Myocardial transcriptomic and proteomic landscapes across the menopausal continuum in a murine model of chemically induced accelerated ovarian failure

Marissa A. Lopez-Pier; Vito A. Marino; Andrea C. Vazquez-Loreto; Rinku S. Skaria; Danielle K. Cannon; Christina H. Hoyer-Kimura; Alice E. Solomon; Yulia Lipovka; Kevin Doubleday; Maricela Pier; Meinsung Chu; Rachel Mayfield; Samantha M. Behunin; Tianjing Hu; Paul R. Langlais; Timothy A. McKinsey; John P. Konhilas

doi:10.1152/physiolgenomics.00133.2024

Myocardial transcriptomic and proteomic landscapes across the menopausal continuum in a murine model of chemically induced accelerated ovarian failure

Marissa A. Lopez-Pier
, Vito A. Marino
, Andrea C. Vazquez-Loreto
, Rinku S. Skaria
, Danielle K. Cannon
, Christina H. Hoyer-Kimura
, Alice E. Solomon
, Yulia Lipovka
, Kevin Doubleday
, Maricela Pier
, Meinsung Chu
, Rachel Mayfield
, Samantha M. Behunin
, Tianjing Hu
, Paul R. Langlais
, Timothy A. McKinsey
, John P. Konhilas

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

Abstract

Risk of cardiovascular disease (CVD) in women increases with the menopausal transition. Using a chemical model (4-vinylcyclohexene diepoxide; VCD) of accelerated ovarian failure, we previously demonstrated that menopausal females are more susceptible to CVD compared with peri-or premenopausal females like humans. Yet, the cellular and molecular mechanisms underlying this shift in CVD susceptibility across the pre-to peri-to menopause continuum remain understudied. In this work using the VCD mouse model, we phenotyped cellular and molecular signatures from hearts at each hormonally distinct stage that included transcriptomic, proteomic, and cell biological analyses. The transcriptional profile of premenopausal hearts clustered separately from perimenopausal and menopausal hearts, which clustered more similarly. Proteomics also revealed hormonal clustering; perimenopausal hearts grouped more closely with premenopausal than menopausal hearts. Both proteomes and transcriptomes showed similar trends in genes associated with atherothrombosis, contractility, and impaired nuclear signaling between pre-, peri-, and menopausal murine hearts. Further analysis of posttranslational modifications (PTMs) showed hormone-dependent shifts in the phosphoproteome and acetylome. To further interro-gate these findings, we triggered pathological remodeling using angiotensin II (Ang II). Phosphorylation of AMP-activated protein kinase (AMPK) signaling and histone deacetylase (HDAC) activity were found to be dependent on hormonal status and Ang II stimulation. Finally, knockdown of anti-inflammatory regulatory T cells (Treg) exacerbated Ang II-dependent fibrosis implicating HDAC-mediated epi-genetic suppression of Treg activity. Taken together, we demonstrated unique cellular and molecular profiles underlying the cardiac phenotype of pre-, peri-, and menopausal mice supporting the necessity to study CVD in females across the hormonal transition. NEW & NOTEWORTHY Cycling and perimenopausal females are protected from cardiovascular disease (CVD) whereas menopausal females are more susceptible to CVD and other pathological sequalae. The cellular and molecular mechanisms underlying loss of CVD protection across the pre-to peri-to menopause transition remain understudied. Using the murine 4-vinylcyclohexene diepoxide (VCD) model of menopause we highlight cellular and molecular signatures from hearts at each hormonally distinct stage that included transcriptomic, proteomic, and cell biological analyses.

Original language	English (US)
Pages (from-to)	409-430
Number of pages	22
Journal	Physiological Genomics
Volume	57
Issue number	7
DOIs	https://doi.org/10.1152/physiolgenomics.00133.2024
State	Published - Jul 2025

Keywords

4-vinylcyclohexenediepoxide
AMP-activated protein kinase
heart disease
menopause
proteomics

ASJC Scopus subject areas

Physiology
Genetics

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10.1152/physiolgenomics.00133.2024

Cite this

Lopez-Pier, M. A., Marino, V. A., Vazquez-Loreto, A. C., Skaria, R. S., Cannon, D. K., Hoyer-Kimura, C. H., Solomon, A. E., Lipovka, Y., Doubleday, K., Pier, M., Chu, M., Mayfield, R., Behunin, S. M., Hu, T., Langlais, P. R., McKinsey, T. A., & Konhilas, J. P. (2025). Myocardial transcriptomic and proteomic landscapes across the menopausal continuum in a murine model of chemically induced accelerated ovarian failure. Physiological Genomics, 57(7), 409-430. https://doi.org/10.1152/physiolgenomics.00133.2024

