grant

Human placental biodisposition of novel antiherpesviral drugs, amenamevir and pritelivir, using ex vivo and in vitro experimental models

Organization UNIVERSITY OF TEXAS MED BR GALVESTONLocation GALVESTON, UNITED STATESPosted 11 Aug 2022Deadline 31 Jul 2026
NIHUS FederalResearch GrantFY20240-4 weeks oldABC20ABCB1ABCB1 geneAcicloftalAclovirAcuteAcycloguanosineAcyclovirAffectAgeAnimal ModelAnimal Models and Related StudiesBirthBody TissuesCargosilCell BodyCellsCells Placenta-TissueCessation of lifeChildbirthChoriocarcinomaCongenital herpes simplexCongenital herpes simplex infectionDNA HelicasesDNA PrimaseDNA Unwinding ProteinsDNA unwinding enzymeDataDeathDevelopmentDisease OutbreaksDomestic RabbitDrug PrecursorsDrug TherapyDrugsEmbryoEmbryonicEndothelial CellsExperimental ModelsExposure toFetal safetyFetusGP170Genital Herpes SimplexGestationGoalsHHV-2HHV2HSVHSV infection in neonatesHSV-1HSV-2HSV1HSV2Herpes GenitalisHerpes SimplexHerpes Simplex InfectionsHerpes Simplex Type 1Herpes Simplex VirusHerpes Simplex Virus 1Herpes Simplex Virus 2Herpes Simplex Virus Type 1Herpes Simplex Virus Type 2Herpes ZosterHerpes infectionHerpes labialis VirusHerpes simplex diseaseHerpes zoster diseaseHerpesviridaeHerpesviridae InfectionsHerpesviridae diseaseHerpesvirus 1Herpesvirus 2 (alpha), HumanHerpesvirus InfectionsHerpesvirus hominis diseaseHerpesvirus progenitalisHerpesvirusesHumanHuman (alpha) herpes virus 2Human Herpesvirus 2Human herpes simplex virus type 2ImmunocompromisedImmunocompromised HostImmunocompromised PatientImmunosuppressed HostIn VitroIncidenceIndividualInvestigationJapanLobuleMDR-1MDR1MDR1 ProteinMediatingMedicationMembrane Transport ProteinsMembrane TransportersMiceMice MammalsModern ManMolecular WeightMorbidityMorbidity - disease rateMothersMultidrug Resistance 1Multidrug Resistance Gene-1Multidrug Resistance Gene-1sMultidrug Resistance ProteinsMultidrug Resistant ProteinsMurineMusNeonatal herpes simplexNeurological disabilityNewborn InfantNewbornsNormal PlacentomaOryctolagus cuniculusOutbreaksP-GPP-GlycoproteinP-Glycoprotein 1 GenePGY-1 ProteinPGY1ParturitionPatientsPerfusionPerinatal transmissionPharmaceutical PreparationsPharmacotherapyPhase 2 Clinical TrialsPhase 3 Clinical TrialsPhase II Clinical TrialsPhase III Clinical TrialsPlacebosPlacentaPlacenta Embryonic TissuePlacentomePoviralPregnancyPregnant WomenPrimasePro-DrugsProdrugsRabbitsRabbits MammalsRecurrenceRecurrentReportingResistanceRiskRisk ReductionRoleSafetySham TreatmentShinglesSimplexvirusTechniquesTherapeuticTimeTissuesToxic effectToxicitiesToxicokineticsTransmissionUmbilical veinUnited StatesViral SheddingViroraxVirus SheddingVirus-Genital HerpesWomanWorkZonaZosterZoviraxagesalternative treatmentchild birthchorioepitheliomaclinical developmentcongenital herpes simplex virus infectionconventional therapyconventional treatmentdevelopmentaldevelopmental toxicitydrug distributiondrug treatmentdrug/agentexpectant motherexpecting motherexperiencefetalgenital herpeshazardhelicaseherpes genitaliaherpes simplex iherpes simplex iiherpes simplex virus 1 infectionherpes simplex virus infectionherpes simplex-1herpes virusherpes zonahuman alphaherpesvirus 2immunosuppressed patientinfected neonateinfected newborninhibitorlipophilicitymenmodel of animalmortalityneonatal HSV infectionneonatal herpesneonatal infectionneonatenew drug treatmentsnew drugsnew pharmacological therapeuticnew therapeuticsnew therapynewborn childnewborn childrennewborn infectionnext generation therapeuticsnovelnovel drug treatmentsnovel drugsnovel pharmaco-therapeuticnovel pharmacological therapeuticnovel therapeuticsnovel therapynucleoside analogphase II protocolphase III protocolplacental transferpre-clinicalpreclinicalpregnantpregnant motherspreventpreventingreduce riskreduce risksreduce that riskreduce the riskreduce these risksreduces riskreduces the riskreducing riskreducing the riskreproductiveresistantresponserisk-reducingsafety testingsham therapysocial rolestandard carestandard treatmenttransmission processtrophoblastvalacyclovirvenereal herpesviral transmissionvirus transmission
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Full Description

ABSTRACT
Genital herpes simplex virus (HSV) infections in pregnancy pose a risk for perinatal transmission of the
virus to neonates, and HSV infections in the newborns are associated with severe morbidity and mortality. A
standard treatment of HSV infections with nucleoside analogs such as acyclovir does not eliminate
asymptomatic viral shedding and is ineffective against acyclovir-resistant HSV strains. Amenamevir and
pritelivir, the helicase-primase inhibitors, represent novel antiherpesviral medications that were developed to
circumvent the limitations of the nucleoside analogs. Both novel drugs completed Phase II clinical trials in
treatment of genital herpes in men and nonpregnant women and demonstrated superiority over placebo and
standard treatments. While amenamevir is currently indicated for the treatment of herpes zoster in Japan,
pritelivir received an FDA Breakthrough Therapy designation and has entered a Phase III clinical trial.
Pregnant women infected with genital herpes could benefit from amenamevir and pritelivir in suppressive or
episodic treatments to prevent the transmission of HSV to neonates. The first step to determine the potential
use of the novel drugs in pregnancy is to obtain preclinical data on their placental biodisposition.
The focus of the proposed investigation is to determine the biodisposition of amenamevir and pritelivir by
human placenta using ex vivo and in vitro experimental models. Meanwhile, assessing fetal safety for
amenamevir and pritelivir, as well as their effect on placental function, is imperative in clinical development of
these novel drugs for their potential use in pregnancy. While existing data from toxicity studies in animal
models suggest a favorable reproductive and developmental safety profile for amenamevir, assessment of
potential developmental hazards of pritelivir remains to be conducted. The specific aims are to
1) Determine the extent of bidirectional transfer of amenamevir and pritelivir across term human placenta
ex vivo, the distribution of these drugs in the placental tissue and maternal and fetal circuits, and their
effect on placental viability and functional parameters;
2) Determine the role of placental efflux membrane transporters in the placental disposition of amenamevir
and pritelivir; and
3) Determine potential embryo-fetal developmental toxicity of pritelivir in mice.
This work will provide the preclinical data needed to determine potential use of amenamevir and pritelivir in
the treatment of newly acquired and reactivated genital herpes in pregnancy as well as in HSV suppressive
therapy during pregnancy. Amenamevir and pritelivir could be effective alternative treatments to manage
genital herpes in pregnancy to reduce the risk of mother-to-neonate HSV transmission in women with
asymptomatic presentation of genital herpes at the time of delivery and for those with inadequate response to
standard treatment with nucleoside analogs.

Grant Number: 5R01HD107428-03
NIH Institute/Center: NIH
Principal Investigator: Valentina Bryant

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