Infectivity of a Cryptosporidium parvum isolate of cervine origin for healthy adults and interferon-γ knockout mice

Pablo C. Okhuysen; Stephen M. Rich; Cynthia L. Chappell; Kevin A. Grimes; Giovanni Widmer; Xiaochuan Feng; Saul Tzipori

doi:10.1086/340132

Infectivity of a Cryptosporidium parvum isolate of cervine origin for healthy adults and interferon-γ knockout mice

Pablo C. Okhuysen, Stephen M. Rich, Cynthia L. Chappell, Kevin A. Grimes, Giovanni Widmer, Xiaochuan Feng, Saul Tzipori

Research output: Contribution to journal › Article › peer-review

76 Scopus citations

Abstract

The infectivity of a Cryptosporidium parvum isolate of cervine origin (type 2, Moredun) propagated in calves was investigated simultaneously in healthy adult human volunteers and in interferon-γ knockout (GKO) mice. After exposure to 100-3000 oocysts, 16 volunteers recorded, for a duration of 6 weeks, the number and form of stools that they passed and any symptoms that they experienced. Oocyst excretion was assessed by enzyme-linked immunosorbent assay and direct immunofluorescence assay. Eleven subjects (69%) became ill, and 8 subjects (50%) shed oocysts in stool. The median duration of illness was 169 h, and the median number of unformed stools passed was 24. The duration and intensity of symptoms were more severe than were those associated with previously studied isolates. The median infectious dose was estimated to be 300 oocysts for humans and 1 oocyst for the GKO mouse model. The Moredun isolate was more pathogenic than the reference GCH-1 isolate. The GKO mouse model of cryptosporidiosis is useful for discerning isolate-specific differences in pathogenicity.

Original language	English (US)
Pages (from-to)	1320-1325
Number of pages	6
Journal	Journal of Infectious Diseases
Volume	185
Issue number	9
DOIs	https://doi.org/10.1086/340132
State	Published - May 1 2002

ASJC Scopus subject areas

Immunology and Allergy
Infectious Diseases

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@article{dffd8862b1fe4c568e6d75ebf9520432,

title = "Infectivity of a Cryptosporidium parvum isolate of cervine origin for healthy adults and interferon-γ knockout mice",

abstract = "The infectivity of a Cryptosporidium parvum isolate of cervine origin (type 2, Moredun) propagated in calves was investigated simultaneously in healthy adult human volunteers and in interferon-γ knockout (GKO) mice. After exposure to 100-3000 oocysts, 16 volunteers recorded, for a duration of 6 weeks, the number and form of stools that they passed and any symptoms that they experienced. Oocyst excretion was assessed by enzyme-linked immunosorbent assay and direct immunofluorescence assay. Eleven subjects (69%) became ill, and 8 subjects (50%) shed oocysts in stool. The median duration of illness was 169 h, and the median number of unformed stools passed was 24. The duration and intensity of symptoms were more severe than were those associated with previously studied isolates. The median infectious dose was estimated to be 300 oocysts for humans and 1 oocyst for the GKO mouse model. The Moredun isolate was more pathogenic than the reference GCH-1 isolate. The GKO mouse model of cryptosporidiosis is useful for discerning isolate-specific differences in pathogenicity.",

author = "Okhuysen, {Pablo C.} and Rich, {Stephen M.} and Chappell, {Cynthia L.} and Grimes, {Kevin A.} and Giovanni Widmer and Xiaochuan Feng and Saul Tzipori",

note = "Funding Information: Financial support: US Food and Drug Administration (FD-U-001621-01); Environmental Protection Agency (CR-819814, CR-824759); National Institutes of Health (AI-41735, RR-02558); Department of Agriculture (NRI 98-00919).",

year = "2002",

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language = "English (US)",

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AU - Okhuysen, Pablo C.

AU - Rich, Stephen M.

AU - Chappell, Cynthia L.

AU - Grimes, Kevin A.

AU - Widmer, Giovanni

AU - Feng, Xiaochuan

AU - Tzipori, Saul

N1 - Funding Information: Financial support: US Food and Drug Administration (FD-U-001621-01); Environmental Protection Agency (CR-819814, CR-824759); National Institutes of Health (AI-41735, RR-02558); Department of Agriculture (NRI 98-00919).

PY - 2002/5/1

Y1 - 2002/5/1

N2 - The infectivity of a Cryptosporidium parvum isolate of cervine origin (type 2, Moredun) propagated in calves was investigated simultaneously in healthy adult human volunteers and in interferon-γ knockout (GKO) mice. After exposure to 100-3000 oocysts, 16 volunteers recorded, for a duration of 6 weeks, the number and form of stools that they passed and any symptoms that they experienced. Oocyst excretion was assessed by enzyme-linked immunosorbent assay and direct immunofluorescence assay. Eleven subjects (69%) became ill, and 8 subjects (50%) shed oocysts in stool. The median duration of illness was 169 h, and the median number of unformed stools passed was 24. The duration and intensity of symptoms were more severe than were those associated with previously studied isolates. The median infectious dose was estimated to be 300 oocysts for humans and 1 oocyst for the GKO mouse model. The Moredun isolate was more pathogenic than the reference GCH-1 isolate. The GKO mouse model of cryptosporidiosis is useful for discerning isolate-specific differences in pathogenicity.

AB - The infectivity of a Cryptosporidium parvum isolate of cervine origin (type 2, Moredun) propagated in calves was investigated simultaneously in healthy adult human volunteers and in interferon-γ knockout (GKO) mice. After exposure to 100-3000 oocysts, 16 volunteers recorded, for a duration of 6 weeks, the number and form of stools that they passed and any symptoms that they experienced. Oocyst excretion was assessed by enzyme-linked immunosorbent assay and direct immunofluorescence assay. Eleven subjects (69%) became ill, and 8 subjects (50%) shed oocysts in stool. The median duration of illness was 169 h, and the median number of unformed stools passed was 24. The duration and intensity of symptoms were more severe than were those associated with previously studied isolates. The median infectious dose was estimated to be 300 oocysts for humans and 1 oocyst for the GKO mouse model. The Moredun isolate was more pathogenic than the reference GCH-1 isolate. The GKO mouse model of cryptosporidiosis is useful for discerning isolate-specific differences in pathogenicity.

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Infectivity of a Cryptosporidium parvum isolate of cervine origin for healthy adults and interferon-γ knockout mice

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