| Literature DB >> 24553455 |
Stefan F C Vaessen1, Martijn W P Bruysters2, Rob J Vandebriel2, Saertje Verkoeijen1, Rogier Bos3, Cyrille A M Krul1, Arnoud M Akkermans2.
Abstract
Pertussis vaccines are routinely administered to infants to protect them from whooping cough. Still, an adequate safety test for pertussis toxin (PT), one of the main antigens in these vaccines, is not available. The histamine sensitization test is currently the only assay accepted by regulatory authorities to test for the absence of active PT in vaccines. This is however, a lethal animal test with poor reproducibility. In addition, it is not clear whether the assumed underlying mechanism, i.e., ADP-ribosylation of G proteins, is the only effect that should be considered in safety evaluation of PT. The in vitro safety test for PT that we developed is based on the clinical effects of PT in humans. For this, human cell lines were chosen based on the cell types involved in the clinical effects of PT. These cell lines were exposed to PT and analyzed by microarray. In this review, we discuss the clinical effects of PT and the mechanisms that underlie them. The approach taken may provide as an example for other situations in which an in vitro assay based on clinical effects in humans is required.Entities:
Keywords: in vitro; microarray; pertussis toxin; safety; vaccine
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Year: 2014 PMID: 24553455 PMCID: PMC4896582 DOI: 10.4161/hv.28001
Source DB: PubMed Journal: Hum Vaccin Immunother ISSN: 2164-5515 Impact factor: 3.452