Enhancing KLF15 activity in cardiomyocytes: a novel approach to prevent pathological reprogramming and fibrosis via nuclease-deficient dCas9VPR

Eric Schoger; Rosa Kim; Federico Bleckwedel; Tomas Peralta; Laura Priesmeier; Janek Fischer; Laura Stengel; Cheila Rocha; Gabriela L. Santos; Susanne Lutz; Etienne Boileau; Nina Baumgarten; Marcel H. Schulz; Christoph Dieterich; Oliver J. Müller; Lukas Cyganek; Alfredo Cabrera-Orefice; Hanna Eberl; Christoph Maack; Katrin Streckfuss-Bömeke; Mario Pavez-Giani; Shirin Doroudgar; Samuel T. Sossalla; Laura C. Zelarayán

doi:10.1038/s41392-026-02593-9

Enhancing KLF15 activity in cardiomyocytes: a novel approach to prevent pathological reprogramming and fibrosis via nuclease-deficient dCas9VPR

Eric Schoger
, Rosa Kim
, Federico Bleckwedel
, Tomas Peralta
, Laura Priesmeier
, Janek Fischer
, Laura Stengel
, Cheila Rocha
, Gabriela L. Santos
, Susanne Lutz
, Etienne Boileau
, Nina Baumgarten
, Marcel H. Schulz
, Christoph Dieterich
, Oliver J. Müller
, Lukas Cyganek
, Alfredo Cabrera-Orefice
, Hanna Eberl
, Christoph Maack
, Katrin Streckfuss-Bömeke

Mario Pavez-Giani, Shirin Doroudgar, Samuel T. Sossalla, Laura C. Zelarayán

Research output: Contribution to journal › Article › peer-review

Abstract

Transcriptional activity perturbation holds promise for selectively modulating harmful transcriptional networks, but its therapeutic potential remains largely unexplored. We employed a network-based analysis of single-cell heart transcriptomes to identify transcription factor activities linked to pathological cardiomyocytes in vivo. This analysis revealed that transcriptional activity of Krüppel-like factor 15 (KLF15) exhibited the most significant change in pathological cardiomyocytes, characterized by less effective repression of disease-associated genes in stressed hearts, which correlated with reduced KLF15 expression. To restore KLF15 activity, we utilized CRISPR/nuclease-dead (d)Cas9-based transcriptional enhancement (CRISPRa) in cardiomyocytes, which effectively abolished fetal reprogramming by simultaneously suppressing pathological gene expression and restoring metabolic homeostasis under sustained stress conditions. Furthermore, we identified a novel cell-nonautonomous anti-fibrotic effect mediated by cardiomyocyte-fibroblast crosstalk, and revealed the contribution of KLF15-dependent Alpha-2-glycoprotein 1, zinc-binding (AZGP1) regulation in this process. We also elucidated the upstream mechanisms of KLF15 regulation, highlighting its role as a cell-specific downstream target of the broad TGF-β canonical signaling pathway, along with its downstream-dependent mechanisms in human cardiomyocytes. Finally, to enhance the therapeutic potential of this approach, we engineered and validated an adeno-associated viral (AAV) vector with a small CRISPRa system for endogenous regulation in human cardiomyocytes suitable for clinical applications. Overall, we elucidated a regulatory circuit involving TGF-β, KLF15, and AZGP1, which coordinates critical pathological responses through cellular crosstalk between cardiomyocytes and fibroblasts. Importantly, we demonstrated the efficacy of CRISPRa as an epigenetic intervention restoring a critical transcriptional function disrupted in non-genetic heart failure. This approach provides a promising blueprint for future adaptation targeting additional non-hereditary pathologies.

Original language	English (US)
Article number	76
Journal	Signal Transduction and Targeted Therapy
Volume	11
Issue number	1
DOIs	https://doi.org/10.1038/s41392-026-02593-9
State	Published - Dec 2026

ASJC Scopus subject areas

Genetics
Cancer Research

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10.1038/s41392-026-02593-9

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Schoger, E., Kim, R., Bleckwedel, F., Peralta, T., Priesmeier, L., Fischer, J., Stengel, L., Rocha, C., Santos, G. L., Lutz, S., Boileau, E., Baumgarten, N., Schulz, M. H., Dieterich, C., Müller, O. J., Cyganek, L., Cabrera-Orefice, A., Eberl, H., Maack, C., ... Zelarayán, L. C. (2026). Enhancing KLF15 activity in cardiomyocytes: a novel approach to prevent pathological reprogramming and fibrosis via nuclease-deficient dCas9VPR. Signal Transduction and Targeted Therapy, 11(1), Article 76. https://doi.org/10.1038/s41392-026-02593-9

