An SAMT-247 microbicide provides potent protection against intravaginal simian immunodeficiency virus infection of rhesus macaques, whereas an added vaccine component elicits mixed outcomes

Sabrina Helmold Hait; Christopher James Hogge; Mohammad Arif Rahman; Eun Ju Ko; Ruth Hunegnaw; Zuena Mushtaq; Gospel Enyindah-Asonye; Tanya Hoang; Lisa M.Miller Jenkins; Ettore Appella; Daniel H. Appella; Marjorie Robert-Guroff

doi:10.4049/jimmunol.2000165

An SAMT-247 microbicide provides potent protection against intravaginal simian immunodeficiency virus infection of rhesus macaques, whereas an added vaccine component elicits mixed outcomes

Sabrina Helmold Hait, Christopher James Hogge, Mohammad Arif Rahman, Eun Ju Ko, Ruth Hunegnaw, Zuena Mushtaq, Gospel Enyindah-Asonye, Tanya Hoang, Lisa M.Miller Jenkins, Ettore Appella, Daniel H. Appella, Marjorie Robert-Guroff

National Institutes of Health

Research output: Contribution to journal › Article › peer-review

9 Scopus citations

Abstract

Because of microbicide noncompliance and lack of a durable, highly effective vaccine, a combined approach might improve HIV prophylaxis. We tested whether a vaccine-microbicide combination would enhance protection against SIV infection in rhesus macaques. Four macaque groups included vaccine only, vaccine-microbicide, microbicide only, and controls. Vaccine groups were primed twice mucosally with replicating adenovirus type 5 host range mutant SIV env/rev, gag, and nef recombinants and boosted twice i.m. with SIV gp120 proteins in alum. Controls and the microbicide-only group received adenovirus type 5 host range mutant empty vector and alum. The microbicide was SAMT-247, a 2-mercaptobenzamide thioester that targets the viral nucleocapsid protein NCp7, causing zinc ejection and preventing RNA encapsidation. Following vaccination, macaques were challenged intravaginally with repeated weekly low doses of SIV_mac251 administered 3 h after application of 0.8% SAMT-247 gel (vaccine-microbicide and microbicide groups) or placebo gel (vaccine-only and control groups). The microbicide-only group exhibited potent protection; 10 of 12 macaques remained uninfected following 15 SIV challenges. The vaccine-only group developed strong mucosal and systemic humoral and cellular immunity but did not exhibit delayed acquisition compared with adjuvant controls. However, the vaccine-microbicide group exhibited significant acquisition delay compared with both control and vaccine-only groups, indicating further exploration of the combination strategy is warranted. Impaired protection in the vaccine-microbicide group compared with the microbicide-only group was not attributed to a vaccine-induced increase in SIV target cells. Possible Ab-dependent enhancement will be further investigated. The potent protection provided by SAMT-247 encourages its movement into human clinical trials.

Original language	English
Pages (from-to)	3315-3328
Number of pages	14
Journal	Journal of Immunology
Volume	204
Issue number	12
DOIs	https://doi.org/10.4049/jimmunol.2000165
State	Published - Jun 15 2020
Externally published	Yes

Scopus Subject Areas

Immunology and Allergy
Immunology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.4049/jimmunol.2000165

Cite this

Hait, S. H., Hogge, C. J., Rahman, M. A., Ko, E. J., Hunegnaw, R., Mushtaq, Z., Enyindah-Asonye, G., Hoang, T., Jenkins, L. M. M., Appella, E., Appella, D. H., & Robert-Guroff, M. (2020). An SAMT-247 microbicide provides potent protection against intravaginal simian immunodeficiency virus infection of rhesus macaques, whereas an added vaccine component elicits mixed outcomes. Journal of Immunology, 204(12), 3315-3328. https://doi.org/10.4049/jimmunol.2000165

