Cargando…
Biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice
Duchenne muscular dystrophy is initiated by dystrophin deficiency, but downstream pathophysiological pathways such as membrane instability, NFĸB activation, mitochondrial dysfunction, and induction of TGFβ fibrosis pathways are thought to drive the disability. Dystrophin replacement strategies are h...
| Autores principales: | , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Public Library of Science
2021
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7899329/ https://www.ncbi.nlm.nih.gov/pubmed/33617542 http://dx.doi.org/10.1371/journal.pone.0246507 |
| _version_ | 1783654031282929664 |
|---|---|
| author | Ziemba, Michael Barkhouse, Molly Uaesoontrachoon, Kitipong Giri, Mamta Hathout, Yetrib Dang, Utkarsh J. Gordish-Dressman, Heather Nagaraju, Kanneboyina Hoffman, Eric P. |
| author_facet | Ziemba, Michael Barkhouse, Molly Uaesoontrachoon, Kitipong Giri, Mamta Hathout, Yetrib Dang, Utkarsh J. Gordish-Dressman, Heather Nagaraju, Kanneboyina Hoffman, Eric P. |
| author_sort | Ziemba, Michael |
| collection | PubMed |
| description | Duchenne muscular dystrophy is initiated by dystrophin deficiency, but downstream pathophysiological pathways such as membrane instability, NFĸB activation, mitochondrial dysfunction, and induction of TGFβ fibrosis pathways are thought to drive the disability. Dystrophin replacement strategies are hopeful for addressing upstream dystrophin deficiency; however, all methods to date use semi-functional dystrophin proteins that are likely to trigger downstream pathways. Thus, combination therapies that can target multiple downstream pathways are important in treating DMD, even for dystrophin-replacement strategies. We sought to define blood pharmacodynamic biomarkers of drug response in the mdx mouse model of Duchenne muscular dystrophy using a series of repurposed drugs. Four-week-old mdx mice were treated for four weeks with four different drugs singly and in combination: vehicle, prednisolone, vamorolone, rituximab, β-aminoisobutyric acid (BAIBA) (11 treatment groups; n = 6/group). Blood was collected via cardiac puncture at study termination, and proteomic profiling was carried out using SOMAscan aptamer panels (1,310 proteins assayed). Prednisolone was tested alone and in combination with other drugs. It was found to have a good concordance of prednisolone-responsive biomarkers (56 increased by prednisolone, 39 decreased) focused on NFκB and TGFβ cascades. Vamorolone shared 45 (80%) of increased biomarkers and 13 (33%) of decreased biomarkers with prednisolone. Comparison of published human corticosteroid-responsive biomarkers to our mdx data showed 14% (3/22) concordance between mouse and human. Rituximab showed fewer drug-associated biomarkers, with the most significant being human IgG. On the other hand, BAIBA treatment (high and low dose) showed a drug-associated increase in 40 serum proteins and decreased 5 serum proteins. Our results suggest that a biomarker approach could be employed for assessing drug combinations in both mouse and human studies. |
| format | Online Article Text |
| id | pubmed-7899329 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2021 |
| publisher | Public Library of Science |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-78993292021-03-02 Biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice Ziemba, Michael Barkhouse, Molly Uaesoontrachoon, Kitipong Giri, Mamta Hathout, Yetrib Dang, Utkarsh J. Gordish-Dressman, Heather Nagaraju, Kanneboyina Hoffman, Eric P. PLoS One Research Article Duchenne muscular dystrophy is initiated by dystrophin deficiency, but downstream pathophysiological pathways such as membrane instability, NFĸB activation, mitochondrial dysfunction, and induction of TGFβ fibrosis pathways are thought to drive the disability. Dystrophin replacement strategies are hopeful for addressing upstream dystrophin deficiency; however, all methods to date use semi-functional dystrophin proteins that are likely to trigger downstream pathways. Thus, combination therapies that can target multiple downstream pathways are important in treating DMD, even for dystrophin-replacement strategies. We sought to define blood pharmacodynamic biomarkers of drug response in the mdx mouse model of Duchenne muscular dystrophy using a series of repurposed drugs. Four-week-old mdx mice were treated for four weeks with four different drugs singly and in combination: vehicle, prednisolone, vamorolone, rituximab, β-aminoisobutyric acid (BAIBA) (11 treatment groups; n = 6/group). Blood was collected via cardiac puncture at study termination, and proteomic profiling was carried out using SOMAscan aptamer panels (1,310 proteins assayed). Prednisolone was tested alone and in combination with other drugs. It was found to have a good concordance of prednisolone-responsive biomarkers (56 increased by prednisolone, 39 decreased) focused on NFκB and TGFβ cascades. Vamorolone shared 45 (80%) of increased biomarkers and 13 (33%) of decreased biomarkers with prednisolone. Comparison of published human corticosteroid-responsive biomarkers to our mdx data showed 14% (3/22) concordance between mouse and human. Rituximab showed fewer drug-associated biomarkers, with the most significant being human IgG. On the other hand, BAIBA treatment (high and low dose) showed a drug-associated increase in 40 serum proteins and decreased 5 serum proteins. Our results suggest that a biomarker approach could be employed for assessing drug combinations in both mouse and human studies. Public Library of Science 2021-02-22 /pmc/articles/PMC7899329/ /pubmed/33617542 http://dx.doi.org/10.1371/journal.pone.0246507 Text en © 2021 Ziemba et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. |
| spellingShingle | Research Article Ziemba, Michael Barkhouse, Molly Uaesoontrachoon, Kitipong Giri, Mamta Hathout, Yetrib Dang, Utkarsh J. Gordish-Dressman, Heather Nagaraju, Kanneboyina Hoffman, Eric P. Biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice |
| title | Biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice |
| title_full | Biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice |
| title_fullStr | Biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice |
| title_full_unstemmed | Biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice |
| title_short | Biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice |
| title_sort | biomarker-focused multi-drug combination therapy and repurposing trial in mdx mice |
| topic | Research Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7899329/ https://www.ncbi.nlm.nih.gov/pubmed/33617542 http://dx.doi.org/10.1371/journal.pone.0246507 |
| work_keys_str_mv | AT ziembamichael biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice AT barkhousemolly biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice AT uaesoontrachoonkitipong biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice AT girimamta biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice AT hathoutyetrib biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice AT dangutkarshj biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice AT gordishdressmanheather biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice AT nagarajukanneboyina biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice AT hoffmanericp biomarkerfocusedmultidrugcombinationtherapyandrepurposingtrialinmdxmice |