March 2025
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17 Reads
Bioconjugate Chemistry
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March 2025
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17 Reads
Bioconjugate Chemistry
March 2025
Journal of Pharmacology and Experimental Therapeutics
August 2024
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19 Reads
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2 Citations
Biomaterials
May 2024
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4 Reads
Journal of Pharmacology and Experimental Therapeutics
May 2024
Journal of Pharmacology and Experimental Therapeutics
March 2024
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80 Reads
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5 Citations
Introduction Fentanyl and fentanyl analogs (F/FA) have become increasingly common adulterants in counterfeit prescription pills and illicit street drug mixtures due to their ease of synthesis and exceedingly high potency. The ongoing epidemic of fatal overdoses fueled by F/FA continues to highlight the need for longer-acting therapies than naloxone (NLX), the current gold-standard for reversing opioid overdoses, which shows limited efficacy to prevent renarcotization associated with F/FA toxicity. A novel opioid reversal agent based on covalent naloxone nanoparticles (cNLX-NP) has been shown to blunt fentanyl-induced respiratory depression out to 48 hr, demonstrating its potential therapeutic utility. The purpose of this study was to characterize how rapidly cNLX-NP reverses fentanyl-induced respiratory effects as well as the duration of its protective effects. Methods Sprague Dawley male rats (n=6/group) were tested on an oximeter for baseline percent arterial oxygen saturation (%SaO2) challenged with 0.1 mg/kg SC fentanyl and 15 min later given 10 mg/kg IM doses of NLX, nalmefene (NLMF), or cNLX-NP and continuously monitored via oximetry for 10 minutes. One week later the experiment was repeated using a 1:1 mixture of NLX:cNLX-NP as the reversal agent in the rats that previously received NLX alone. Results While both NLX and NLMF rapidly reversed %SaO2 to baseline within 1 min, rats that received cNLX-NP did not return to >90% SaO2 levels until 9 min after administration. Similarly, heart and breath rates returned to baseline within 1 min of treatment with NLX and NLMF but did not return to baseline until 10 minutes after cNLX-NP administration. In contrast, NLX:cNLX-NP reversed all fentanyl-induced respiratory depressive effects within one minute. Discussion While cNLX-NP alone may not sufficiently reverse F/FA overdose in a timely manner, mixing free NLX with cNLX-NP can provide a mechanism to both rapidly reverse fentanyl-related effects and maintain extended protection against synthetic opioid toxicity. These data support further development of cNLX-NP as a fast-acting and long-lasting antidote to treat F/FA-induced respiratory depression and overdose, and potentially prevent renarcotization in humans.
December 2023
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22 Reads
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4 Citations
ACS Pharmacology & Translational Science
July 2023
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80 Reads
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20 Citations
npj Vaccines
Opioid use disorders (OUD) and overdose are public health threats worldwide. Widespread access to highly potent illicit synthetic opioids such as fentanyl is driving the recent rise in fatal overdoses. Vaccines containing fentanyl-based haptens conjugated to immunogenic carrier proteins offer a long-lasting, safe, and cost-effective strategy to protect individuals from overdose upon accidental or deliberate exposure to fentanyl and its analogs. Prophylactic or therapeutic active immunization with an anti-fentanyl vaccine induces the production of fentanyl-specific antibodies that bind the drug in the blood and prevent its distribution to the brain, which reduces its reinforcing effects and attenuates respiratory depression and bradycardia. To increase the efficacy of a lead anti-fentanyl vaccine, this study tested whether the incorporation of synthetic toll-like receptor (TLR) 4 and TLR7/8 agonists as vaccine adjuvants would increase vaccine efficacy against fentanyl challenge, overdose, and self-administration in either rats or Hanford miniature pigs. Formulation of the vaccine with a nucleolipid TLR7/8 agonist enhanced its immunogenicity and efficacy in preventing fentanyl-induced respiratory depression, analgesia, bradycardia, and self-administration in either rats or mini-pigs. These studies support the use of TLR7/8 adjuvants in vaccine formulations to improve their clinical efficacy against OUD and potentially other substance use disorders (SUD).
May 2023
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10 Reads
Journal of Pharmacology and Experimental Therapeutics
May 2023
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11 Reads
Journal of Pharmacology and Experimental Therapeutics
... Recently, PLGA/lipid hybrid NPs have been extensively explored as potent nanocarriers for various antigens. For example, recent research results have demonstrated that the OVA-encapsulated/adsorbed hNPs were capable of eliciting an extraordinary antigen-specific immune response [21,22]. Moreover, the versatile functionalized lipids offer the opportunity to display proteins on the surface of the hNPs which could increase the immunogenicity of a protein antigen [23]. ...
August 2024
Biomaterials
... For example, the transfer half-life of naloxone from the plasma to the MORs at the effector site in the brain is only 6.5 min. After intravenous infusion, the elimination half-life of naloxone is 32-33 min, whereas the plasma-to-effect site transfer half-life for morphine is 2-3 h; for fentanyl and its congeners it is only 5-15 min (64)(65)(66). Reversal of morphineinduced RD by naloxone is short-lived (28). ...
March 2024
... There has been research on vaccines to treat substance use disorders and overdose, including to nicotine, [12] cocaine, [13] and heroin, [14] though none have been licensed, and there have not yet been any authorized or licensed vaccines targeting protection from overdose. [15] Awareness of these efforts among the public and biomedical professionals is likely minimal and attitudes toward substance use, [16] addiction, [17] and vaccines [18] are complex, suggesting a non-linear path toward vaccine acceptability. ...
December 2023
ACS Pharmacology & Translational Science
... However, exogenous adjuvants (e.g., Advax and mastoparan-7) have been established to increase immune responses to both VLP-and non-VLP-based vaccines for drugs of abuse 41,76 . Recently, A TLR7/8 agonist was shown to significantly improve the vaccine efficacy of anti-fentanyl vaccines 77 . It has been shown also that while IgG is the predominant isotype in blood and should play a significant role in drug sequestration within blood, IgA also plays an important role in mediating opioid vaccine protection 36 . ...
July 2023
npj Vaccines
... Efforts to better understand and account for B-cell and T-cell activity, for example, can help to more accurately identify those most likely to demonstrate a good response to candidate vaccines [21,32,120]. In our current oxycodone vaccine trial, years of preclinical work to understand B and T cells, Fc effector functions, microbiome factors, and cytokine levels contributed to development of our vaccine [21,32,100,103,121,122]. In our ongoing clinical trial [NCT04458545; 107] efforts to characterize B cell activity as a potential biomarker of vaccine response is therefore an important aim. ...
August 2021
... These vaccines have shown efficacy in rodent and nonhuman primate models after three or more immunizations [31][32][33][34] . Fentanyl vaccine candidates have also been developed with the leading candidates using a cross-reactive material 197 (CRM-197) -based design and demonstrating promising pre-clinical protection with plans to enter clinical trials [35][36][37] . ...
December 2021
npj Vaccines
... In this study, we explored the effect of liposomal formulations of INI-4001 and their surface charge on immunogenicity and efficacy of anti-fentanyl vaccines, a promising vaccine candidate to counteract deliberate and accidental fentanyl exposure-related overdose and OUD 6,25 . INI-4001 is a novel lipidated oxoadenine TLR7/8 agonist that was previously shown to significantly enhance the immunogenicity and efficacy of the anti-fentanyl vaccine when adsorbed on Alum 11,12 . ...
November 2018
Journal of Pharmacology and Experimental Therapeutics