2015 White Paper on Recent Issues in Bioanalysis: Focus on New Technologies and Biomarkers (Part 2 – Hybrid LBA/LCMS and Input from Regulatory Agencies)

Ackermann, Brad; Neubert, Hendrik; Hughes, Nicola; Garofolo, Fabio; Abberley, Lee; Alley, Stephen C.; Brown‐Augsburger, Patricia; Bustard, Mark Thomas; Chen, Linzhi; Heinrich, Joachim; Katori, Noriko; Kaur, Surinder; Kirkovsky, Leo; Laterza, Omar; Blaye, Olivier Le; Lévesque, Ann; Santos, Gustavo Mendes Lima; Olah, Timothy; Savoie, Natasha; Skelly, Michael; Spitz, Susan; Szapacs, Matthew; Tampal, Nilufer; Wang, Jian; Welink, Jan; Wieling, Jaap; Haidar, Sam; Vinter, Stephen; Whale, Emma; Witte, Bärbel

doi:10.4155/bio.15.214

Cited by 48 publications

(45 citation statements)

References 25 publications

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“…Prior to any cross-validation of LBA and LCMS techniques, it was recommended in 2014 to confirm that both technologies measure the same analyte [12]. It was not generally recommended to measure an analyte with both approaches; however, this may happen when one assay or technology runs into issues such as matrix interference, when early data are generated on one platform and then the platform is switched to the other; or when the molecular complexity necessitates additional characterization.…”

Section: Cross-validating (Lba and Lcms)mentioning

confidence: 99%

“…When cross-validating between LCMS and LBA, QC samples and incurred samples should be used, and the general acceptance criteria that should be applied are twothirds of sample results within 30% [9]. The following year, this recommendation was expanded to conclude that if cross-validation of LBA and LCMS data are required, then it is recommended to use the same capture reagent [12].…”

Section: Cross-validating (Lba and Lcms)mentioning

confidence: 99%

“…Potential binding molecules should be evaluated as part of an assay performance QC if it is judged that the assay could be impacted by the presence of these molecules. Capture with target, receptors and other reagents was proposed [12]. It was also recommended that the choices of instruments (HRMS or triple quadrupole), internal standards (SIL intact protein or SIL flanked peptide), extraction techniques and signature peptide should all be thoroughly evaluated to optimize method performance.…”

Section: Hybrid Lba/lcms Assays: Development and Validationmentioning

confidence: 99%

“…Discussing hybrid LBA/LCMS method development in 2015 concluded that existing LBA workflows can be used. Commercial LBA reagents can also be used [12]. Binding interferences can often be removed by using an acid pretreatment step.…”

Section: Hybrid Lba/lcms Assays: Development and Validationmentioning

confidence: 99%

“…These recommendations support original discussions in 2015, where it had been concluded that LCMS is best used as an orthogonal tool to assist when needed for ADA determination, for example, to overcome the lack of drug tolerance or other analytical interferences. LCMS can be used for immunoglobulin allotyping/isotyping by specific immunocapture of IgG, IgM and other immunoglobulin subclasses and/or by analysis of specific signature tryptic peptides reflecting immunoglobin subclasses [12].…”

Section: Immunogenicity (Ada) Assays: Drug Tolerancementioning

confidence: 99%

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The Decennial Index of The White Papers in Bioanalysis: ‘A Decade of Recommendations (2007–2016)’

Garofolo¹,

Savoie²

2017

Bioanalysis

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Each year, the Workshop on Recent Issues in Bioanalysis (WRIB) gathers a wide range of industry opinion leaders and regulatory authorities working on bioanalysis, biomarkers and immunogenicity to discuss the most current topics of interest, and to provide potential solutions aiming to improve quality, increase regulatory compliance and achieve scientific excellence.These yearly 'hot' topics (covering both small and large molecules), are the starting point for fruitful exchanges of knowledge, and extensive sharing of ideas among presenters, regulators and attendees, and are distilled into a series of relevant recommendations. The resultant White Papers summarizing these conclusions and consensus points from each WRIB provide the global bioanalytical community with key information and practical solutions on topics and issues addressed each year. This series of White Papers has always been among the 'most read' articles in Bioanalysis over the past 10 years [17].WRIB White Papers are designed to be 'horizontal' documents providing consensus on multiple topics rather than 'vertical' (i.e., 'consensus documents on a single topic for standardizing industry practice'). It is a cumulative effort spanning more than a year, with tremendous work behind the scenes by each co-author, starting from exhaustive preparation/design of each issue long before the WRIB, then extensive working-dinner discussions to prepare open panel discussions at the WRIB, and finally the refinement and critical review of the draft recommendations before turning it into a consensus paper.In recent years, to reflect the new structure of three sequential, core workshop days at WRIB, each White Paper has been divided into three parts to reflect the focus of each core workshop day: Part 1 on LCMS, Part 2 on hybrid ligand-binding assays (LBA)/LCMS and Regulatory Inputs and Part 3 on LBA.Although the recommendations presented in this article demonstrate that some topics have been extensively discussed repeatedly in the last decade, the evolution of bioanalysis, biomarkers and immunogenicity, and the accompanying technologies and regulations continue to bring additional challenges and solutions to existing problems. Continued assembly of industry and regulators will ensure that best practices continue in order to market safe and effective pharmaceutical products. The future publication of the 2017 White Paper in Bioanalysis signals the global bioanalytical community's intent to continue providing a consensus document for such discussions.After a decade of discussions and consensus, this article acts as a general index, organized by topic in alphabetic order, to easily consult all these recommendations and their evolution over time.

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Section: Cross-validating (Lba and Lcms)mentioning

confidence: 99%

Section: Cross-validating (Lba and Lcms)mentioning

confidence: 99%

Section: Hybrid Lba/lcms Assays: Development and Validationmentioning

confidence: 99%

Section: Hybrid Lba/lcms Assays: Development and Validationmentioning

confidence: 99%

Section: Immunogenicity (Ada) Assays: Drug Tolerancementioning

confidence: 99%

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