Peter J. Cowan scite author profile

Podocyte dysfunction, represented by foot process effacement and proteinuria, is often the starting point for progressive kidney disease. Therapies aimed at the cellular level of the disease are currently not available. Here we show that induction of urokinase receptor (uPAR) signaling in podocytes leads to foot process effacement and urinary protein loss via a mechanism that includes lipid-dependent activation of alphavbeta3 integrin. Mice lacking uPAR (Plaur-/-) are protected from lipopolysaccharide (LPS)-mediated proteinuria but develop disease after expression of a constitutively active beta3 integrin. Gene transfer studies reveal a prerequisite for uPAR expression in podocytes, but not in endothelial cells, for the development of LPS-mediated proteinuria. Mechanistically, uPAR is required to activate alphavbeta3 integrin in podocytes, promoting cell motility and activation of the small GTPases Cdc42 and Rac1. Blockade of alphavbeta3 integrin reduces podocyte motility in vitro and lowers proteinuria in mice. Our findings show a physiological role for uPAR signaling in the regulation of kidney permeability.

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Gut Microbiota Elicits a Protective Immune Response against Malaria Transmission

Yılmaz

Portugal

Tran

et al. 2014

Cell

301

390

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SummaryGlycosylation processes are under high natural selection pressure, presumably because these can modulate resistance to infection. Here, we asked whether inactivation of the UDP-galactose:β-galactoside-α1-3-galactosyltransferase (α1,3GT) gene, which ablated the expression of the Galα1-3Galβ1-4GlcNAc-R (α-gal) glycan and allowed for the production of anti-α-gal antibodies (Abs) in humans, confers protection against Plasmodium spp. infection, the causative agent of malaria and a major driving force in human evolution. We demonstrate that both Plasmodium spp. and the human gut pathobiont E. coli O86:B7 express α-gal and that anti-α-gal Abs are associated with protection against malaria transmission in humans as well as in α1,3GT-deficient mice, which produce protective anti-α-gal Abs when colonized by E. coli O86:B7. Anti-α-gal Abs target Plasmodium sporozoites for complement-mediated cytotoxicity in the skin, immediately after inoculation by Anopheles mosquitoes. Vaccination against α-gal confers sterile protection against malaria in mice, suggesting that a similar approach may reduce malaria transmission in humans.PaperFlick

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Renal Xenografts From Triple-Transgenic Pigs Are Not Hyperacutely Rejected but Cause Coagulopathy in Non-Immunosuppressed Baboons

Cowan¹,

Aminian²,

Barlow³

et al. 2000

Transplantation

196

164

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Regulated necrosis in kidney ischemia-reperfusion injury

Pefanis

Ierino

Murphy

et al. 2019

Kidney International

243

145

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Peter J. Cowan

Modification of kidney barrier function by the urokinase receptor

Gut Microbiota Elicits a Protective Immune Response against Malaria Transmission

Renal Xenografts From Triple-Transgenic Pigs Are Not Hyperacutely Rejected but Cause Coagulopathy in Non-Immunosuppressed Baboons

Regulated necrosis in kidney ischemia-reperfusion injury

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