Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen

Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen

Recombinant BCGs (rBCGs) containing extrachromosomal plasmids with different HIV-1 insert sequences: nef, env (V3J1 and E9Q), gag p17 or whole gag p55 were evaluated for their immunogenicity, safety and persistent infection in BALB/c mice. Animal injected with, rBCG-pIJKV3J1, rBCG-pSO gag p17 or rBC...

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Main Authors: Witthawat Wiriyarat, Sanya Sukpanichnant, Nopporn Sittisombut, Kruavon Balanchandra, Duanthanorm Promkhatkaew, Raywadee Butraporn, Ruengpung Sutthent, Jotika Boonlong, Kazuhiro Matsuo, Mitsuo Honda, Paijit Warachit, Pilaipan Puthavathana
Format: Journal
Published: 2018
Subjects:
Medicine
Online Access:https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=20344390518&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/62416
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Institution: Chiang Mai University
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spelling th-cmuir.6653943832-624162018-09-11T09:27:01Z Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen Witthawat Wiriyarat Sanya Sukpanichnant Nopporn Sittisombut Kruavon Balanchandra Duanthanorm Promkhatkaew Raywadee Butraporn Ruengpung Sutthent Jotika Boonlong Kazuhiro Matsuo Mitsuo Honda Paijit Warachit Pilaipan Puthavathana Medicine Recombinant BCGs (rBCGs) containing extrachromosomal plasmids with different HIV-1 insert sequences: nef, env (V3J1 and E9Q), gag p17 or whole gag p55 were evaluated for their immunogenicity, safety and persistent infection in BALB/c mice. Animal injected with, rBCG-pIJKV3J1, rBCG-pSO gag p17 or rBCG-pSO gag p55 could elicit lymphocyte proliferation as tested by specific HIV-1 peptides or protein antigen. Inoculation with various concentration of rBCG-pSO gag p55 generated satisfactory specific lymphocyte proliferation in dose escalation trials. The rBCG-pSO gag p55 recovered from spleen tissues at different time interval post-inoculation could express the HIV protein as determined by ELISA p24 antigen detection kit. This result indicated that the extrachromosomal plasmid was stable and capable to express Gag protein. It was also demonstrated that rBCGs did not cause serious pathological change in the inoculated animals. The present study suggested the role of BCG as a potential vehicle for using in HIV vaccine development. 2018-09-11T09:27:01Z 2018-09-11T09:27:01Z 2005-03-01 Journal 0125877X 2-s2.0-20344390518 https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=20344390518&origin=inward http://cmuir.cmu.ac.th/jspui/handle/6653943832/62416
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
collection CMU Intellectual Repository
topic Medicine
spellingShingle Medicine
Witthawat Wiriyarat
Sanya Sukpanichnant
Nopporn Sittisombut
Kruavon Balanchandra
Duanthanorm Promkhatkaew
Raywadee Butraporn
Ruengpung Sutthent
Jotika Boonlong
Kazuhiro Matsuo
Mitsuo Honda
Paijit Warachit
Pilaipan Puthavathana
Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen
description Recombinant BCGs (rBCGs) containing extrachromosomal plasmids with different HIV-1 insert sequences: nef, env (V3J1 and E9Q), gag p17 or whole gag p55 were evaluated for their immunogenicity, safety and persistent infection in BALB/c mice. Animal injected with, rBCG-pIJKV3J1, rBCG-pSO gag p17 or rBCG-pSO gag p55 could elicit lymphocyte proliferation as tested by specific HIV-1 peptides or protein antigen. Inoculation with various concentration of rBCG-pSO gag p55 generated satisfactory specific lymphocyte proliferation in dose escalation trials. The rBCG-pSO gag p55 recovered from spleen tissues at different time interval post-inoculation could express the HIV protein as determined by ELISA p24 antigen detection kit. This result indicated that the extrachromosomal plasmid was stable and capable to express Gag protein. It was also demonstrated that rBCGs did not cause serious pathological change in the inoculated animals. The present study suggested the role of BCG as a potential vehicle for using in HIV vaccine development.
format Journal
author Witthawat Wiriyarat
Sanya Sukpanichnant
Nopporn Sittisombut
Kruavon Balanchandra
Duanthanorm Promkhatkaew
Raywadee Butraporn
Ruengpung Sutthent
Jotika Boonlong
Kazuhiro Matsuo
Mitsuo Honda
Paijit Warachit
Pilaipan Puthavathana
author_facet Witthawat Wiriyarat
Sanya Sukpanichnant
Nopporn Sittisombut
Kruavon Balanchandra
Duanthanorm Promkhatkaew
Raywadee Butraporn
Ruengpung Sutthent
Jotika Boonlong
Kazuhiro Matsuo
Mitsuo Honda
Paijit Warachit
Pilaipan Puthavathana
author_sort Witthawat Wiriyarat
title Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen
title_short Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen
title_full Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen
title_fullStr Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen
title_full_unstemmed Specific immune response and pathological findings in BALB/c mice inoculated with recombinat BCG expressing HIV-1 antigen
title_sort specific immune response and pathological findings in balb/c mice inoculated with recombinat bcg expressing hiv-1 antigen
publishDate 2018
url https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=20344390518&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/62416
_version_ 1681425802807214080

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