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Infection and Immunity, July 2000, p. 4108-4116, Vol. 68, No. 7
0019-9567/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Molecular Cloning and Expression of a Gene Encoding
Cryptosporidium parvum Glycoproteins gp40 and gp15
Ana Maria
Cevallos,1
Xiaoping
Zhang,1
Matthew K.
Waldor,1
Smitha
Jaison,1
Xiaoyin
Zhou,2
Saul
Tzipori,1,3
Marian R.
Neutra,2 and
Honorine
D.
Ward1,3,*
Division of Geographic Medicine and Infectious Diseases,
New England Medical Center, Tufts University School of Medicine,
Boston, Massachusetts 021111; Division
of Infectious Diseases, Tufts University School of Veterinary
Medicine, North Grafton, Massachusetts
015363; and GI Cell Biology Laboratory,
Children's Hospital and Harvard Medical School, Boston,
Massachusetts 021152
Received 7 January 2000/Accepted 1 April 2000
Cryptosporidium parvum is a significant cause of
diarrheal disease worldwide. The specific molecules that mediate
C. parvum-host cell interactions and the molecular
mechanisms involved in the pathogenesis of cryptosporidiosis are
unknown. In this study we have shown that gp40, a mucin-like
glycoprotein, is localized to the surface and apical region of invasive
stages of the parasite and is shed from its surface. gp40-specific
antibodies neutralize infection in vitro, and native gp40 binds
specifically to host cells, implicating this glycoprotein in C. parvum attachment to and invasion of host cells. We have cloned
and sequenced a gene designated Cpgp40/15 that encodes gp40
as well as gp15, an antigenically distinct, surface glycoprotein also
implicated in C. parvum-host cell interactions. Analysis of
the deduced amino acid sequence of the 981-bp Cpgp40/15
revealed the presence of an N-terminal signal peptide, a polyserine
domain, multiple predicted O-glycosylation sites, a single
potential N-glycosylation site, and a hydrophobic region at
the C terminus, a finding consistent with what is required for the
addition of a GPI anchor. There is a single copy of
Cpgp40/15 in the C. parvum genome, and this
gene does not contain introns. Our data indicate that the two
Cpgp40/15-encoded proteins, gp40 and gp15, are products of
proteolytic cleavage of a 49-kDa precursor protein which is expressed
in intracellular stages of the parasite. The surface localization of
gp40 and gp15 and their involvement in the host-parasite interaction
suggest that either or both of these glycoproteins may serve as
effective targets for specific preventive or therapeutic measures for cryptosporidiosis.
*
Corresponding author. Mailing address: New England
Medical Center, Division of Geographic Medicine and Infectious
Diseases, 750 Washington St., NEMC Box 041, Boston, MA 02111. Phone:
(617) 636-7032. Fax: (617) 636-5292. E-mail:
hward{at}lifespan.org.
Infection and Immunity, July 2000, p. 4108-4116, Vol. 68, No. 7
0019-9567/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
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