Schoger, E, Kim, R, Bleckwedel, F, Peralta, T, Priesmeier, L, Fischer, J, Stengel, L, Rocha, C, Santos, GL, Lutz, S, Boileau, E, Baumgarten, N, Schulz, MH, Dieterich, C, Müller, OJ, Cyganek, L, Cabrera-Orefice, A, Eberl, H, Maack, C, Streckfuss-Bömeke, K, Pavez-Giani, M, Doroudgar, S, Sossalla, ST & Zelarayán, LC 2026, 'Enhancing KLF15 activity in cardiomyocytes: a novel approach to prevent pathological reprogramming and fibrosis via nuclease-deficient dCas9VPR', Signal Transduction and Targeted Therapy, vol. 11, no. 1, 76. https://doi.org/10.1038/s41392-026-02593-9

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title = "Enhancing KLF15 activity in cardiomyocytes: a novel approach to prevent pathological reprogramming and fibrosis via nuclease-deficient dCas9VPR",

abstract = "Transcriptional activity perturbation holds promise for selectively modulating harmful transcriptional networks, but its therapeutic potential remains largely unexplored. We employed a network-based analysis of single-cell heart transcriptomes to identify transcription factor activities linked to pathological cardiomyocytes in vivo. This analysis revealed that transcriptional activity of Kr{\"u}ppel-like factor 15 (KLF15) exhibited the most significant change in pathological cardiomyocytes, characterized by less effective repression of disease-associated genes in stressed hearts, which correlated with reduced KLF15 expression. To restore KLF15 activity, we utilized CRISPR/nuclease-dead (d)Cas9-based transcriptional enhancement (CRISPRa) in cardiomyocytes, which effectively abolished fetal reprogramming by simultaneously suppressing pathological gene expression and restoring metabolic homeostasis under sustained stress conditions. Furthermore, we identified a novel cell-nonautonomous anti-fibrotic effect mediated by cardiomyocyte-fibroblast crosstalk, and revealed the contribution of KLF15-dependent Alpha-2-glycoprotein 1, zinc-binding (AZGP1) regulation in this process. We also elucidated the upstream mechanisms of KLF15 regulation, highlighting its role as a cell-specific downstream target of the broad TGF-β canonical signaling pathway, along with its downstream-dependent mechanisms in human cardiomyocytes. Finally, to enhance the therapeutic potential of this approach, we engineered and validated an adeno-associated viral (AAV) vector with a small CRISPRa system for endogenous regulation in human cardiomyocytes suitable for clinical applications. Overall, we elucidated a regulatory circuit involving TGF-β, KLF15, and AZGP1, which coordinates critical pathological responses through cellular crosstalk between cardiomyocytes and fibroblasts. Importantly, we demonstrated the efficacy of CRISPRa as an epigenetic intervention restoring a critical transcriptional function disrupted in non-genetic heart failure. This approach provides a promising blueprint for future adaptation targeting additional non-hereditary pathologies.",

author = "Eric Schoger and Rosa Kim and Federico Bleckwedel and Tomas Peralta and Laura Priesmeier and Janek Fischer and Laura Stengel and Cheila Rocha and Santos, \{Gabriela L.\} and Susanne Lutz and Etienne Boileau and Nina Baumgarten and Schulz, \{Marcel H.\} and Christoph Dieterich and M{\"u}ller, \{Oliver J.\} and Lukas Cyganek and Alfredo Cabrera-Orefice and Hanna Eberl and Christoph Maack and Katrin Streckfuss-B{\"o}meke and Mario Pavez-Giani and Shirin Doroudgar and Sossalla, \{Samuel T.\} and Zelaray{\'a}n, \{Laura C.\}",

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doi = "10.1038/s41392-026-02593-9",

language = "English (US)",

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T1 - Enhancing KLF15 activity in cardiomyocytes

T2 - a novel approach to prevent pathological reprogramming and fibrosis via nuclease-deficient dCas9VPR

AU - Schoger, Eric

AU - Kim, Rosa

AU - Bleckwedel, Federico

AU - Peralta, Tomas

AU - Priesmeier, Laura

AU - Fischer, Janek

AU - Stengel, Laura

AU - Rocha, Cheila

AU - Santos, Gabriela L.

AU - Lutz, Susanne

AU - Boileau, Etienne

AU - Baumgarten, Nina

AU - Schulz, Marcel H.

