Nucleotide sequence of the glycoprotein gene and intergenic region of the Lassa virus S genome RNA

The complete nucleotide sequence of the rat alpha 1-acid glycoprotein gene has been determined from an isolated lambda recombinant bacteriophage. Southern blot analysis and DNA sequencing indicate that there is only one gene per genome; it contains six exons and is located within a 3,200-base-pair fragment starting from a TATA box and extending to the polyadenylation signal AATAAA. Transcription starts 37 base pairs upstream from the beginning of the translation codon ATG. The TATA box (TATAAA) lies 26 base pairs upstream from this site. The gene contains several potential glucocorticoid receptor-binding sites, both inside and outside the structural gene.

Download Full-text

Nucleotide sequence specifying the glycoprotein gene, gB, of herpes simplex virus type 1

Virology ◽

10.1016/0042-6822(84)90397-0 ◽

1984 ◽

Vol 133 (2) ◽

pp. 301-314 ◽

Cited By ~ 88

Author(s):

David J. Bzik ◽

Barbara A. Fox ◽

Neal A. DeLuca ◽

Stanley Person

Keyword(s):

Herpes Simplex Virus ◽

Herpes Simplex ◽

Nucleotide Sequence ◽

Virus Type ◽

Herpes Simplex Virus Type ◽

Glycoprotein Gene ◽

Simplex Virus

Download Full-text

A Lassa Virus Live-Attenuated Vaccine Candidate Based on Rearrangement of the Intergenic Region

mBio ◽

10.1128/mbio.00186-20 ◽

2020 ◽

Vol 11 (2) ◽

Cited By ~ 3

Author(s):

Yingyun Cai ◽

Masaharu Iwasaki ◽

Daisuke Motooka ◽

David X. Liu ◽

Shuiqing Yu ◽

...

Keyword(s):

Intergenic Region ◽

Guinea Pigs ◽

Cultured Cells ◽

Vaccine Candidate ◽

Lassa Fever ◽

Lassa Virus ◽

Wild Type ◽

Live Attenuated Vaccine ◽

Attenuated Vaccine ◽

Western Africa

ABSTRACT Lassa virus (LASV) poses a significant public health problem within the regions of Lassa fever endemicity in Western Africa. LASV infects several hundred thousand individuals yearly, and a considerable number of Lassa fever cases are associated with high morbidity and lethality. No approved LASV vaccine is available, and current therapy is limited to an off-label usage of ribavirin that is only partially effective and associated with significant side effects. The impact of Lassa fever on human health, together with the limited existing countermeasures, highlights the importance of developing effective vaccines against LASV. Here, we present the development and characterization of a recombinant LASV (rLASV) vaccine candidate [rLASV(IGR/S-S)], which is based on the presence of the noncoding intergenic region (IGR) of the small (S) genome segment (S-IGR) in both large (L) and S LASV segments. In cultured cells, rLASV(IGR/S-S) was modestly less fit than wild-type rLASV (rLASV-WT). rLASV(IGR/S-S) was highly attenuated in guinea pigs, and a single subcutaneous low dose of the virus completely protected against otherwise lethal infection with LASV-WT. Moreover, rLASV(IGR/S-S) was genetically stable during serial passages in cultured cells. These findings indicate that rLASV(IGR/S-S) can be developed into a LASV live-attenuated vaccine (LAV) that has the same antigenic composition as LASV-WT and a well-defined mechanism of attenuation that overcomes concerns about increased virulence that could be caused by genetic changes in the LAV during multiple rounds of multiplication. IMPORTANCE Lassa virus (LASV), the causative agent of Lassa fever, infects several hundred thousand people in Western Africa, resulting in many lethal Lassa fever cases. No U.S. Food and Drug Administration-licensed countermeasures are available to prevent or treat LASV infection. We describe the generation of a novel LASV live-attenuated vaccine candidate rLASV(IGR/S-S), which is based on the replacement of the large genomic segment noncoding intergenic region (IGR) with that of the small genome segment. rLASV(IGR/S-S) is less fit in cell culture than wild-type virus and does not cause clinical signs in inoculated guinea pigs. Importantly, rLASV(IGR/S-S) protects immunized guinea pigs against an otherwise lethal exposure to LASV.

Download Full-text