Molecular Cloning and Characterization of a Defective Recombinant Feline Leukaemia Virus Associated with Myeloid Leukaemia

Overview

Journal J Gen Virol

Specialty Microbiology

Date 1990 Feb 1

PMID 2155287

Citations 18

Authors

T Tzavaras

M Stewart

A McDougall

R Fulton

N Testa

D E Onions

J C Neil

Affiliations

Soon will be listed here.

Abstract

The GM1 strain of feline leukaemia virus (FeLV) was isolated from a naturally occurring case of myeloid leukaemia and induces severe haematopoietic abnormalities, including myeloblastic leukaemia, on inoculation into cats. Molecular clones of FeLV-GM1 proviruses were obtained and studied by restriction enzyme mapping, blot hybridization and partial DNA sequence analysis. Two types of clone were isolated; the first was a replication-competent FeLV of subgroup A, resembling other low or minimally pathogenic FeLV-A isolates; the second was replication-defective with extensive deletions and mutations in gag and pol, although it has an intact env gene of subgroup B phenotype. Large segments of the defective proviruses, from the 5' leader sequence upstream of the gag gene to the 5' half of the env gene, show structural hallmarks of endogenous FeLV-related proviruses. Infectious FeLV-GM1 viruses recovered after transfection were tested for their leukaemogenic potential in newborn cats. Early polyclonal myeloproliferative changes were observed in cats inoculated with FeLV-A/GM1 alone, although these were more pronounced in animals receiving the full FeLV-AB/GM1 complex reconstituted by cotransfection of the defective virus FeLV-B with its FeLV-A helper. Analysis of viruses in the bone marrow showed that replication of the subgroup B component is delayed and restricted to a proportion of cats. Most of the infected cats developed persistent abnormalities of haematopoiesis and one progressed to disseminated myeloid leukaemia. The defective recombinant FeLV-B/GM1 appears to play an indirect but important role in myeloid leukaemogenesis.

Citing Articles

Molecular detection of feline leukemia virus in clinically ill cats in Klang Valley, Malaysia.

Mummoorthy K, Yasmin A, Arshad S, Omar A, Nur-Fazila S, Anand P Vet World. 2021; 14(2):405-409.

PMID: 33776305 PMC: 7994122. DOI: 10.14202/vetworld.2021.405-409.

Multiple Introductions of Domestic Cat Feline Leukemia Virus in Endangered Florida Panthers.

Chiu E, Kraberger S, Cunningham M, Cusack L, Roelke M, VandeWoude S Emerg Infect Dis. 2018; 25(1):92-101.

PMID: 30561312 PMC: 6302599. DOI: 10.3201/eid2501.181347.

A Retrospective Examination of Feline Leukemia Subgroup Characterization: Viral Interference Assays to Deep Sequencing.

Chiu E, Hoover E, VandeWoude S Viruses. 2018; 10(1).

PMID: 29320424 PMC: 5795442. DOI: 10.3390/v10010029.

Barriers to Infection of Human Cells by Feline Leukemia Virus: Insights into Resistance to Zoonosis.

Terry A, Kilbey A, Naseer A, Levy L, Ahmad S, Watts C J Virol. 2016; 91(5).

PMID: 28031367 PMC: 5309941. DOI: 10.1128/JVI.02119-16.

Mice lacking the sodium-dependent phosphate import protein, PiT1 (SLC20A1), have a severe defect in terminal erythroid differentiation and early B cell development.

Liu L, Sanchez-Bonilla M, Crouthamel M, Giachelli C, Keel S Exp Hematol. 2013; 41(5):432-43.e7.

PMID: 23376999 PMC: 3948150. DOI: 10.1016/j.exphem.2013.01.004.