AU - Dieterich, Christoph

AU - Müller, Oliver J.

AU - Cyganek, Lukas

AU - Cabrera-Orefice, Alfredo

AU - Eberl, Hanna

AU - Maack, Christoph

AU - Streckfuss-Bömeke, Katrin

AU - Pavez-Giani, Mario

AU - Doroudgar, Shirin

AU - Sossalla, Samuel T.

AU - Zelarayán, Laura C.

PY - 2026/12

Y1 - 2026/12

N2 - Transcriptional activity perturbation holds promise for selectively modulating harmful transcriptional networks, but its therapeutic potential remains largely unexplored. We employed a network-based analysis of single-cell heart transcriptomes to identify transcription factor activities linked to pathological cardiomyocytes in vivo. This analysis revealed that transcriptional activity of Krüppel-like factor 15 (KLF15) exhibited the most significant change in pathological cardiomyocytes, characterized by less effective repression of disease-associated genes in stressed hearts, which correlated with reduced KLF15 expression. To restore KLF15 activity, we utilized CRISPR/nuclease-dead (d)Cas9-based transcriptional enhancement (CRISPRa) in cardiomyocytes, which effectively abolished fetal reprogramming by simultaneously suppressing pathological gene expression and restoring metabolic homeostasis under sustained stress conditions. Furthermore, we identified a novel cell-nonautonomous anti-fibrotic effect mediated by cardiomyocyte-fibroblast crosstalk, and revealed the contribution of KLF15-dependent Alpha-2-glycoprotein 1, zinc-binding (AZGP1) regulation in this process. We also elucidated the upstream mechanisms of KLF15 regulation, highlighting its role as a cell-specific downstream target of the broad TGF-β canonical signaling pathway, along with its downstream-dependent mechanisms in human cardiomyocytes. Finally, to enhance the therapeutic potential of this approach, we engineered and validated an adeno-associated viral (AAV) vector with a small CRISPRa system for endogenous regulation in human cardiomyocytes suitable for clinical applications. Overall, we elucidated a regulatory circuit involving TGF-β, KLF15, and AZGP1, which coordinates critical pathological responses through cellular crosstalk between cardiomyocytes and fibroblasts. Importantly, we demonstrated the efficacy of CRISPRa as an epigenetic intervention restoring a critical transcriptional function disrupted in non-genetic heart failure. This approach provides a promising blueprint for future adaptation targeting additional non-hereditary pathologies.

AB - Transcriptional activity perturbation holds promise for selectively modulating harmful transcriptional networks, but its therapeutic potential remains largely unexplored. We employed a network-based analysis of single-cell heart transcriptomes to identify transcription factor activities linked to pathological cardiomyocytes in vivo. This analysis revealed that transcriptional activity of Krüppel-like factor 15 (KLF15) exhibited the most significant change in pathological cardiomyocytes, characterized by less effective repression of disease-associated genes in stressed hearts, which correlated with reduced KLF15 expression. To restore KLF15 activity, we utilized CRISPR/nuclease-dead (d)Cas9-based transcriptional enhancement (CRISPRa) in cardiomyocytes, which effectively abolished fetal reprogramming by simultaneously suppressing pathological gene expression and restoring metabolic homeostasis under sustained stress conditions. Furthermore, we identified a novel cell-nonautonomous anti-fibrotic effect mediated by cardiomyocyte-fibroblast crosstalk, and revealed the contribution of KLF15-dependent Alpha-2-glycoprotein 1, zinc-binding (AZGP1) regulation in this process. We also elucidated the upstream mechanisms of KLF15 regulation, highlighting its role as a cell-specific downstream target of the broad TGF-β canonical signaling pathway, along with its downstream-dependent mechanisms in human cardiomyocytes. Finally, to enhance the therapeutic potential of this approach, we engineered and validated an adeno-associated viral (AAV) vector with a small CRISPRa system for endogenous regulation in human cardiomyocytes suitable for clinical applications. Overall, we elucidated a regulatory circuit involving TGF-β, KLF15, and AZGP1, which coordinates critical pathological responses through cellular crosstalk between cardiomyocytes and fibroblasts. Importantly, we demonstrated the efficacy of CRISPRa as an epigenetic intervention restoring a critical transcriptional function disrupted in non-genetic heart failure. This approach provides a promising blueprint for future adaptation targeting additional non-hereditary pathologies.

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Enhancing KLF15 activity in cardiomyocytes: a novel approach to prevent pathological reprogramming and fibrosis via nuclease-deficient dCas9VPR

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