategies involving the H3K4 and H3K27 methyltransferases MLL2 and EZH2, however, were predicted to be less effective. Our theoretical framework provides a coherent basis for the development of an in silico platform capable of identifying the epigenetic drugs combinations best-suited to therapeutically manage non-uniform responses of heterogenous cancer cell populations. |
url |
https://doi.org/10.1371/journal.pcbi.1008408 |
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