Aims T cells contribute to hypertension; however, hypertension occurs in settings of T cell deficiency. Methods and results We studied two colonies of T/B cell-deficient RAG-1−/− mice with disparate responses to angiotensin II, being one protected from blood pressure increase and the other one responsive. This difference depends on the capability of hypertensive RAG-1−/− mice to expand natural killer and innate lymphoid cells (NK/ILCs) that produce pro-hypertensive cytokines. This process is regulated by the DNA methylation status of the β2 adrenergic receptor (β2-AdR). Angiotensin II caused blood pressure elevation in T and NK/ILCs-deficient mice only when either T or NK/ILCs cells were adoptively reconstituted. Additional studies showed NK cell expansion in humans that underwent B cell depletion, and this was augmented in those with hypertension. Conclusions These findings illustrate that the modulation of NK/ILCs activation by adrenergic signalling governs an escape mechanism in lymphocyte-deficient host, enabling the development of hypertension.
Beta 2 adrenergic receptor gene methylation activates innate lymphoid cells to drive hypertension in lymphocyte deficient hosts / Chen, Wei; Perrotta, Sara; Xiao, Liang; Carnevale, Lorenzo; Abd-ElDayem, Marwa A; Hennen, Elizabeth M; Rivera-Medina, Luis Miguel; Patrick, David M; Ao, Mingfang; Pallante, Fabio; Zonfrilli, Azzurra; Zhao, Shilin; Migliaccio, Agnese; Lan, Lan; Fardella, Stefania; Sciume, Giuseppe; Mastroiacovo, Francesco; Lembo, Giuseppe; Carnevale, Daniela; Harrison, David G. - In: CARDIOVASCULAR RESEARCH. - ISSN 0008-6363. - 121:5(2025), pp. 817-831. [10.1093/cvr/cvaf042]
Beta 2 adrenergic receptor gene methylation activates innate lymphoid cells to drive hypertension in lymphocyte deficient hosts
Carnevale, Lorenzo;Zonfrilli, Azzurra;Sciume, Giuseppe;Lembo, Giuseppe;Carnevale, Daniela
;
2025
Abstract
Aims T cells contribute to hypertension; however, hypertension occurs in settings of T cell deficiency. Methods and results We studied two colonies of T/B cell-deficient RAG-1−/− mice with disparate responses to angiotensin II, being one protected from blood pressure increase and the other one responsive. This difference depends on the capability of hypertensive RAG-1−/− mice to expand natural killer and innate lymphoid cells (NK/ILCs) that produce pro-hypertensive cytokines. This process is regulated by the DNA methylation status of the β2 adrenergic receptor (β2-AdR). Angiotensin II caused blood pressure elevation in T and NK/ILCs-deficient mice only when either T or NK/ILCs cells were adoptively reconstituted. Additional studies showed NK cell expansion in humans that underwent B cell depletion, and this was augmented in those with hypertension. Conclusions These findings illustrate that the modulation of NK/ILCs activation by adrenergic signalling governs an escape mechanism in lymphocyte-deficient host, enabling the development of hypertension.| File | Dimensione | Formato | |
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