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Inter-Laboratory Robustness of Next-Generation Bile Acid Study in Mice and Humans: International Ring Trial Involving 12 Laboratories.

Publication ,  Journal Article
Pham, HT; Arnhard, K; Asad, YJ; Deng, L; Felder, TK; St John-Williams, L; Kaever, V; Leadley, M; Mitro, N; Muccio, S; Prehn, C; Rauh, M ...
Published in: J Appl Lab Med
September 1, 2016

BACKGROUND: The increasing relevance of individual bile acids quantification in biological samples requires analytical standardization to guarantee robustness and reliability of laboratory results. We have organized the first international ring trial, carried out in 12 laboratories, to evaluate the newly developed LC-MS/MS-based test kit for bile acid analysis. METHODS: Each laboratory received a Biocrates® Bile Acids Kit including system suitability test (SST) protocol. The kit is designed to analyze 16 individual human and 19 mouse bile acids. A set of 9 human and mouse plasma samples was measured in replicates. Laboratories were first required to pass the acceptance criteria for the SST. Within the subset of laboratories passing SST criteria, we evaluated how many laboratories met the target criteria of 80% of reported values with a relative accuracy within the 70%-130% range and analytical precisions (%CV) below 30%. RESULTS: A total of 12 of 16 participating laboratories passed the SST as the prerequisite to enter the ring trial. All 12 laboratories were then able to successfully run the kit and ring trial samples. Of the overall reported values, 94% were within 70%-130% relative accuracy range. Mean precision was 8.3% CV. The condition of CV <30% was fulfilled by 99% of the reported values. CONCLUSIONS: The first publically available interlaboratory ring trial for standardized bile acids quantification in human and mouse plasma samples showed very good analytical performance, within acceptance criteria typically applied in the preclinical environment. The kit is therefore suitable for standardized quantitative bile acid analysis and the establishment of reference values.

Duke Scholars

Published In

J Appl Lab Med

DOI

ISSN

2576-9456

Publication Date

September 1, 2016

Volume

1

Issue

2

Start / End Page

129 / 142

Location

England

Related Subject Headings

  • 3205 Medical biochemistry and metabolomics
  • 3202 Clinical sciences
 

Citation

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MLA
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Pham, H. T., Arnhard, K., Asad, Y. J., Deng, L., Felder, T. K., St John-Williams, L., … Koal, T. (2016). Inter-Laboratory Robustness of Next-Generation Bile Acid Study in Mice and Humans: International Ring Trial Involving 12 Laboratories. J Appl Lab Med, 1(2), 129–142. https://doi.org/10.1373/jalm.2016.020537
Pham, Hai T., Kathrin Arnhard, Yasmin J. Asad, Lu Deng, Thomas K. Felder, Lisa St John-Williams, Volkhard Kaever, et al. “Inter-Laboratory Robustness of Next-Generation Bile Acid Study in Mice and Humans: International Ring Trial Involving 12 Laboratories.J Appl Lab Med 1, no. 2 (September 1, 2016): 129–42. https://doi.org/10.1373/jalm.2016.020537.
Pham HT, Arnhard K, Asad YJ, Deng L, Felder TK, St John-Williams L, et al. Inter-Laboratory Robustness of Next-Generation Bile Acid Study in Mice and Humans: International Ring Trial Involving 12 Laboratories. J Appl Lab Med. 2016 Sep 1;1(2):129–42.
Pham, Hai T., et al. “Inter-Laboratory Robustness of Next-Generation Bile Acid Study in Mice and Humans: International Ring Trial Involving 12 Laboratories.J Appl Lab Med, vol. 1, no. 2, Sept. 2016, pp. 129–42. Pubmed, doi:10.1373/jalm.2016.020537.
Pham HT, Arnhard K, Asad YJ, Deng L, Felder TK, St John-Williams L, Kaever V, Leadley M, Mitro N, Muccio S, Prehn C, Rauh M, Rolle-Kampczyk U, Thompson JW, Uhl O, Ulaszewska M, Vogeser M, Wishart DS, Koal T. Inter-Laboratory Robustness of Next-Generation Bile Acid Study in Mice and Humans: International Ring Trial Involving 12 Laboratories. J Appl Lab Med. 2016 Sep 1;1(2):129–142.

Published In

J Appl Lab Med

DOI

ISSN

2576-9456

Publication Date

September 1, 2016

Volume

1

Issue

2

Start / End Page

129 / 142

Location

England

Related Subject Headings

  • 3205 Medical biochemistry and metabolomics
  • 3202 Clinical sciences