Bolstering Components of the Immune Response Compromised by Prior Exposure to Adenovirus: Guided Formulation Development for a Nasal Ebola Vaccine

Choi, Jin Huk; Schafer, Stephen C.; Freiberg, Alexander N.; Croyle, Maria A.

doi:10.1021/mp5006454

Cited by 8 publications

(13 citation statements)

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“…Calorimetric assessment of the optimized film matrix indicates that it has a Tg' above 140°C, suggesting that at each of the temperatures used in the assessment of adenovirus stability, none of the excipients were susceptible to crystallization, which could compromise the adenovirus capsid and facilitate precipitation of buffer components and other excipients, allowing the virus to remain stably suspended in an amorphous polymer matrix during long-term storage. We have shown previously that addition of a zwitterionic surfactant to our preparations at the concentration used here significantly improves the potency of an adenovirus-based Ebola vaccine (29,30) and attributed it to the fact that it is capable of significantly reducing the energy barrier for the virus to cross the lipid bilayer of the cell membrane (57). Here, we show that it is paramount for conferring stability of virus in the film matrix and rehydrated films when stored at ambient and elevated temperatures (Figs.…”

Section: Downloaded Frommentioning

confidence: 90%

“…In this paper, we summarize our efforts to develop a novel platform that can reduce costs associated with storage, distribution, and administration of vaccines and other biological drug products. Initially, more than 400 formulations were screened for their ability to enhance the immune response of an adenovirus-based Ebola vaccine (29). Formulations providing favorable in vivo data were then assessed for their ability to stabilize recombinant adenoviruses in a thin, peelable film matrix (Fig.…”

Section: Introductionmentioning

confidence: 99%

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Novel technology for storage and distribution of live vaccines and other biological medicines at ambient temperature

et al. 2020

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A novel, thin-film platform that preserves live viruses, bacteria, antibodies, and enzymes without refrigeration for extended periods of time is described. Studies with recombinant adenovirus in an optimized formulation that supports recovery of live virus through 16 freeze-thaw cycles revealed that production of an amorphous solid with a glass transition above room temperature and nitrogen-hydrogen bonding between virus and film components are critical determinants of stability. Administration of live influenza virus in the optimized film by the sublingual and buccal routes induced antibody-mediated immune responses as good as or better than those achieved by intramuscular injection. This work introduces the possibility of improving global access to a variety of medicines by offering a technology capable of reducing costs of production, distribution, and supply chain maintenance.

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Section: Downloaded Frommentioning

confidence: 90%

Section: Introductionmentioning

confidence: 99%

Novel technology for storage and distribution of live vaccines and other biological medicines at ambient temperature

et al. 2020

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“…These approaches have demonstrated both a significantly improved persistence of HAdv in the circulation after intravenous virus administration and a reduction in the amount of inflammatory cytokines in the blood [48,131]. Although shielding of HAdv with PEG effectively prevents virus neutralization by preexisting neutralizing antibodies, allowing for repeated gene delivery in a gene transfer or vaccination setting [132,133], the utility of this approach in other applications has limitations. Specifically, although shielding oncolytic HAdv with PEG or protein conjugates significantly increases the efficacy of oncolytic HAdvbased vectors in mouse models [130,132], after the initial round of replication, the progeny of oncolytic virus produced in tumor sites would not be covered with PEG or protein shields, thus exposing the virus to receptors and cells of the innate immune system.…”

Section: Complexity Of Designing Hadv Vectors With Reduced Innate Immmentioning

confidence: 99%

Innate immunity to adenovirus: lessons from mice

2019

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Adenovirus is a highly evolutionary successful pathogen, as it is widely prevalent across the animal kingdom, infecting hosts ranging from lizards and frogs to dolphins, birds, and humans. Although natural adenovirus infections in humans rarely cause severe pathology, intravenous injection of high doses of adenovirus-based vectors triggers rapid activation of the innate immune system, leading to cytokine storm syndrome, disseminated intravascular coagulation, thrombocytopenia, and hepatotoxicity, which individually or in combination may cause morbidity and mortality. Much of the information on exactly how adenovirus activates the innate immune system has been gathered from mouse experimental systems. Intravenous administration of adenovirus to mice revealed mechanistic insights into cellular and molecular components of the innate immunity that detect adenovirus particles, activate pro-inflammatory signaling pathways and cytokine production, sequester adenovirus particles from the bloodstream, and eliminate adenovirus-infected cells. Collectively, this information greatly improved our understanding of mechanisms of activation of innate immunity to adenovirus and may pave the way for designing safer adenovirus-based vectors for therapy of genetic and acquired human diseases.Human adenovirus (HAdv) is remarkably efficient at infecting and replicating in human cells. These properties made HAdv-based vectors an attractive platform for developing novel therapeutics to combat genetic diseases and cancer. Unfortunately, early studies revealed that HAdv is a potent activator of the innate and adaptive arms of the immune system, and administration to animals or patients of high doses of HAdv-based vectors, especially via an intravascular route, leads to severe immunopathology, manifested by cytokine storm syndrome, disseminated intravascular coagulation, thrombocytopenia, and hepatotoxicity, which may lead to morbidity and even mortality. To harness the full potential of HAdv as a gene delivery or oncolytic virus platform, a complete understanding of the molecular and cellular components of innate Abbreviations is a founder, shareholder, and chief scientific officer of AdCure Bio, LLC, which develops Ad-based therapies for clinical use.

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“…Formulations of currently marketed biologics for nasal administration support stability at refrigerated and ambient temperatures [13,14]. Several formulations that support stability of recombinant adenoviruses (the platform of two of the vaccine candidates) for nasal administration have been described [15,16]. Information about the stability of attenuated vesicular stomatitis V viruses (VSV), the third vaccine platform is limited and should be evaluated further since storing this vaccine at ultralow temperatures currently poses a significant administrative challenge and additional expense and delay in setting up clinical trials in Africa [17].…”

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confidence: 99%

“…VSV vectors have been evaluated for nasal immunization against HIV [24,25]. Formulations that stabilize recombinant adenovirus at ambient temperatures and improve the immune response have been developed for intranasal administration and could be implemented in products currently in the clinic [15][16]26].…”

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confidence: 99%