SBIR-STTR Award

Ind-Enabling Preclinical Development of a System for the Multipurpose Prevention of HIV and Unintended Pregnancy
Award last edited on: 3/2/2021

Sponsored Program
SBIR
Awarding Agency
NIH : NIAID
Total Award Amount
$2,219,320
Award Phase
2
Solicitation Topic Code
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Principal Investigator
Thomas J Smith

Company Information

Auritec Pharmaceuticals LLC (AKA: Auritec Pharma~Auritec Pharmaceuticals LLC)

1512 11th Street Suite 203
Santa Monica, CA 90401
   (310) 434-0185
   mblake@auritecpharma.com
   www.auritecpharma.com
Location: Multiple
Congr. District: 36
County: Los Angeles

Phase I

Contract Number: 1R43AI124815-01
Start Date: 7/8/2016    Completed: 6/30/2017
Phase I year
2016
Phase I Amount
$219,324
The broad, long-term goal of this research program is to develop a dual protection intravaginal product that will provide contraception and pre-exposure HIV prophylaxis to women in the developing world. Dual protection is a high priority for the NIH, the WHO and for leading NGOs such as the Gates Foundation. NuvaRing(r) is the only intravaginal ring (IVR) approved for contraception. Truvada(r) [tenofovir disoproxil fumarate (TDF)/emtricitabine (FTC)] is the only drug approved for pre-exposure prophylaxis. Our strategy is based on delivering the drugs of the NuvaRing(r) in conjunction with the drugs of Truvada(r). In an adaptation of our "pod" IVR platform we will develop independent TDF and FTC "beads" that can be attached to an IVR. Simultaneously we will develop a generic version of the NuvaRing(r) that will be approvable through the ANDA mechanism. Through correspondence with the FDA we have determined the Target Product Profile (TPP) including qualitative and quantitative (Q1Q2) requirements for generic NuvaRing(r)s. We have determined the in vitro release methods and specifications and have manufactured batches of pilot generic NuvaRing(r)s. We have developed pod IVRs delivering TDF-FTC and have demonstrated safety, pharmacokinetics, and efficacy in sheep and primate models. The specific aims of this Phase 1 project will be to select the batch of generic NuvaRing(r)s that match the predicate release, to manufacture a pilot batch of the TDF-FTC pods, and to carry out a pilot safety-PK study to demonstrate feasibility in sheep. In Phase 2 and subsequent work we will confirm bioequivalence of the generic ring to the NuvaRing(r) leading to ANDA approval, and confirm bioequivalence of the contraceptive rings to the rings plus pods. Approval of the pods, although requiring large Phase 3 studies, is none the less feasible. Current competing strategies suffer from serious and potentially fatal scientific and regulatory flaws.

Public Health Relevance Statement:


Public Health Relevance:
Dual protection is a high priority for the NIH, the WHO and for leading NGOs such as the Gates Foundation Our strategy is based on piggy-backing contraceptive and pre-exposure strategies that are known to work. We have manufactured generic NuvaRing(r) (etonogestrel/ethinyl estradiol) and pod IVRs delivering Truvada(r) [tenofovir disoproxil fumarate (TDF)/emtricitabine (FTC)]. This Phase 1 study will comprise manufacturing two products that when used simultaneously can provide both contraception and pre-exposure prophylaxis against HIV.

Project Terms:
Agreement; AIDS prevention; Animals; Antiviral Agents; aqueous; Back; base; Chemistry; Clinical; Clinical Trials; Collaborations; Contraceptive Agents; Contraceptive methods; controlled release; Development; Devices; Drug Delivery Systems; drug development; Drug Kinetics; emtricitabine; Engineering; Environment; Ethinyl Estradiol; Etonogestrel; experience; FDA approved; Female of child bearing age; Foundations; Fumarates; Generic Drugs; Goals; HIV; HIV Infections; Hormones; Human; In Vitro; in vitro testing; in vivo; Infectious Pregnancy Complications; innovation; Lead; Licensing; Macaca; Marketing; material transfer agreement; Methods; Modeling; Oryctolagus cuniculus; Pharmaceutical Preparations; Pharmacologic Substance; Phase; phase 1 study; phase 3 study; pre-clinical; Primates; Process; programs; prophylactic; Prophylactic treatment; public health relevance; Qualifying; Research; research clinical testing; Research Personnel; Safety; Sheep; Solubility; Tenofovir; Testing; Therapeutic Equivalency; Time; truvada; unintended pregnancy; United States National Institutes of Health; Unwanted pregnancy; Vaginal Ring; Woman; Work

Phase II

Contract Number: 2R44AI124815-02A1
Start Date: 00/00/00    Completed: 00/00/00
Phase II year
2019
(last award dollars: 2020)
Phase II Amount
$1,999,996

