Literature DB >> 28797318

Single-Laboratory Validation of the Neogen Qualitative Lateral Flow Immunoassay for the Detection of Paralytic Shellfish Toxins in Mussels and Oysters.

Alison R Turnbull1, Jessica Y C Tan1, Sarah C Ugalde2, Gustaaf M Hallegraeff2, Katrina Campbell3, D Tim Harwood4, Juan José Dorantes-Aranda5.   

Abstract

Detection of paralytic shellfish toxins (PSTs) in bivalve shellfish by analytical methods is complicated and costly, requiring specific expertise and equipment. Following extensive blooms of Alexandrium tamarense Group 1 in Tasmania, Australia, an investigation was made into commercially available screening test kits suitable for use with the toxin profiles found in affected bivalves. The qualitative Neogen rapid test kit, with a modified protocol to convert gonyautoxins GTX1&4 and GTX2&3 into neosaxitoxin and saxitoxin (STX), respectively, with higher cross-reactivities, was the best fit-for-purpose. This validation study of the test kit and the modified protocol was undertaken following AOAC INTERNATIONAL guidelines for the validation of qualitative binary chemistry methods. The validation used four different PST profiles representing natural profiles found in Australia and in Europe: two in a mussel matrix and two in an oyster matrix. The test kit was shown to have appropriate selectivity of the toxin analogs commonly found in bivalve shellfish. The matrix and probability of detection (POD) study showed that the rapid test kit used with the modified protocol was able to consistently detect PST at the bivalve regulatory level of 0.8 mg STX⋅2HCl eq/kg, with a POD estimated via the binomial logistic regression of 1.0 at 0.8 mg STX⋅2HCl eq/kg in all tested profiles in both matrixes. The POD at 0.4 mg STX⋅2HCl eq/kg was 0.75 and 0.46 for the two toxin profiles in an oyster matrix and 0.96 and 1.0 for the two toxin profiles in a mussel matrix. No significant differences in the PODs of the PSTs at the regulatory level were found between production lots of the test kits. The results suggest the method is suitable to undergo a collaborative validation study.

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Year:  2017        PMID: 28797318     DOI: 10.5740/jaoacint.17-0135

Source DB:  PubMed          Journal:  J AOAC Int        ISSN: 1060-3271            Impact factor:   1.913


  4 in total

1.  Improved Accuracy of Saxitoxin Measurement Using an Optimized Enzyme-Linked Immunosorbent Assay.

Authors:  Jennifer R McCall; W Christopher Holland; Devon M Keeler; D Ransom Hardison; R Wayne Litaker
Journal:  Toxins (Basel)       Date:  2019-10-31       Impact factor: 4.546

2.  Lobster Supply Chains Are Not at Risk from Paralytic Shellfish Toxin Accumulation during Wet Storage.

Authors:  Alison Turnbull; Andreas Seger; Jessica Jolley; Gustaaf Hallegraeff; Graeme Knowles; Quinn Fitzgibbon
Journal:  Toxins (Basel)       Date:  2021-02-09       Impact factor: 4.546

Review 3.  Current Trends and Challenges for Rapid SMART Diagnostics at Point-of-Site Testing for Marine Toxins.

Authors:  Michael Dillon; Maja A Zaczek-Moczydlowska; Christine Edwards; Andrew D Turner; Peter I Miller; Heather Moore; April McKinney; Linda Lawton; Katrina Campbell
Journal:  Sensors (Basel)       Date:  2021-04-03       Impact factor: 3.576

4.  A Comparative Analysis of Methods (LC-MS/MS, LC-MS and Rapid Test Kits) for the Determination of Diarrhetic Shellfish Toxins in Oysters, Mussels and Pipis.

Authors:  Penelope A Ajani; Chowdhury Sarowar; Alison Turnbull; Hazel Farrell; Anthony Zammit; Stuart Helleren; Gustaaf Hallegraeff; Shauna A Murray
Journal:  Toxins (Basel)       Date:  2021-08-11       Impact factor: 4.546

  4 in total

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