Clinical trials of Shigella vaccines: two steps forward and one step back on a long, hard road

Levine, Myron M.; Kotloff, Karen L.; Barry, Eileen M.; Pasetti, Marcela F.; Sztein, Marcelo B.

doi:10.1038/nrmicro1662

Cited by 306 publications

(339 citation statements)

References 114 publications

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“…Ty21a offers moderate efficacy against typhoid fever (reported at 48% over 3 years in a recent systematic review [13]), although there is no evidence to suggest that this is lower than protection offered to travelers from high-income, non-endemic countries [14,15]. One live-attenuated Shigella vaccine candidate was reactogenic and immunogenic when administered to North-American adults; however, when the same vaccine was tested in Bangladesh, it elicited no adverse reactions and failed to induce a serological response in any recipient [16,17]. Poor immunogenicity has also been observed for an oral-killed cholera vaccine among children in Nicaragua compared with Sweden [18].…”

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confidence: 99%

Causes of Impaired Oral Vaccine Efficacy in Developing Countries

et al. 2017

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Oral vaccines are less immunogenic when given to infants in low-income compared with high-income countries, limiting their potential public health impact. Here, we review factors that might contribute to this phenomenon, including transplacental antibodies, breastfeeding, histo blood group antigens, enteric pathogens, malnutrition, microbiota dysbiosis and environmental enteropathy. We highlight several clear risk factors for vaccine failure, such as the inhibitory effect of enteroviruses on oral poliovirus vaccine. We also highlight the ambiguous and at times contradictory nature of the available evidence, which undoubtedly reflects the complex and interconnected nature of the factors involved. Mechanisms responsible for diminished immunogenicity may be specific to each oral vaccine. Interventions aiming to improve vaccine performance may need to reflect the diversity of these mechanisms. Enteric pathogens are a substantial threat to public health. This threat takes many forms, from the toxin-producing bacteria (e.g., Vibrio cholerae) and flagellated protozoa (e.g., Giardia lamblia) that colonize the mucosal surface of the small intestine to the enteroviruses that are capable of spreading via the bloodstream to the CNS, causing acute flaccid paralysis (e.g., poliovirus). Each year, enteric pathogens cause hundreds of millions of cases of diarrhea and approximately 800,000 deaths, the vast majority of which occur among children in low-income countries [1]. The most common causes of childhood diarrheal morbidity include rotavirus, Cryptosporidium, enterotoxigenic Escherichia coli and Shigella [2].Vaccines against enteric pathogens are important tools for mitigating this disease burden. Oral vaccines offer several distinct benefits compared with parenteral vaccines. They can be produced in large quantities at relatively low cost, are easy to administer and have the capacity to induce local immunity in the intestinal mucosa, thereby protecting vaccinated individuals against subsequent infection and -by blocking onward transmission -enhancing herd immunity [3,4]. Currently licensed oral vaccines include live-attenuated poliovirus vaccines containing one, two or three serotypes, live-attenuated rotavirus vaccines (Rotarix R , RotaTeq R , Lanzhou lamb rotavirus vaccine [China only] and Rotavac R [India only]), live-attenuated cholera vaccine (CVD 103-HgR or Vaxchora TM ), inactivated cholera vaccines (Dukoral R and Shanchol R ) and live-attenuated typhoid vaccine (Ty21a). Other oral vaccines are in development, including those against Shigella, enterotoxigenic E. coli, Campylobacter and Clostridium difficile, as well as several novel rotavirus vaccine candidates (including the human neonatal vaccine RV3-BB [5] and an oral bovine pentavalent vaccine [6]).Yet oral vaccines have an Achilles' heel -their immunogenicity and efficacy is impaired in low-income countries that experience the greatest burden of enteric disease (Box 1). For example, Rotarix has a 1-year protective efficacy against severe rotavirus-associated gas...

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Causes of Impaired Oral Vaccine Efficacy in Developing Countries

et al. 2017

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“…Current vaccines strategies against Shigella can be grouped into two fundamental approaches: live-attenuated vaccines and nonliving vaccines [6][7][8]. While the essential concern regarding live attenuated candidates is to find the appropriate balance between immunogenicity and acceptable side effects, different scenery appears for inactivated whole cell or subunit vaccines.…”

Section: Discussionmentioning

confidence: 99%

“…In the absence of an existing effective vaccine and the ever-increasing frequency of antimicrobial-resistant Shigella strains worldwide, Shigellosis has become a major source of concern [5]. Several candidate shigellosis vaccines are currently in development including live attenuated, inactivated whole cell, or subunit vaccines [6][7][8]. Considering intrinsic risk of living vaccines, the non-living vaccine alternative, including either inactivated whole-cell or acellular approaches, results the safest direction.…”

Section: Introductionmentioning

confidence: 99%

Towards a non-living vaccine against Shigella flexneri: From the inactivation procedure to protection studies

Camacho

Souza-Rebouças

Irache

et al. 2013

Methods

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Shigellosis is one of the leading causes of diarrhea worldwide with more than 165 million cases annually. Hence, a vaccine against this disease is a priority, but no licensed vaccine is still available. Considering target population as well as intrinsic risks of live attenuated vaccines, non-living strategies appear as the most promising candidates. Remarkably, the preservation of antigenic properties is a major concern since inactivation methods of bacteria affect these qualities. We previously reported the use of a subcellular antigen complex for vaccination against Shigellosis, based on outer membrane vesicles (OMVs) released from Shigella flexneri. Now, we describe in more detail the employment of binary ethylenimine (BEI) for inactivation of Shigella and its subsequent effect on the antigenic conservation of the vaccinal product. Results demonstrate the effectiveness of BEI treatment to completely inactivate Shigella cells without disturbing the antigenicity and immunogenicity of the OMVs. Thus, OMVs harvested after BEI inactivation were able to protect mice against an experimental infection with S. flexneri.

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“…The lack of a clear correlate of protection for Shigella vaccines has hampered vaccine development over the past several decades [8,10,11]. Even so, the importance of the serotype specific LPS antigen is widely recognized and included as a component of all vaccine approaches actively being pursued.…”

Section: Introductionmentioning

confidence: 99%

Safety and immunogenicity of an intranasal Shigella flexneri 2a Invaplex 50 vaccine

Riddle¹,

Kaminski²,

Williams³

et al. 2011

Vaccine

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Results: There were no serious adverse events and the majority of adverse events (98%) were mild. Antibody secreting cells (ASC), plasma, and mucosal immune responses to Shigella antigens were detected at all three dose levels with the 690 g dose inducing the highest magnitude and frequency of responses. Vaccination with comparable doses of Invaplex 50 via the Dolphin TM resulted in higher plasma and ASC immune responses as compared to pipette delivery. Conclusion: In this trial the S. flexneri 2a Invaplex 50 vaccine was safe, well-tolerated and induced robust levels of antigen-specific intestinal IgA and ASC responses. The spray device performed well and offered an advantage over pipette intranasal delivery.Published by Elsevier Ltd.

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Clinical trials of Shigella vaccines: two steps forward and one step back on a long, hard road

Cited by 306 publications

References 114 publications

Causes of Impaired Oral Vaccine Efficacy in Developing Countries

Causes of Impaired Oral Vaccine Efficacy in Developing Countries

Towards a non-living vaccine against Shigella flexneri: From the inactivation procedure to protection studies

Safety and immunogenicity of an intranasal Shigella flexneri 2a Invaplex 50 vaccine

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