@article{66da0ef5b74349c492524c59ec3b68a5,

title = "An SAMT-247 microbicide provides potent protection against intravaginal simian immunodeficiency virus infection of rhesus macaques, whereas an added vaccine component elicits mixed outcomes",

abstract = "Because of microbicide noncompliance and lack of a durable, highly effective vaccine, a combined approach might improve HIV prophylaxis. We tested whether a vaccine-microbicide combination would enhance protection against SIV infection in rhesus macaques. Four macaque groups included vaccine only, vaccine-microbicide, microbicide only, and controls. Vaccine groups were primed twice mucosally with replicating adenovirus type 5 host range mutant SIV env/rev, gag, and nef recombinants and boosted twice i.m. with SIV gp120 proteins in alum. Controls and the microbicide-only group received adenovirus type 5 host range mutant empty vector and alum. The microbicide was SAMT-247, a 2-mercaptobenzamide thioester that targets the viral nucleocapsid protein NCp7, causing zinc ejection and preventing RNA encapsidation. Following vaccination, macaques were challenged intravaginally with repeated weekly low doses of SIVmac251 administered 3 h after application of 0.8% SAMT-247 gel (vaccine-microbicide and microbicide groups) or placebo gel (vaccine-only and control groups). The microbicide-only group exhibited potent protection; 10 of 12 macaques remained uninfected following 15 SIV challenges. The vaccine-only group developed strong mucosal and systemic humoral and cellular immunity but did not exhibit delayed acquisition compared with adjuvant controls. However, the vaccine-microbicide group exhibited significant acquisition delay compared with both control and vaccine-only groups, indicating further exploration of the combination strategy is warranted. Impaired protection in the vaccine-microbicide group compared with the microbicide-only group was not attributed to a vaccine-induced increase in SIV target cells. Possible Ab-dependent enhancement will be further investigated. The potent protection provided by SAMT-247 encourages its movement into human clinical trials.",

author = "Hait, {Sabrina Helmold} and Hogge, {Christopher James} and Rahman, {Mohammad Arif} and Ko, {Eun Ju} and Ruth Hunegnaw and Zuena Mushtaq and Gospel Enyindah-Asonye and Tanya Hoang and Jenkins, {Lisa M.Miller} and Ettore Appella and Appella, {Daniel H.} and Marjorie Robert-Guroff",

year = "2020",

month = jun,

day = "15",

doi = "10.4049/jimmunol.2000165",

language = "English",

volume = "204",

pages = "3315--3328",

journal = "Journal of Immunology",

issn = "0022-1767",

publisher = "American Association of Immunologists",

number = "12",

}

Hait, SH, Hogge, CJ, Rahman, MA, Ko, EJ, Hunegnaw, R, Mushtaq, Z, Enyindah-Asonye, G, Hoang, T, Jenkins, LMM, Appella, E, Appella, DH & Robert-Guroff, M 2020, 'An SAMT-247 microbicide provides potent protection against intravaginal simian immunodeficiency virus infection of rhesus macaques, whereas an added vaccine component elicits mixed outcomes', Journal of Immunology, vol. 204, no. 12, pp. 3315-3328. https://doi.org/10.4049/jimmunol.2000165

An SAMT-247 microbicide provides potent protection against intravaginal simian immunodeficiency virus infection of rhesus macaques, whereas an added vaccine component elicits mixed outcomes. / Hait, Sabrina Helmold; Hogge, Christopher James; Rahman, Mohammad Arif et al.
In: Journal of Immunology, Vol. 204, No. 12, 15.06.2020, p. 3315-3328.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - An SAMT-247 microbicide provides potent protection against intravaginal simian immunodeficiency virus infection of rhesus macaques, whereas an added vaccine component elicits mixed outcomes

AU - Hait, Sabrina Helmold

AU - Hogge, Christopher James

AU - Rahman, Mohammad Arif

AU - Ko, Eun Ju

AU - Hunegnaw, Ruth

AU - Mushtaq, Zuena

AU - Enyindah-Asonye, Gospel

AU - Hoang, Tanya

AU - Jenkins, Lisa M.Miller

AU - Appella, Ettore

AU - Appella, Daniel H.

