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The moloney murine leukemia virus enhancer and its flanking sequences collaborate to determine virulence in T-cell lymphomagenesis

✍ Scribed by Pick-Hoong Yuen; Yong-Ho Khang; Abhay Kumar; Paul F. Szurek; Elizabeth A. Maull


Publisher
John Wiley and Sons
Year
1991
Tongue
English
Weight
763 KB
Volume
4
Category
Article
ISSN
0899-1987

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✦ Synopsis


A panel of recombinant virus genomes was constructed by exchanging homologous genome fragments between the potent T-cell lymphoma inducer Moloney murine leukemia virus (MoMuLV) and its closely related but significantly less virulent relative MoMuLV-TB. Testing of these recombinant viruses in BALB/c mice established that only nucleotide changes within the Clal(-590)-Kpnl(36) fragment altered virulence. Fine analysis of this fragment showed that while mutations within the enhancer of MoMuLV-TB attenuated the latency period most, mutations within the MoMuLV-TB fragments flanking the enhancer also helped reduce the virulence of MoMuLV. The present study also suggests that the small difference in the relative number of lymphomas that developed primarily in the spleens of MoMuLV- or MoMuLV-TB-infected mice may correlate with nucleotide differences between the Clal-Kpnl fragments of the two viruses. However, the significantly greater proportion of premature death observed in MoMuLV-TB-relative to MoMuLV-infected mice could not be correlated with nucleotide differences in a specific genome fragment.


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✍ Roger S. Case; Yong-Ho Khang; Abhay Kumar; Pick-Hoong Yuen 📂 Article 📅 1990 🏛 John Wiley and Sons 🌐 English ⚖ 1016 KB

## Abstract The genetic determinant responsible for virulence in Moloney murine leukemia virus (MoMuLV) induced T‐cell lymphomagenesis has recently been mapped [J Virol 63:471–480, 1989] by homologous genomic fragment exchange between MoMuLV and MoMuLV‐TB to the Clal/Xbal at the 3' end of the genom