The broad, long-term goal of this research program is to develop an intravaginal multipurpose prevention technology (MPT) product to provide HIV pre-exposure prophylaxis (PrEP) and contraception to women in the developing world. MPT is a high priority for the NIH, the WHO and for leading NGOs. Our strategy is based on delivering the best-in-class HIV PrEP candidates using our proprietary and novel “intravaginal beads” in conjunction with FDA-approved contraceptive IVRs. Truvada® (TDF-FTC combination) is the only FDA-approved drug product for HIV PrEP. However, recent studies have shown NRTI-associated vaginal mitochondrial toxicity, including the data found in our Phase I SBIR efforts. In our original Phase II SBIR (Jan ’18) submission, we presented pre-clinical results for a TDF- FTC bead formulation, and a proposal to adapt the bead technology to the cabotegravir (CBT)-rilpivirine (RPV) combination. At that time, the FDA had just approved Juluca®, which till date remains to be the only two-drug (dolutegravir [DTG] + rilpivirine) medication for HIV treatment. In the past twelve months, several post- marketing studies of Juluca® have been published showing enhanced safety and efficacy. Additionally, the DTG-RPV combination can also act as PrEP agents at very low levels and has a long half-life with lesser known potential for mitochondrial toxicity than NRTIs. On the other hand, the CBT-RPV combination, although in late-stage clinical trials, is not yet approved by the regulatory agencies. Hence, given the significant regulatory and scientific advantages of DTG-RPV drug combination over CBT-RPV, we shifted our product development focus towards the former. One of the main concerns with our original submission was the lack of preliminary data. In response, we resubmit this application with pre-clinical results for the proposed drug selection. Briefly, a 1-month pharmacokinetics (PK) study was performed in a sheep model to evaluate feasibility of the DTG-RPV beads when delivered in combination with a contraceptive IVR (NuvaRing®). The beads demonstrated an average in vivo release of 2.4 mg/d DTG and 0.6 mg/d RPV. The resulting average cervicovaginal fluid (CVF) levels were 537 ng/ml DTG and 807 ng/ml RPV suggesting sustained delivery at concentrations greater than their respective EC50 levels. The drug loading capacity of these beads allows us to formulate them as 3-month beads making it feasible for use in combination with either a monthly Nuvaring® (in this scenario, one bead will be used for three consecutive monthly IVRs over a 3-month period) or a yearly Annovera® (here, four beads will be required for one IVR over a 12-month period), depending on the user’s choice. This Phase II SBIR resubmission proposes the following revised plan: In Year 1, we will manufacture pre- clinical batches of DTG and RPV beads; and conduct IND-enabling safety/PK studies in sheep and macaques. In Year 2, we will test the formulation for efficacy in a macaque model. Finally, we will perform IND-enabling chemistry, manufacturing and controls (CMC) activities for the lead formulation to submit an IND. We have been granted 13 IND approvals, and the only sustained release antiviral drug delivery device ever approved by the FDA (the Vitrasert®) was developed by the Principal Investigator of this proposal. Successful completion of the work described in this proposal will allow human testing of this novel intravaginal MPT.

Public Health Relevance Statement:
NARRATIVE (changes are underlined) The broad, long-term goal of this research program is to develop an intravaginal multipurpose prevention technology (MPT) product that will provide HIV pre-exposure prophylaxis (PrEP) and contraception to women in the developing world. We propose the development of intravaginal “beads” of the long acting potent drugs, dolutegravir (DTG) and rilpivirine (RPV), to be used in conjunction with an FDA-approved contraceptive intravaginal ring (IVR). The DTG-RPV combination is the only commercially available 2-drug regimen for HIV treatment. Thus, we expect significant regulatory advantage with this choice of agents. The specific aims of this Phase II SBIR proposal are to build on the demonstrated feasibility of the bead platform we demonstrated in Phase I. The milestone of this application is to achieve an IND approval for a first-in-human safety and pharmacokinetics testing of the proposed bead-IVR product.

Project Terms:
AIDS prevention; Animals; Anti-Retroviral Agents; Antiviral Agents; base; cervicovaginal; Chemistry; Clinical; Clinical Trials; Collaborations; commercialization; Contraceptive Agents; Contraceptive methods; Data; Development; Devices; Dose; Drug Combinations; Drug Delivery Systems; drug development; Drug Kinetics; emtricitabine; Engineering; Environment; experience; FDA approved; Female of child bearing age; first-in-human; Formulation; Foundations; Fumarates; Goals; Grant; Gynecology; Half-Life; HIV; HIV Infections; HIV therapy; Hormones; Human; in vivo; Infectious Pregnancy Complications; inhibitor/antagonist; innovation; Integrase; Lead; Liquid substance; Macaca; Maintenance; Marketing; microbiome; Mitochondria; Modeling; novel; Nucleosides; Oryctolagus cuniculus; Pharmaceutical Preparations; Phase; pre-clinical; pre-exposure prophylaxis; preclinical development; preclinical efficacy; Prevention; Principal Investigator; Process; product development; programs; Publishing; Recording of previous events; Regimen; Reporting; Research; Research Personnel; response; RNA-Directed DNA Polymerase; Safety; scaffold; Sheep; Small Business Innovation Research Grant; System; Technology; Tenofovir; Testing; Therapeutic Index; Time; Toxic effect; truvada; unintended pregnancy; United States National Institutes of Health; uptake; Vagina; vaginal microbiome; Vaginal Ring; Woman; Work