Literature DB >> 18216318

Acute rejection modulates gene expression in the collecting duct.

Bayram Edemir1, Stefan Reuter, Reka Borgulya, Rita Schröter, Ute Neugebauer, Gert Gabriëls, Eberhard Schlatter.   

Abstract

Kidney transplantation, especially when associated with acute rejection, leads to changes in the expression of many genes, including those encoding solute transporters and water channels. In a rat model of acute rejection after allogeneic renal transplantation, impaired renal function, increased urine volume, and increased fractional excretion of sodium were observed. Gene array analysis revealed that these findings were associated with significant downregulation of water channels (aquaporin-1, -2, -3, and -4) and transporters of sodium, glucose, urea, and other solutes. In addition, changes in expression of various receptors, kinases, and phosphatases that modulate the expression or activity of renal transport systems were observed. Syngeneic transplantation or treatment with cyclosporine A following allogeneic transplantation did not impair graft function but did lead to the downregulation of aquaporin-1, -3, and -4 and several solute transporters. However, expression of aquaporin-2 and the epithelial sodium channel did not change, suggesting that the downregulation of these transporters following allogeneic transplantation is rejection-dependent. In conclusion, changes in gene expression may explain the impaired handling of solute and water after allogeneic transplantation, especially during acute rejection. Treatment with cyclosporine A improves the regulation of solute and water by preventing the downregulation of aquaporin-2 and epithelial sodium channel, even though many other transporter genes remain downregulated.

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Year:  2008        PMID: 18216318      PMCID: PMC2391056          DOI: 10.1681/ASN.2007040513

Source DB:  PubMed          Journal:  J Am Soc Nephrol        ISSN: 1046-6673            Impact factor:   10.121


  39 in total

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7.  Acute rejection after rat renal transplantation leads to downregulation of NA+ and water channels in the collecting duct.

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9.  Long-term treatment with cyclosporine decreases aquaporins and urea transporters in the rat kidney.

Authors:  Sun-Woo Lim; Can Li; Bo-Kyung Sun; Ki-Hwan Han; Wan-Young Kim; Yoon-Wha Oh; Jong-Un Lee; Peter F Kador; Mark A Knepper; Jeff M Sands; Jin Kim; Chul-Woo Yang
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10.  Renal transplantation modulates expression and function of receptors and transporters of rat proximal tubules.

Authors:  Ana Velic; Jochen R Hirsch; Jasmin Bartel; Regina Thomas; Rita Schröter; Heike Stegemann; Bayram Edemir; Christian August; Eberhard Schlatter; Gert Gabriëls
Journal:  J Am Soc Nephrol       Date:  2004-04       Impact factor: 10.121

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3.  Urinary extracellular vesicular release of aquaporins in patients with renal transplantation.

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5.  Carbenoxolone induces apoptosis and inhibits survivin and survivin-ΔEx3 genes expression in human leukemia K562 cells.

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6.  Detecting Renal Allograft Inflammation Using Quantitative Urine Metabolomics and CXCL10.

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7.  Apocynin and catalase prevent hypertension and kidney injury in Cyclosporine A-induced nephrotoxicity in rats.

Authors:  Yong Chia Tan; Munavvar Abdul Sattar; Ahmad F Ahmeda; Nurzalina Abdul Karim Khan; Vikneswaran Murugaiyah; Ashfaq Ahmad; Zurina Hassan; Gurjeet Kaur; Mohammed Hadi Abdulla; Edward James Johns
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8.  C4d Deposition after Allogeneic Renal Transplantation in Rats Is Involved in Initial Apoptotic Cell Clearance.

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  8 in total

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