The chloride intracellular channel 5A stimulates podocyte Rac1, protecting against hypertension-induced glomerular injury

Tavasoli, Mahtab; Li, Laiji; Al-Momany, Abass; Zhu, Lijun; Adam, Benjamin; Wang, Zhixiang; Ballermann, Barbara J.

doi:10.1016/j.kint.2016.01.001

Cited by 21 publications

(19 citation statements)

References 53 publications

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“…Podocytes cultured in vitro are sensitive to shear stress, which induces reorganization of cytoskeleton (Friedrich et al 2006), and this helps them to cover an expanding GBM which further leads to foot process effacement. In desoxycorticosterone-trimethylacetate (DOCA) hypertensive mice, chloride intracellular channel 5A, which is highly enriched in podocytes foot process, protects against hypertension-induced podocyte injury through weakening the tensile strength of the actin cytoskeleton in Rac1-dependent manner (Tavasoli et al 2016). This has been considered to be the protective response for podocyte to escape detachment.…”

Section: Role Of Hypertension In the Damage Of Podocytesmentioning

confidence: 99%

Role of Podocyte Injury in Glomerulosclerosis

Lü

Wang

Lü

et al. 2019

Advances in Experimental Medicine and Biology

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Finding new therapeutic targets of glomerulosclerosis treatment is an ongoing quest. Due to a living environment of various stresses and pathological stimuli, podocytes are prone to injuries; moreover, as a cell without proliferative potential, loss of podocytes is vital in the pathogenesis of glomerulosclerosis. Thus, sufficient understanding of factors and underlying mechanisms of podocyte injury facilitates the advancement of treating and prevention of glomerulosclerosis. The clinical symptom of podocyte injury is proteinuria, sometimes with loss of kidney functions progressing to glomerulosclerosis. Injury-induced changes in podocyte physiology and function are actually not a simple passive process, but a complex interaction of proteins that comprise the anatomical structure of podocytes at molecular levels. This chapter lists several aspects of podocyte injuries along with potential mechanisms, including glucose and lipid metabolism disorder, hypertension, RAS activation, micro-inflammation, immune disorder, and other factors. These aspects are not technically separated items, but intertwined with each other in the pathogenesis of podocyte injuries.

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Section: Role Of Hypertension In the Damage Of Podocytesmentioning

confidence: 99%

Role of Podocyte Injury in Glomerulosclerosis

Lü

Wang

Lü

et al. 2019

Advances in Experimental Medicine and Biology

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“… Caucasian [ 69 ] CLIC5 rs321329 SNP influenced response to hydrochlorothiazide treatment, 45722988A/G. Caucasian [ 67 , 70 ] CSMD1 and CUB rs2776546 and rs11993031 AA genotype increased BP response to HCTZ compared to AT and TT genotype. Caucasian [ 69 ] DOT1L rs2269879 SNP was strongly associated with greater SBP and DBP blood in Caucasians.…”

Section: Pharmacogenomics and Inter-individual Variation Of Hypertensmentioning

confidence: 99%

Pharmacogenomics of amlodipine and hydrochlorothiazide therapy and the quest for improved control of hypertension: a mini review

et al. 2019

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Blood pressure (BP) is a complex trait that is regulated by multiple physiological pathways and include but is not limited to extracellular fluid volume homeostasis, cardiac contractility, and vascular tone through renal, neural, or endocrine systems. Uncontrolled hypertension (HTN) has been associated with an increased mortality risk. Therefore, understanding the genetics that underpins and influence BP regulation will have a major impact on public health. Moreover, uncontrolled HTN has been linked to inter-individual variation in the drugs’ response and this has been associated with an individual’s genetics architecture. However, the identification of candidate genes that underpin the genetic basis of HTN remains a major challenge. To date, few variants associated with inter-individual BP regulation have been identified and replicated. Research in this field has accelerated over the past 5 years as a direct result of on-going genome-wide association studies (GWAS) and the progress in the identification of rare gene variants and mutations, epigenetic markers, and the regulatory pathways involved in the pathophysiology of BP. In this review we describe and enhance our current understanding of how genetic variants account for the observed variability in BP response in patients on first-line antihypertensive drugs, amlodipine and hydrochlorothiazide.

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“…This suggests that, in addition to a role in protecting against TGF--induced increases in glomerular permeability (Dahly-Vernon et al, 2005), it may regulate podocyte function via the actin network. Other pathways that regulate the actin cytoskeleton in podocytes include chloride intracellular channel 5A (Wegner et al, 2010); hypertension-induced albuminuria was worse in mice with a knockout of this channel (Tavasoli et al, 2016). The Wilms tumor 1-interacting protein regulates actin in podocytes (Sedor et al, 2011;Kim et al, 2012), however, manipulation of this pathway has not yet been examined for anti-fibrotic or renoprotective effects.…”

Section: Additional Pathwaysmentioning

confidence: 99%

The cytoskeleton as a novel target for treatment of renal fibrosis

Parrish

2016

Pharmacology & Therapeutics

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The chloride intracellular channel 5A stimulates podocyte Rac1, protecting against hypertension-induced glomerular injury

Cited by 21 publications

References 53 publications

Role of Podocyte Injury in Glomerulosclerosis

Role of Podocyte Injury in Glomerulosclerosis

Pharmacogenomics of amlodipine and hydrochlorothiazide therapy and the quest for improved control of hypertension: a mini review

The cytoskeleton as a novel target for treatment of renal fibrosis

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