Lopez-Pier, MA, Marino, VA, Vazquez-Loreto, AC, Skaria, RS, Cannon, DK, Hoyer-Kimura, CH, Solomon, AE, Lipovka, Y, Doubleday, K, Pier, M, Chu, M, Mayfield, R, Behunin, SM, Hu, T, Langlais, PR, McKinsey, TA & Konhilas, JP 2025, 'Myocardial transcriptomic and proteomic landscapes across the menopausal continuum in a murine model of chemically induced accelerated ovarian failure', Physiological Genomics, vol. 57, no. 7, pp. 409-430. https://doi.org/10.1152/physiolgenomics.00133.2024

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title = "Myocardial transcriptomic and proteomic landscapes across the menopausal continuum in a murine model of chemically induced accelerated ovarian failure",

abstract = "Risk of cardiovascular disease (CVD) in women increases with the menopausal transition. Using a chemical model (4-vinylcyclohexene diepoxide; VCD) of accelerated ovarian failure, we previously demonstrated that menopausal females are more susceptible to CVD compared with peri-or premenopausal females like humans. Yet, the cellular and molecular mechanisms underlying this shift in CVD susceptibility across the pre-to peri-to menopause continuum remain understudied. In this work using the VCD mouse model, we phenotyped cellular and molecular signatures from hearts at each hormonally distinct stage that included transcriptomic, proteomic, and cell biological analyses. The transcriptional profile of premenopausal hearts clustered separately from perimenopausal and menopausal hearts, which clustered more similarly. Proteomics also revealed hormonal clustering; perimenopausal hearts grouped more closely with premenopausal than menopausal hearts. Both proteomes and transcriptomes showed similar trends in genes associated with atherothrombosis, contractility, and impaired nuclear signaling between pre-, peri-, and menopausal murine hearts. Further analysis of posttranslational modifications (PTMs) showed hormone-dependent shifts in the phosphoproteome and acetylome. To further interro-gate these findings, we triggered pathological remodeling using angiotensin II (Ang II). Phosphorylation of AMP-activated protein kinase (AMPK) signaling and histone deacetylase (HDAC) activity were found to be dependent on hormonal status and Ang II stimulation. Finally, knockdown of anti-inflammatory regulatory T cells (Treg) exacerbated Ang II-dependent fibrosis implicating HDAC-mediated epi-genetic suppression of Treg activity. Taken together, we demonstrated unique cellular and molecular profiles underlying the cardiac phenotype of pre-, peri-, and menopausal mice supporting the necessity to study CVD in females across the hormonal transition. NEW \& NOTEWORTHY Cycling and perimenopausal females are protected from cardiovascular disease (CVD) whereas menopausal females are more susceptible to CVD and other pathological sequalae. The cellular and molecular mechanisms underlying loss of CVD protection across the pre-to peri-to menopause transition remain understudied. Using the murine 4-vinylcyclohexene diepoxide (VCD) model of menopause we highlight cellular and molecular signatures from hearts at each hormonally distinct stage that included transcriptomic, proteomic, and cell biological analyses.",

keywords = "4-vinylcyclohexenediepoxide, AMP-activated protein kinase, heart disease, menopause, proteomics",

author = "Lopez-Pier, \{Marissa A.\} and Marino, \{Vito A.\} and Vazquez-Loreto, \{Andrea C.\} and Skaria, \{Rinku S.\} and Cannon, \{Danielle K.\} and Hoyer-Kimura, \{Christina H.\} and Solomon, \{Alice E.\} and Yulia Lipovka and Kevin Doubleday and Maricela Pier and Meinsung Chu and Rachel Mayfield and Behunin, \{Samantha M.\} and Tianjing Hu and Langlais, \{Paul R.\} and McKinsey, \{Timothy A.\} and Konhilas, \{John P.\}",

note = "Publisher Copyright: {\textcopyright} 2025 The Authors.",

year = "2025",

month = jul,

doi = "10.1152/physiolgenomics.00133.2024",

language = "English (US)",

volume = "57",

pages = "409--430",

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T1 - Myocardial transcriptomic and proteomic landscapes across the menopausal continuum in a murine model of chemically induced accelerated ovarian failure

AU - Lopez-Pier, Marissa A.

AU - Marino, Vito A.

AU - Vazquez-Loreto, Andrea C.

AU - Skaria, Rinku S.

AU - Cannon, Danielle K.

AU - Hoyer-Kimura, Christina H.

AU - Solomon, Alice E.

AU - Lipovka, Yulia

AU - Doubleday, Kevin

AU - Pier, Maricela

AU - Chu, Meinsung

AU - Mayfield, Rachel

AU - Behunin, Samantha M.

AU - Hu, Tianjing

AU - Langlais, Paul R.

AU - McKinsey, Timothy A.

AU - Konhilas, John P.

