Antihypertensive therapy induces compartment-specific chemokine expression and a Th1 immune response in the clipped kidney of Goldblatt hypertensive rats.

Oliver Steinmetz; S Sadaghiani; Ulf Panzer; Christian Krebs; Catherine Meyer-Schwesinger; Thomas Streichert; Susanne Fehr; I Hamming; H van Goor; Rolf A.K. Stahl; Ulrich Wenzel

Antihypertensive therapy induces compartment-specific chemokine expression and a Th1 immune response in the clipped kidney of Goldblatt hypertensive rats.

Standard

Antihypertensive therapy induces compartment-specific chemokine expression and a Th1 immune response in the clipped kidney of Goldblatt hypertensive rats. / Steinmetz, Oliver; Sadaghiani, S; Panzer, Ulf ; Krebs, Christian ; Meyer-Schwesinger, Catherine; Streichert, Thomas; Fehr, Susanne; Hamming, I; van Goor, H; Stahl, Rolf A.K.; Wenzel, Ulrich.

In: AM J PHYSIOL-RENAL, Vol. 292, No. 2, 2, 2007, p. 876-887.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Steinmetz, O, Sadaghiani, S, Panzer, U , Krebs, C , Meyer-Schwesinger, C, Streichert, T, Fehr, S, Hamming, I, van Goor, H, Stahl, RAK & Wenzel, U 2007, 'Antihypertensive therapy induces compartment-specific chemokine expression and a Th1 immune response in the clipped kidney of Goldblatt hypertensive rats.', AM J PHYSIOL-RENAL, vol. 292, no. 2, 2, pp. 876-887. <http://www.ncbi.nlm.nih.gov/pubmed/17062848?dopt=Citation>

APA

Steinmetz, O., Sadaghiani, S., Panzer, U., Krebs, C., Meyer-Schwesinger, C., Streichert, T., Fehr, S., Hamming, I., van Goor, H., Stahl, R. A. K., & Wenzel, U. (2007). Antihypertensive therapy induces compartment-specific chemokine expression and a Th1 immune response in the clipped kidney of Goldblatt hypertensive rats. AM J PHYSIOL-RENAL, 292(2), 876-887. [2]. http://www.ncbi.nlm.nih.gov/pubmed/17062848?dopt=Citation

Vancouver

Steinmetz O, Sadaghiani S, Panzer U , Krebs C , Meyer-Schwesinger C, Streichert T et al. Antihypertensive therapy induces compartment-specific chemokine expression and a Th1 immune response in the clipped kidney of Goldblatt hypertensive rats. AM J PHYSIOL-RENAL. 2007;292(2):876-887. 2.

Bibtex

@article{73ab7a201cb348be8a8ae88347fb71f1,

title = "Antihypertensive therapy induces compartment-specific chemokine expression and a Th1 immune response in the clipped kidney of Goldblatt hypertensive rats.",

abstract = "The present study examined the pathogenesis of interstitial inflammation and fibrosis in antihypertensively treated rats with two-kidney, one-clip hypertension. Hypertensive rats were randomized into four groups: no treatment and moderate, intermediate, and intensified lowering of blood pressure with increasing doses of a vasopeptidase inhibitor for 6 wk. The vasopeptidase inhibitor dose dependently lowered blood pressure. The tubulointerstitial damage was accompanied by a diffuse infiltration of mononuclear cells and circumscript mononuclear inflammatory cell cluster formation consisting mainly of T cells and to a lesser degree of macrophages and B cells. Real-time PCR analyses showed a dose-dependent induction of MCP-1 and the Th1-type chemokines IP10 and Mig as well as their receptor CXCR3 and the Th1 cytokine IFN-gamma. In situ hybridization and laser microdissection revealed a strong expression of these Th1-associated transcripts in the clusters and, in the case of MCP-1, also diffusely in the interstitium. The inflammation was accompanied by the appearance of myofibroblasts and synthesis of the fibrogenic factor plasminogen activator inhibitor-1 as well as the collagenase matrix metalloproteinase-2, leading to collagen I upregulation and interstitial scarring. No inflammation or fibrosis was found in normotensive rats treated with the vasopeptidase inhibitor. The renal injury in the clipped kidney is accompanied by compartment-specific chemokine expression and cell cluster formation of Th1 specificity associated with upregulation of fibrogenic proteins and matrix metalloproteinases. These findings suggest that the Th1 chemokines IP10 and Mig as well as their receptor CXCR3 are potential targets for therapeutic interventions in ischemic nephropathy.",

author = "Oliver Steinmetz and S Sadaghiani and Ulf Panzer and Christian Krebs and Catherine Meyer-Schwesinger and Thomas Streichert and Susanne Fehr and I Hamming and {van Goor}, H and Stahl, {Rolf A.K.} and Ulrich Wenzel",

year = "2007",

language = "Deutsch",

volume = "292",

pages = "876--887",

journal = "AM J PHYSIOL-RENAL",

issn = "1931-857X",

publisher = "AMER PHYSIOLOGICAL SOC",

number = "2",

}

RIS

TY - JOUR

T1 - Antihypertensive therapy induces compartment-specific chemokine expression and a Th1 immune response in the clipped kidney of Goldblatt hypertensive rats.

