Abrogation of Experimental Colitis Correlates with Increased Apoptosis in Mice Deficient for CD44 Variant Exon 7 (CD44v7)

doi:10.1084/jem.191.12.2053

Published online 12 June 2000.

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© The Rockefeller University Press, 0022-1007/2000/6/2053/ $5.00
The Journal of Experimental Medicine, Volume 191, Number 12, June 19, 2000 2053-2064

Original Article

Abrogation of Experimental Colitis Correlates with Increased Apoptosis in Mice Deficient for CD44 Variant Exon 7 (CD44v7)

Bianca M. Wittig^a, Britt Johansson^b, Margot Zöller^a, Christoph Schwärzler^b, and Ursula Günthert^b
^a German Cancer Research Center, D-69120 Heidelberg, Germany
^b Basel Institute for Immunology, CH-4005 Basel, Switzerland

Correspondence to: Ursula Günthert, Basel Institute for Immunology, Grenzacher Strasse 487, CH-4005 Basel, Switzerland. Tel:41-61-605-1111 Fax:41-61-605-1385 E-mail:guenthert{at}bii.ch.

Experimental colitis in mice is characterized by infiltrationof activated T helper (Th) cells and macrophages into the laminapropria. Particularly, these cells expressed CD44 variant exon7 (CD44v7)-containing isoforms. Upregulation of CD44v7 isoformswas induced by CD40 ligation, an inflammation-driving interactionbetween activated Th cells and macrophages. To define the roleof CD44v7 in colitis, mice bearing a targeted deletion for exonv7 were generated. In trinitrobenzene sulfonic acid–inducedcolitis, wild-type mice developed severe signs of persistentinflammation. Mice lacking CD44v7 initially showed unspecificinflammation, then recovered completely. The pathogenic originwas shown to reside in bone marrow–derived CD44v7⁺ cells,because adoptive transfer experiments demonstrated an absoluterequirement for CD44v7 on hematopoietic cells for maintenanceof colitis. Interleukin (IL)-10–deficient mice, whichdevelop a chronic Th1-driven enterocolitis, were crossbred withCD44v6/v7 null mice. In IL-10 x CD44v6/v7 double deficient mice,intestinal inflammation developed only weakly and at an olderage. Analysis of cell death in the inflamed lesions revealedthat mononuclear cells in the CD44v7 null infiltrates had higherrates of apoptosis than those from wild-type mice. Thus, theregion encoded by CD44v7 appears to be essential for survivalof effector lymphocytes, resulting in persistence of inflammation.

Key Words: experimental colitis, CD44 knockout, IL-10 knockout, TNBS, apoptosis

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