Loss of Resistance to Angiotensin II–Induced Hypertension in the Jackson Laboratory Recombination-Activating Gene Null Mouse on the C57BL/6J Background

Ji, Hong; Pai, Amrita V.; West, Crystal A.; Wu, Xie; Speth, Robert C.; Sandberg, Kathryn

doi:10.1161/hypertensionaha.117.09063

Cited by 45 publications

(30 citation statements)

References 29 publications

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“…Inhibition of ANG II-induced hypertension in Rag1Ϫ/Ϫ mice have been confirmed by several distinct institutions (432,829,1074,1095). One laboratory, however, could not confirm their finding (432) when the mice were repurchased recently (431), suggesting that spontaneous mutations might be occurring in the inbred strain. Distinct expression levels of glomerular ANG II receptors were suggested to explain the difference according to binding studies.…”

Section: Limitations and Pitfalls In Ang II Signaling Researchmentioning

confidence: 99%

Angiotensin II Signal Transduction: An Update on Mechanisms of Physiology and Pathophysiology

Forrester

Booz

Sigmund

et al. 2018

Physiological Reviews

778

780

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The renin-angiotensin-aldosterone system plays crucial roles in cardiovascular physiology and pathophysiology. However, many of the signaling mechanisms have been unclear. The angiotensin II (ANG II) type 1 receptor (ATR) is believed to mediate most functions of ANG II in the system. ATR utilizes various signal transduction cascades causing hypertension, cardiovascular remodeling, and end organ damage. Moreover, functional cross-talk between ATR signaling pathways and other signaling pathways have been recognized. Accumulating evidence reveals the complexity of ANG II signal transduction in pathophysiology of the vasculature, heart, kidney, and brain, as well as several pathophysiological features, including inflammation, metabolic dysfunction, and aging. In this review, we provide a comprehensive update of the ANG II receptor signaling events and their functional significances for potential translation into therapeutic strategies. ATR remains central to the system in mediating physiological and pathophysiological functions of ANG II, and participation of specific signaling pathways becomes much clearer. There are still certain limitations and many controversies, and several noteworthy new concepts require further support. However, it is expected that rigorous translational research of the ANG II signaling pathways including those in large animals and humans will contribute to establishing effective new therapies against various diseases.

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Section: Limitations and Pitfalls In Ang II Signaling Researchmentioning

confidence: 99%

Angiotensin II Signal Transduction: An Update on Mechanisms of Physiology and Pathophysiology

Forrester

Booz

Sigmund

et al. 2018

Physiological Reviews

778

780

View full text Add to dashboard Cite

show abstract

“…81 Just recently, the importance of T cells in hypertension, as recruited to the PVAT, in both Ang-II and DOCA-salt hypertension in mice, was called into question with the inability of multiple labs across the country to reproduce the previously observed protection of the Rag1 mice (lack T and B cells) from Ang-II-induced hypertension. 82 In dysfunctional PVAT (e.g., hypertension), immune cell infiltration becomes more prominent. Infiltrating cells include macrophages, memory T cells, IL-10-producing FoxP3 + T regulatory cells, natural killer cells, and granulocytes.…”

Section: Immune Cell Infiltration and Pvatmentioning

confidence: 99%

Hypertension Induced Morphological and Physiological Changes in Cells of the Arterial Wall

Martinez‐Quinones

McCarthy

Watts

et al. 2018

American Journal of Hypertension

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Morphological and physiological changes in the vasculature have been described in the evolution and maintenance of hypertension. Hypertension-induced vascular dysfunction may present itself as a contributing, or consequential factor, to vascular remodeling caused by chronically elevated systemic arterial blood pressure. Changes in all vessel layers, from the endothelium to the perivascular adipose tissue (PVAT), have been described. This mini-review focuses on the current knowledge of the structure and function of the vessel layers, specifically muscular arteries: intima, media, adventitia, PVAT, and the cell types harbored within each vessel layer. The contributions of each cell type to vessel homeostasis and pathophysiological development of hypertension will be highlighted.

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“…These provocative findings(2,(5)(6)(7), which challenge those that initially demonstrated blunted hypertension responses in Rag1-deficient mice(3), raise a number of important questions. Firstly, why does the same Rag1 immunodeficient mouse model yield diametrically opposed results?Secondly is the Rag1 KO animal the most appropriate pre-clinical model to study immune responses in hypertension?…”

mentioning

confidence: 93%

“…Ji et al also failed to show that Rag1 KO mice are protected from Ang II-induced hypertension (6) and Uchida et al demonstrated that total lymphocyte deficiency in Rag1-/-mice had no effect on systolic blood pressure prior to and during Ang II infusion (2). Moreover, in a model of arterial injury, immune deficiency in Rag1 KO mice was associated with augmented, rather than reduced, neointima formation, effects that were attenuated by CD8 T cells, but not by CD4 T cells (7).…”

mentioning

confidence: 99%

Lessons Learned From RAG-1-Deficient Mice in Hypertension

Montezano

Touyz

2020

Hypertension

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Loss of Resistance to Angiotensin II–Induced Hypertension in the Jackson Laboratory Recombination-Activating Gene Null Mouse on the C57BL/6J Background

Cited by 45 publications

References 29 publications

Angiotensin II Signal Transduction: An Update on Mechanisms of Physiology and Pathophysiology

Angiotensin II Signal Transduction: An Update on Mechanisms of Physiology and Pathophysiology

Hypertension Induced Morphological and Physiological Changes in Cells of the Arterial Wall

Lessons Learned From RAG-1-Deficient Mice in Hypertension

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