An HSV-2 Trivalent Vaccine Is Immunogenic in Rhesus Macaques and Highly Efficacious in Guinea Pigs

Awasthi, Sita; Hook, Lauren M.; Shaw, Carolyn E.; Pahar, Bapi; Stagray, Jacob A.; Liu, David; Veazey, Ronald S.; Friedman, Harvey M.

doi:10.1371/journal.ppat.1006141

Cited by 48 publications

(82 citation statements)

References 50 publications

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“…However, the risk of using live vaccines in pregnancy is likely to be unacceptable at the regulatory level. It might be fruitful, therefore, to reconsider the use of polyvalent subunit, inactivated, or disabled infectious single-cycle (DISC) virus preparations in at-risk women for the protection of their babies from neonatal HSV ( 48 , 49 ).…”

Section: Discussionmentioning

confidence: 99%

Maternal Antiviral Immunoglobulin Accumulates in Neural Tissue of Neonates To Prevent HSV Neurological Disease

Jiang

Leib

Manivanh

et al. 2017

mBio

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While antibody responses to neurovirulent pathogens are critical for clearance, the extent to which antibodies access the nervous system to ameliorate infection is poorly understood. In this study on herpes simplex virus 1 (HSV-1), we demonstrate that HSV-specific antibodies are present during HSV-1 latency in the nervous systems of both mice and humans. We show that antibody-secreting cells entered the trigeminal ganglion (TG), a key site of HSV infection, and persisted long after the establishment of latent infection. We also demonstrate the ability of passively administered IgG to enter the TG independently of infection, showing that the naive TG is accessible to antibodies. The translational implication of this finding is that human fetal neural tissue could contain HSV-specific maternally derived antibodies. Exploring this possibility, we observed HSV-specific IgG in HSV DNA-negative human fetal TG, suggesting passive transfer of maternal immunity into the prenatal nervous system. To further investigate the role of maternal antibodies in the neonatal nervous system, we established a murine model to demonstrate that maternal IgG can access and persist in neonatal TG. This maternal antibody not only prevented disseminated infection but also completely protected the neonate from neurological disease and death following HSV challenge. Maternal antibodies therefore have a potent protective role in the neonatal nervous system against HSV infection. These findings strongly support the concept that prevention of prenatal and neonatal neurotropic infections can be achieved through maternal immunization.

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Section: Discussionmentioning

confidence: 99%

Maternal Antiviral Immunoglobulin Accumulates in Neural Tissue of Neonates To Prevent HSV Neurological Disease

Jiang

Leib

Manivanh

et al. 2017

mBio

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“… 67 Given that the gD/AS04 subunit vaccine demonstrated no efficacy against HSV-2 in the Phase 3 field study 68 a variety of vaccines employing multiple antigenic targets (gC, gD, gE in combination) have been tested and have met with success in animal models of HSV pathogenesis. 69 – 71 Furthermore, Genocea Biosciences tested the GEN-003 vaccine containing both soluble gD and the ICP4.2 T-cell epitope in phase 2 trials, resulting in a measurable reduction in viral shedding (though comparable to valacyclovir drug therapy). 72 …”

Section: Neutralizing Vs Non-neutralizing Antibody Responsesmentioning

confidence: 99%

A new era in cytomegalovirus vaccinology: considerations for rational design of next-generation vaccines to prevent congenital cytomegalovirus infection

2018

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Human cytomegalovirus (HCMV), a member of the beta-herpesvirus family, is the most common cause of congenital infection worldwide as well as an important cause of morbidity in transplant recipients and immunosuppressed individuals. An estimated 1 in 150 infants are infected with HCMV at birth, which can result in lifelong, debilitating neurologic sequelae including microcephaly, sensorineural hearing loss, and cognitive impairment. Natural maternal immunity to HCMV decreases the frequency of reinfection and reduces risk of congenital transmission but does not completely protect against neonatal disease. Thus, a vaccine to reduce the incidence and severity of infant infection is a public health priority. A variety of candidate HCMV vaccine approaches have been tried previously, including live-attenuated viruses, glycoprotein subunit formulations, viral vectors, and single/bivalent DNA plasmids, but all have failed to reach target endpoints in clinical trials. Nevertheless, there is a great deal to be learned from the successes and failures of the HCMV vaccine field (both congenital and transplant-associated), as well as from vaccine development efforts for other herpesvirus pathogens including herpes simplex virus 1 and 2, varicella zoster virus, and Epstein–Barr virus. Here, we review those successes and failures, evaluating recent cutting-edge discoveries that have shaped the HCMV vaccine field and identifying topics of critical importance for future investigation. These considerations will inform rational design and evaluation of next-generation vaccines to prevent HCMV-associated congenital infection and disease.

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“…Nevertheless, there have been some positive clinical achievements. For example, in a recent preclinical study, an HSV2 trivalent subunit vaccine containing glycoproteins C, D, and E (gC2, gD2, and gE2) showed immunogenicity in rhesus macaques and displayed more than 97% efficacy in guinea pigs . Also, results from a phase III clinical trial study showed that a recombinant glycoprotein D vaccine, conferred approximately 74% prevention of genital HSV disease in women seronegative for both HSV serotypes …”

Section: Introductionmentioning

confidence: 99%

Toll‐like receptors as novel therapeutic targets for herpes simplex virus infection

Jahanban‐Esfahlan

Seidi

Majidinia

et al. 2019

Reviews in Medical Virology

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Seropositivity for HSV reaches more than 70% within the world population, and yet no approved vaccine exists. While HSV1 is responsible for keratitis, encephalitis, and labialis, HSV2 carriers have a high susceptibility to other STD infections, such as HIV. Induction of antiviral innate immune responses upon infection depends on a family of pattern recognition receptors called Toll-like receptors (TLR). TLRs bridge innate and adaptive immunity by sensing virus infection and activating antiviral immune responses. HSV adopts smart tricks to evade innate immunity and can also manipulate TLR signaling to evade the immune system or even confer destructive effects in favor of virus replication. Here, we review mechanisms by which HSV can trick TLR signaling to impair innate immunity. Then, we analyze the role of HSV-mediated molecular cues, in particular, NF-κB signaling, in promoting protective versus destructive effects of TLRs. Finally, TLR-based therapeutic opportunities with the goal of preventing or treating HSV infection will be discussed.

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An HSV-2 Trivalent Vaccine Is Immunogenic in Rhesus Macaques and Highly Efficacious in Guinea Pigs

Cited by 48 publications

References 50 publications

Maternal Antiviral Immunoglobulin Accumulates in Neural Tissue of Neonates To Prevent HSV Neurological Disease

Maternal Antiviral Immunoglobulin Accumulates in Neural Tissue of Neonates To Prevent HSV Neurological Disease

A new era in cytomegalovirus vaccinology: considerations for rational design of next-generation vaccines to prevent congenital cytomegalovirus infection

Toll‐like receptors as novel therapeutic targets for herpes simplex virus infection

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