Cross-clade HIV-1-specific neutralizing IgA in mucosal and systemic compartment of HIV-1-exposed, persistently seronegative subjects.
Date
2002Author
Devito, C
Hinkula, J
Kaul, R
Kimani, J
Kiama, P
Lopalco, L
Barass, C
Piconi, S
Trabattoni, D
Type
ArticleLanguage
enMetadata
Show full item recordURI
http://www.ncbi.nlm.nih.gov/pubmed/12138348http://erepository.uonbi.ac.ke:8080/xmlui/handle/123456789/42100
Citation
Devito C, Hinkula J, Kaul R, Kimani J, Kiama P, Lopalco L, Barass C, Piconi S, Trabattoni D, ;Cross-clade HIV-1-specific neutralizing IgA in mucosal and systemic compartments of HIV-1-exposed, persistently seronegative subjects;J Acquir Immune Defic Syndr. 2002 Aug 1;30(4):413-20.Bwayo JJ, Plummer F, Clerici M, Broliden KSponsorhip
There is an urgent need for a universally effective HIV-1 vaccine, but whether a vaccine will be able to protect against HIV-1 of different clades is a significant concern. IgA from HIV-1-exposed, persistently seronegative (HEPS) subjects has been shown to neutralize HIV-1 and to block epithelial HIV-1 transcytosis, and it may target novel HIV-1 epitopes. We have tested the ability of plasma and mucosal IgA purified from HEPS subjects to neutralize HIV-1 primary isolates of different viral clades and phenotypes. IgA from two groups of HEPS subjects was tested: sex workers from Nairobi, Kenya, where clades A and D predominate, and the heterosexual partners of individuals infected by clade B virus. HIV-1-infected and low-risk uninfected individuals were included as controls. IgA purified from the blood, genital tract, and saliva of most HEPS sex workers demonstrated significant cross-clade HIV-1 neutralization, whereas a more clade-restricted pattern of neutralization was found in partners of clade B-infected individuals. IgA purified from HIV-1-infected individuals also mediated cross-clade neutralization, whereas IgA from uninfected controls lacked neutralizing activity. In conclusion, mucosal and plasma IgA from HEPS subjects neutralizes HIV-1 of different clades. This ability to induce HIV-1-specific systemic and mucosal IgA may be an important feature of an effective prophylactic HIV-1 vaccine.Publisher
University of Nairobi, College of Health Sciences,
Collections
- Faculty of Health Sciences (FHS) [10387]