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Journal of Clinical Microbiology, January 1998, p. 73-76, Vol. 36, No. 1
0095-1137/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.
Amplification of Ehrlichial DNA from Dogs 34 Months
after Infection with Ehrlichia canis
Shimon
Harrus,1,*
Trevor
Waner,2
Itzhak
Aizenberg,1
Janet E.
Foley,3
Amy M.
Poland,3 and
Hylton
Bark1
Department of Clinical Sciences, School of
Veterinary Medicine, Hebrew University of Jerusalem, Rehovot
76100,1 and
Israel Institute for
Biological Research, Ness Ziona,2 Israel, and
Center for Companion Animal Health, School of Veterinary
Medicine, University of California, Davis, Davis, California
956163
Received 19 May 1997/Returned for modification 7 July 1997/Accepted 5 September 1997
In order to determine whether dogs in the subclinical phase of
canine monocytic ehrlichiosis (CME) are carriers of Ehrlichia canis and to determine the significance of persistent indirect immunofluorescent anti-E. canis antibody titers during this
phase, PCR was performed with blood, bone marrow, and splenic aspirates collected 34 months postinoculation from six clinically healthy beagle
dogs experimentally infected with E. canis. At least one of
the three samples (spleen, bone marrow, and blood) from four of the six
dogs was PCR positive. The spleens of all four of these dogs were PCR
positive, and the bone marrow and blood of two of the four dogs were
PCR positive. Indirect immunofluorescent-antibody titers increased
progressively during the first 5 months postinfection, remained high
for an additional period of more than 11 months, and declined
thereafter, suggesting that the dogs were recovering from the disease.
Five of the dogs remained seropositive 34 months postinfection. The
data obtained in this study demonstrate for the first time that
clinically healthy dogs in the subclinical phase of CME are carriers of
the rickettsia. It was shown that dogs can harbor E. canis
for years without developing the chronic clinical disease and that dogs
can eliminate the parasite and recover from CME without medical
treatment. Our findings suggest that the spleen is the organ most
likely to harbor E. canis parasites during the subclinical
phase and the last organ to accommodate the parasite before
elimination. It was concluded that PCR of DNA extracted from splenic
aspirates is a reliable method for determining the carrier state of
CME.
*
Corresponding author. Mailing address: Department of
Clinical Sciences, Veterinary Teaching Hospital, Hebrew University of Jerusalem, P.O. Box 12, Rehovot 76100, Israel. Phone: 972-3-9688546. Fax: 972-3-9604079. E-mail: harrus{at}agri.huji.ac.il.
Journal of Clinical Microbiology, January 1998, p. 73-76, Vol. 36, No. 1
0095-1137/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.
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