AU - Robert-Guroff, Marjorie

PY - 2020/6/15

Y1 - 2020/6/15

N2 - Because of microbicide noncompliance and lack of a durable, highly effective vaccine, a combined approach might improve HIV prophylaxis. We tested whether a vaccine-microbicide combination would enhance protection against SIV infection in rhesus macaques. Four macaque groups included vaccine only, vaccine-microbicide, microbicide only, and controls. Vaccine groups were primed twice mucosally with replicating adenovirus type 5 host range mutant SIV env/rev, gag, and nef recombinants and boosted twice i.m. with SIV gp120 proteins in alum. Controls and the microbicide-only group received adenovirus type 5 host range mutant empty vector and alum. The microbicide was SAMT-247, a 2-mercaptobenzamide thioester that targets the viral nucleocapsid protein NCp7, causing zinc ejection and preventing RNA encapsidation. Following vaccination, macaques were challenged intravaginally with repeated weekly low doses of SIVmac251 administered 3 h after application of 0.8% SAMT-247 gel (vaccine-microbicide and microbicide groups) or placebo gel (vaccine-only and control groups). The microbicide-only group exhibited potent protection; 10 of 12 macaques remained uninfected following 15 SIV challenges. The vaccine-only group developed strong mucosal and systemic humoral and cellular immunity but did not exhibit delayed acquisition compared with adjuvant controls. However, the vaccine-microbicide group exhibited significant acquisition delay compared with both control and vaccine-only groups, indicating further exploration of the combination strategy is warranted. Impaired protection in the vaccine-microbicide group compared with the microbicide-only group was not attributed to a vaccine-induced increase in SIV target cells. Possible Ab-dependent enhancement will be further investigated. The potent protection provided by SAMT-247 encourages its movement into human clinical trials.

AB - Because of microbicide noncompliance and lack of a durable, highly effective vaccine, a combined approach might improve HIV prophylaxis. We tested whether a vaccine-microbicide combination would enhance protection against SIV infection in rhesus macaques. Four macaque groups included vaccine only, vaccine-microbicide, microbicide only, and controls. Vaccine groups were primed twice mucosally with replicating adenovirus type 5 host range mutant SIV env/rev, gag, and nef recombinants and boosted twice i.m. with SIV gp120 proteins in alum. Controls and the microbicide-only group received adenovirus type 5 host range mutant empty vector and alum. The microbicide was SAMT-247, a 2-mercaptobenzamide thioester that targets the viral nucleocapsid protein NCp7, causing zinc ejection and preventing RNA encapsidation. Following vaccination, macaques were challenged intravaginally with repeated weekly low doses of SIVmac251 administered 3 h after application of 0.8% SAMT-247 gel (vaccine-microbicide and microbicide groups) or placebo gel (vaccine-only and control groups). The microbicide-only group exhibited potent protection; 10 of 12 macaques remained uninfected following 15 SIV challenges. The vaccine-only group developed strong mucosal and systemic humoral and cellular immunity but did not exhibit delayed acquisition compared with adjuvant controls. However, the vaccine-microbicide group exhibited significant acquisition delay compared with both control and vaccine-only groups, indicating further exploration of the combination strategy is warranted. Impaired protection in the vaccine-microbicide group compared with the microbicide-only group was not attributed to a vaccine-induced increase in SIV target cells. Possible Ab-dependent enhancement will be further investigated. The potent protection provided by SAMT-247 encourages its movement into human clinical trials.

UR - http://www.scopus.com/inward/record.url?scp=85086285329&partnerID=8YFLogxK

U2 - 10.4049/jimmunol.2000165

DO - 10.4049/jimmunol.2000165

M3 - Article

C2 - 32393514

AN - SCOPUS:85086285329

SN - 0022-1767

VL - 204

SP - 3315

EP - 3328

JO - Journal of Immunology

JF - Journal of Immunology

IS - 12

ER -

An SAMT-247 microbicide provides potent protection against intravaginal simian immunodeficiency virus infection of rhesus macaques, whereas an added vaccine component elicits mixed outcomes

Abstract

Scopus Subject Areas

UN SDGs

Access to Document

Other files and links

Fingerprint

Cite this