PY - 2025/7

Y1 - 2025/7

N2 - Risk of cardiovascular disease (CVD) in women increases with the menopausal transition. Using a chemical model (4-vinylcyclohexene diepoxide; VCD) of accelerated ovarian failure, we previously demonstrated that menopausal females are more susceptible to CVD compared with peri-or premenopausal females like humans. Yet, the cellular and molecular mechanisms underlying this shift in CVD susceptibility across the pre-to peri-to menopause continuum remain understudied. In this work using the VCD mouse model, we phenotyped cellular and molecular signatures from hearts at each hormonally distinct stage that included transcriptomic, proteomic, and cell biological analyses. The transcriptional profile of premenopausal hearts clustered separately from perimenopausal and menopausal hearts, which clustered more similarly. Proteomics also revealed hormonal clustering; perimenopausal hearts grouped more closely with premenopausal than menopausal hearts. Both proteomes and transcriptomes showed similar trends in genes associated with atherothrombosis, contractility, and impaired nuclear signaling between pre-, peri-, and menopausal murine hearts. Further analysis of posttranslational modifications (PTMs) showed hormone-dependent shifts in the phosphoproteome and acetylome. To further interro-gate these findings, we triggered pathological remodeling using angiotensin II (Ang II). Phosphorylation of AMP-activated protein kinase (AMPK) signaling and histone deacetylase (HDAC) activity were found to be dependent on hormonal status and Ang II stimulation. Finally, knockdown of anti-inflammatory regulatory T cells (Treg) exacerbated Ang II-dependent fibrosis implicating HDAC-mediated epi-genetic suppression of Treg activity. Taken together, we demonstrated unique cellular and molecular profiles underlying the cardiac phenotype of pre-, peri-, and menopausal mice supporting the necessity to study CVD in females across the hormonal transition. NEW & NOTEWORTHY Cycling and perimenopausal females are protected from cardiovascular disease (CVD) whereas menopausal females are more susceptible to CVD and other pathological sequalae. The cellular and molecular mechanisms underlying loss of CVD protection across the pre-to peri-to menopause transition remain understudied. Using the murine 4-vinylcyclohexene diepoxide (VCD) model of menopause we highlight cellular and molecular signatures from hearts at each hormonally distinct stage that included transcriptomic, proteomic, and cell biological analyses.

AB - Risk of cardiovascular disease (CVD) in women increases with the menopausal transition. Using a chemical model (4-vinylcyclohexene diepoxide; VCD) of accelerated ovarian failure, we previously demonstrated that menopausal females are more susceptible to CVD compared with peri-or premenopausal females like humans. Yet, the cellular and molecular mechanisms underlying this shift in CVD susceptibility across the pre-to peri-to menopause continuum remain understudied. In this work using the VCD mouse model, we phenotyped cellular and molecular signatures from hearts at each hormonally distinct stage that included transcriptomic, proteomic, and cell biological analyses. The transcriptional profile of premenopausal hearts clustered separately from perimenopausal and menopausal hearts, which clustered more similarly. Proteomics also revealed hormonal clustering; perimenopausal hearts grouped more closely with premenopausal than menopausal hearts. Both proteomes and transcriptomes showed similar trends in genes associated with atherothrombosis, contractility, and impaired nuclear signaling between pre-, peri-, and menopausal murine hearts. Further analysis of posttranslational modifications (PTMs) showed hormone-dependent shifts in the phosphoproteome and acetylome. To further interro-gate these findings, we triggered pathological remodeling using angiotensin II (Ang II). Phosphorylation of AMP-activated protein kinase (AMPK) signaling and histone deacetylase (HDAC) activity were found to be dependent on hormonal status and Ang II stimulation. Finally, knockdown of anti-inflammatory regulatory T cells (Treg) exacerbated Ang II-dependent fibrosis implicating HDAC-mediated epi-genetic suppression of Treg activity. Taken together, we demonstrated unique cellular and molecular profiles underlying the cardiac phenotype of pre-, peri-, and menopausal mice supporting the necessity to study CVD in females across the hormonal transition. NEW & NOTEWORTHY Cycling and perimenopausal females are protected from cardiovascular disease (CVD) whereas menopausal females are more susceptible to CVD and other pathological sequalae. The cellular and molecular mechanisms underlying loss of CVD protection across the pre-to peri-to menopause transition remain understudied. Using the murine 4-vinylcyclohexene diepoxide (VCD) model of menopause we highlight cellular and molecular signatures from hearts at each hormonally distinct stage that included transcriptomic, proteomic, and cell biological analyses.

KW - 4-vinylcyclohexenediepoxide

KW - AMP-activated protein kinase

KW - heart disease

KW - menopause

KW - proteomics

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M3 - Article

C2 - 40266891

AN - SCOPUS:105007121308

SN - 1094-8341

VL - 57

SP - 409

EP - 430

JO - Physiological Genomics

JF - Physiological Genomics

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ER -

Myocardial transcriptomic and proteomic landscapes across the menopausal continuum in a murine model of chemically induced accelerated ovarian failure

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