Mutation of an upstream cleavage site in the BMP4 prodomain leads to tissue-specific loss of activity

doi:10.1242/dev.02368

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First published online 19 April 2006
doi: 10.1242/dev.02368

Development 133, 1933-1942 (2006)
Published by The Company of Biologists 2006

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Mutation of an upstream cleavage site in the BMP4 prodomain leads to tissue-specific loss of activity

Devorah C. Goldman¹, Renee Hackenmiller¹, Takuya Nakayama¹^,*, Shailaja Sopory¹, Crispin Wong¹, Holger Kulessa²^, and Jan L. Christian¹^,

¹ Department of Cell and Developmental Biology, Oregon Health and Sciences University, School of Medicine, 3181 SW Sam Jackson Park Road, Portland, OR 97239-3098, USA.
² Vanderbilt University Medical Center, Division of Gastroenterology, D4108 Medical Center North, Nashville, TN 37232-2279, USA.

Author for correspondence (e-mail: christia{at}ohsu.edu)

Accepted 16 March 2006

ProBMP4 is initially cleaved at a site adjacent to the matureligand (the S1 site) allowing for subsequent cleavage at anupstream (S2) site. Mature BMP4 synthesized from a precursorin which the S2 site cannot be cleaved remains in a complexwith the prodomain that is targeted for lysosomal degradation,and is thus less active when overexpressed in Xenopus. Herewe report that mice carrying a point mutation that preventsS2 processing show severe loss of BMP4 activity in some tissues,such as testes and germ cells, whereas other tissues that aresensitive to Bmp4 dosage, such as the limb, dorsal vertebraeand kidney, develop normally. In a haploinsufficient background,inability to cleave the S2 site leads to embryonic and postnatallethality due to defects in multiple organ systems includingthe allantois, placental vasculature, ventral body wall, eyeand heart. These data demonstrate that cleavage of the S2 siteis essential for normal development and, more importantly, suggestthat this site might be selectively cleaved in a tissue-specificfashion. In addition, these studies provide the first geneticevidence that BMP4 is required for dorsal vertebral fusion andclosure of the ventral body wall.

Key words: Bone morphogenetic protein, Proprotein convertase, Proteolytic activation, Embryonic patterning, Cleavage mutant mouse

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