AU - Steinmetz, Oliver

AU - Sadaghiani, S

AU - Panzer, Ulf

AU - Krebs, Christian

AU - Meyer-Schwesinger, Catherine

AU - Streichert, Thomas

AU - Fehr, Susanne

AU - Hamming, I

AU - van Goor, H

AU - Stahl, Rolf A.K.

AU - Wenzel, Ulrich

PY - 2007

Y1 - 2007

N2 - The present study examined the pathogenesis of interstitial inflammation and fibrosis in antihypertensively treated rats with two-kidney, one-clip hypertension. Hypertensive rats were randomized into four groups: no treatment and moderate, intermediate, and intensified lowering of blood pressure with increasing doses of a vasopeptidase inhibitor for 6 wk. The vasopeptidase inhibitor dose dependently lowered blood pressure. The tubulointerstitial damage was accompanied by a diffuse infiltration of mononuclear cells and circumscript mononuclear inflammatory cell cluster formation consisting mainly of T cells and to a lesser degree of macrophages and B cells. Real-time PCR analyses showed a dose-dependent induction of MCP-1 and the Th1-type chemokines IP10 and Mig as well as their receptor CXCR3 and the Th1 cytokine IFN-gamma. In situ hybridization and laser microdissection revealed a strong expression of these Th1-associated transcripts in the clusters and, in the case of MCP-1, also diffusely in the interstitium. The inflammation was accompanied by the appearance of myofibroblasts and synthesis of the fibrogenic factor plasminogen activator inhibitor-1 as well as the collagenase matrix metalloproteinase-2, leading to collagen I upregulation and interstitial scarring. No inflammation or fibrosis was found in normotensive rats treated with the vasopeptidase inhibitor. The renal injury in the clipped kidney is accompanied by compartment-specific chemokine expression and cell cluster formation of Th1 specificity associated with upregulation of fibrogenic proteins and matrix metalloproteinases. These findings suggest that the Th1 chemokines IP10 and Mig as well as their receptor CXCR3 are potential targets for therapeutic interventions in ischemic nephropathy.

AB - The present study examined the pathogenesis of interstitial inflammation and fibrosis in antihypertensively treated rats with two-kidney, one-clip hypertension. Hypertensive rats were randomized into four groups: no treatment and moderate, intermediate, and intensified lowering of blood pressure with increasing doses of a vasopeptidase inhibitor for 6 wk. The vasopeptidase inhibitor dose dependently lowered blood pressure. The tubulointerstitial damage was accompanied by a diffuse infiltration of mononuclear cells and circumscript mononuclear inflammatory cell cluster formation consisting mainly of T cells and to a lesser degree of macrophages and B cells. Real-time PCR analyses showed a dose-dependent induction of MCP-1 and the Th1-type chemokines IP10 and Mig as well as their receptor CXCR3 and the Th1 cytokine IFN-gamma. In situ hybridization and laser microdissection revealed a strong expression of these Th1-associated transcripts in the clusters and, in the case of MCP-1, also diffusely in the interstitium. The inflammation was accompanied by the appearance of myofibroblasts and synthesis of the fibrogenic factor plasminogen activator inhibitor-1 as well as the collagenase matrix metalloproteinase-2, leading to collagen I upregulation and interstitial scarring. No inflammation or fibrosis was found in normotensive rats treated with the vasopeptidase inhibitor. The renal injury in the clipped kidney is accompanied by compartment-specific chemokine expression and cell cluster formation of Th1 specificity associated with upregulation of fibrogenic proteins and matrix metalloproteinases. These findings suggest that the Th1 chemokines IP10 and Mig as well as their receptor CXCR3 are potential targets for therapeutic interventions in ischemic nephropathy.

M3 - SCORING: Zeitschriftenaufsatz

VL - 292

SP - 876

EP - 887

JO - AM J PHYSIOL-RENAL

JF - AM J PHYSIOL-RENAL

SN - 1931-857X

IS - 2

M1 - 2

ER -