Pharmacological Profiling of Antifentanyl Monoclonal Antibodies in Combination with Naloxone in Pre- and Postexposure Models of Fentanyl Toxicity

Baehr, Carly; Wu, Mariah; Pandit, Sujata G.; Arias-Umana, Jose; AuCoin, David P.; Pravetoni, Marco

doi:10.1124/jpet.121.001048

Cited by 13 publications

(9 citation statements)

References 24 publications

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“…All mAbs significantly reduced brain fentanyl and increased fentanyl concentration in serum, though HY11-6B2_Ch was least effective at sequestering fentanyl in serum. Because HY6-F9_Mu has previously shown efficacy in rats, 19 , 40 the efficacy of HY6-F9_Ch was also compared to HY6-F9_Mu in rats ( Figure 3 ). Rats were passively immunized with 40 mg/kg of HY6-F9_Mu or HY6-F9_Ch, and 24 hours later challenged with 0.1 mg/kg fentanyl.…”

Section: Resultsmentioning

confidence: 99%

“…Anti-fentanyl murine mAb and chAb isolated by other groups have been shown to prevent fentanyl-induced antinociception and brain distribution at similar mAb and fentanyl doses to those used here. 20 , 21 Meanwhile, HY6-F9_Mu has been shown to prevent fentanyl effects in both mice and rats, 19 and to reverse respiratory depression in rats, 40 a more clinically relevant measure for fentanyl overdose than antinociception. However, as murine and chimeric mAbs are unsuitable for human use due to ADA responses, 26–28 humanization is essential for clinical advancement.…”

Section: Discussionmentioning

confidence: 99%

“…These mAbs offer a promising new treatment for counteracting the effects of synthetic opioid-induced toxicity by providing an alternative to treatment with naloxone, or via dual administration of mAb and naloxone. 40 Further clinical development of the lead α-fentanyl mAbs described herein will grant a first-in-class opportunity to assess the clinical potential of a mAb-based therapeutic at preventing the loss of life caused by synthetic opioids.…”

Section: Discussionmentioning

confidence: 99%

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Advancing humanized monoclonal antibody for counteracting fentanyl toxicity towards clinical development

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Baehr

Silva-Ortiz

et al. 2022

Human Vaccines & Immunotherapeutics

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Innovative therapies to complement current treatments are needed to curb the growing incidence of fatal overdoses related to synthetic opioids. Murine and chimeric monoclonal antibodies (mAb) specific for fentanyl and its analogs have demonstrated pre-clinical efficacy in preventing and reversing drug-induced toxicity in rodent models. However, mAb-based therapeutics require extensive engineering as well as in vitro and in vivo characterization to advance to first-in-human clinical trials. Here, novel murine anti-fentanyl mAbs were selected for development based on affinity for fentanyl, and efficacy in counteracting the pharmacological effects of fentanyl in mice. Humanization and evaluation of mutations designed to eliminate predicted post-translational modifications resulted in two humanized mAbs that were effective at preventing fentanyl-induced pharmacological effects in rats. These humanized mAbs showed favorable biophysical properties with respect to aggregation and hydrophobicity by chromatography-based assays, and thermostability by dynamic scanning fluorimetry. These results collectively support that the humanized anti-fentanyl mAbs developed herein warrant further clinical development for treatment of fentanyl toxicity.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Advancing humanized monoclonal antibody for counteracting fentanyl toxicity towards clinical development

Hicks

Baehr

Silva-Ortiz

et al. 2022

Human Vaccines & Immunotherapeutics

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“…Figures 1A and B) (Raleigh et al, 2019;Robinson et al, 2020;Crouse et al, 2022). After sortase A-mediated conjugation of fen-sort to the surface VSG (Fent-VAST), sortagging efficiency was assessed by flow cytometry using a mouse anti-fentanyl mAb (Baehr et al, 2020(Baehr et al, , 2022. This revealed that 100% of the trypanosomes had been decorated with the fent-sort (Figure 2A).…”

Section: The Vast Platform Induces Antibody Titers Protective Against...mentioning

confidence: 99%

“…These strategies have also been used to generate mAbs against a variety of target drugs of abuse including fentanyl. Notably, fentanyl-specific mAbs are effective in both preventing and reversing fentanyl's pharmacological effects in rodent models, further highlighting the promise of immunotherapeutics in the opioid space (Smith et al, 2019;Baehr et al, 2020Baehr et al, , 2022Ban et al, 2021). While promising indeed, there remains a lack of clinical output in this space and a desperate need for additional intervention options.…”

Section: Introductionmentioning

confidence: 99%

An Epitope-Focused Trypanosome-Derived Vaccine Platform Elicits High-Affinity Antibodies and Immunity Against Fentanyl Effects

Triller

Vlachou

Hashemi

et al. 2022

Preprint

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SummaryPoorly antigenic small molecules pose challenges for the production of clinically efficacious antibodies. To address this, we have developed an immunization platform derived from the antigenic surface coat of the African trypanosome. Through sortase-based conjugation of antigens to the trypanosome surface coat protein variant surface glycoprotein (VSG), we created the VAST (VSG-immunogen Array by Sortase Tagging). We used VAST to elicit protective immunity to the effects fentanyl. Immunizing mice with fentanyl-VAST generated serological memory and protection from fentanyl challenge. Employing single-cell RNAseq, we then developed a streamlined method that synergizes with the VAST to identify immunization-elicited memory B cells and the antibodies they encode. All antibodies selected by this method displayed picomolar affinities for fentanyl. Passive immunization protected animals from fentanyl, while crystallography revealed that the mAbs bind fentanyl in an unusually deep pocket suited to small molecules, demonstrating the ability of the VAST to elicit high-quality therapeutic antibodies.

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Pharmacological Profiling of Antifentanyl Monoclonal Antibodies in Combination with Naloxone in Pre- and Postexposure Models of Fentanyl Toxicity

Cited by 13 publications

References 24 publications

Advancing humanized monoclonal antibody for counteracting fentanyl toxicity towards clinical development

Advancing humanized monoclonal antibody for counteracting fentanyl toxicity towards clinical development

An Epitope-Focused Trypanosome-Derived Vaccine Platform Elicits High-Affinity Antibodies and Immunity Against Fentanyl Effects

A trypanosome-derived immunotherapeutics platform elicits potent high-affinity antibodies, negating the effects of the synthetic opioid fentanyl

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