Anuria, Omphalocele, and Perinatal Lethality in Mice Lacking the Cd34-Related Protein Podocalyxin

doi:10.1084/jem.194.1.13

Published online 2 July 2001. doi:10.1084/jem.194.1.13

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© The Rockefeller University Press, 0022-1007/2001/7/13/ $5.00
The Journal of Experimental Medicine, Volume 194, Number 1, July 2, 2001 13-28

Original Article

Anuria, Omphalocele, and Perinatal Lethality in Mice Lacking the Cd34-Related Protein Podocalyxin

Regis Doyonnas^a, David B. Kershaw^b, Christian Duhme^a, Helen Merkens^a, Shierley Chelliah^a, Thomas Graf^c, and Kelly M. McNagny^a

^a The Biomedical Research Centre, University of British Columbia, Vancouver, BC, Canada
^b University of Michigan Medical Center, Department of Pediatrics, Ann Arbor, MI 48109
^c Albert Einstein College of Medicine, Bronx, NY 10461
Biomedical Research Centre, University of British Columbia, 2222 Health Sciences Mall, Vancouver, BC, Canada V6T 1Z3.604-822-7815604-822-7810

Kelly{at}brc.ubc.ca

Podocalyxin is a CD34-related sialomucin that is expressed athigh levels by podocytes, and also by mesothelial cells, vascularendothelia, platelets, and hematopoietic stem cells. To elucidatethe function of podocalyxin, we generated podocalyxin-deficient(podxl^–/–) mice by homologous recombination. Nullmice exhibit profound defects in kidney development and diewithin 24 hours of birth with anuric renal failure. Althoughpodocytes are present in the glomeruli of the podxl^–/–mice, they fail to form foot processes and slit diaphragms andinstead exhibit cell–cell junctional complexes (tightand adherens junctions). The corresponding reduction in permeable,glomerular filtration surface area presumably leads to the observedblock in urine production. In addition, podxl^–/–mice frequently display herniation of the gut (omphalocele),suggesting that podocalyxin may be required for retraction ofthe gut from the umbilical cord during development. Hematopoieticand vascular endothelial cells develop normally in the podocalyxin-deficientmice, possibly through functional compensation by other sialomucins(such as CD34). Our results provide the first example of anessential role for a sialomucin in development and suggest thatdefects in podocalyxin could play a role in podocyte dysfunctionin renal failure and omphalocele in humans.

Key Words: sialomucin • umbilical hernia • podocyte • hematopoiesis • vascular endothelium

Abbreviations used in this paper: AF, amniotic fluid; AJ, adherensjunction; CD2AP, CD2-associated protein; EC, endothelial cell;ES, embryonic stem; FP, foot process; GBM, glomerular basementmembrane; GLEPP, glomerular epithelial protein; HEV, high endothelialvenule; HPRT, hypoxanthine-guanine phosphoribosyl transferase;JC, junctional complex; KO, knockout; MP, major process; NPHS,congenital nephrotic syndrome; PECAM, platelet endothelial celladhesion molecule; SD, slit diaphragm; TEM, transmission electronmicroscopy; TJ, tight junction.

R. Doyonnas and D.B. Kershaw contributed equally to this manuscript.

C. Duhme's present address is Green College Residence, Universityof British Columbia, Vancouver, BC, Canada.

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