Bottom-up sample preparation for the LC-MS/MS quantification of anti-cancer monoclonal antibodies in bio matrices

Karen A.M. De Jong; Suse J. Van Breugel; Michel J.X. Hillebrand; Hilde Rosing; Alwin D.R. Huitema; Jos H. Beijnen

doi:10.4155/bio-2020-0204

Bottom-up sample preparation for the LC-MS/MS quantification of anti-cancer monoclonal antibodies in bio matrices

Karen A.M. De Jong^*
, Suse J. Van Breugel
, Michel J.X. Hillebrand
, Hilde Rosing
, Alwin D.R. Huitema
, Jos H. Beijnen

^*Corresponding author for this work

Research output: Contribution to journal › Review article › peer-review

Abstract

Therapeutic monoclonal antibodies (mAbs) are rapidly taking over the treatment of many malignancies, and an astonishing number of mAbs is in development. This causes a high demand for quantification of mAbs in biomatrices both for measuring therapeutic mAb concentrations and to support pharmacokinetics and pharmacodynamics studies. Conventionally, ligand-binding assays are used for these purposes, but LC-MS is gaining popularity. Although intact (top-down) and subunit (middle-down) mAb quantification is reported, signature peptide (bottom-up) quantification is currently most advantageous. This review provides an overview of the reported bottom-up mAb quantification methods in biomatrices as well as general recommendations regarding signature peptide and internal standard selection, reagent use and optimization of digestion in bottom-up quantification methods.

Original language	English
Pages (from-to)	1405-1425
Number of pages	21
Journal	Bioanalysis
Volume	12
Issue number	19
DOIs	https://doi.org/10.4155/bio-2020-0204
Publication status	Published - Oct 2020

Keywords

bottom-up
mass spectrometry
monoclonal antibodies
oncology
sample preparation
signature peptide

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10.4155/bio-2020-0204

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title = "Bottom-up sample preparation for the LC-MS/MS quantification of anti-cancer monoclonal antibodies in bio matrices",

abstract = "Therapeutic monoclonal antibodies (mAbs) are rapidly taking over the treatment of many malignancies, and an astonishing number of mAbs is in development. This causes a high demand for quantification of mAbs in biomatrices both for measuring therapeutic mAb concentrations and to support pharmacokinetics and pharmacodynamics studies. Conventionally, ligand-binding assays are used for these purposes, but LC-MS is gaining popularity. Although intact (top-down) and subunit (middle-down) mAb quantification is reported, signature peptide (bottom-up) quantification is currently most advantageous. This review provides an overview of the reported bottom-up mAb quantification methods in biomatrices as well as general recommendations regarding signature peptide and internal standard selection, reagent use and optimization of digestion in bottom-up quantification methods. ",

keywords = "bottom-up, mass spectrometry, monoclonal antibodies, oncology, sample preparation, signature peptide",

author = "\{De Jong\}, \{Karen A.M.\} and \{Van Breugel\}, \{Suse J.\} and Hillebrand, \{Michel J.X.\} and Hilde Rosing and Huitema, \{Alwin D.R.\} and Beijnen, \{Jos H.\}",

year = "2020",

month = oct,

doi = "10.4155/bio-2020-0204",

language = "English",

volume = "12",

pages = "1405--1425",

journal = "Bioanalysis",

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TY - JOUR

T1 - Bottom-up sample preparation for the LC-MS/MS quantification of anti-cancer monoclonal antibodies in bio matrices

AU - De Jong, Karen A.M.

AU - Van Breugel, Suse J.

AU - Hillebrand, Michel J.X.

AU - Rosing, Hilde

AU - Huitema, Alwin D.R.

AU - Beijnen, Jos H.

PY - 2020/10

Y1 - 2020/10

N2 - Therapeutic monoclonal antibodies (mAbs) are rapidly taking over the treatment of many malignancies, and an astonishing number of mAbs is in development. This causes a high demand for quantification of mAbs in biomatrices both for measuring therapeutic mAb concentrations and to support pharmacokinetics and pharmacodynamics studies. Conventionally, ligand-binding assays are used for these purposes, but LC-MS is gaining popularity. Although intact (top-down) and subunit (middle-down) mAb quantification is reported, signature peptide (bottom-up) quantification is currently most advantageous. This review provides an overview of the reported bottom-up mAb quantification methods in biomatrices as well as general recommendations regarding signature peptide and internal standard selection, reagent use and optimization of digestion in bottom-up quantification methods.

AB - Therapeutic monoclonal antibodies (mAbs) are rapidly taking over the treatment of many malignancies, and an astonishing number of mAbs is in development. This causes a high demand for quantification of mAbs in biomatrices both for measuring therapeutic mAb concentrations and to support pharmacokinetics and pharmacodynamics studies. Conventionally, ligand-binding assays are used for these purposes, but LC-MS is gaining popularity. Although intact (top-down) and subunit (middle-down) mAb quantification is reported, signature peptide (bottom-up) quantification is currently most advantageous. This review provides an overview of the reported bottom-up mAb quantification methods in biomatrices as well as general recommendations regarding signature peptide and internal standard selection, reagent use and optimization of digestion in bottom-up quantification methods.

KW - bottom-up

KW - mass spectrometry

KW - monoclonal antibodies

KW - oncology

KW - sample preparation

KW - signature peptide

UR - https://www.scopus.com/pages/publications/85092801582

U2 - 10.4155/bio-2020-0204

DO - 10.4155/bio-2020-0204

M3 - Review article

C2 - 32975434

AN - SCOPUS:85092801582

SN - 1757-6180

VL - 12

SP - 1405

EP - 1425

JO - Bioanalysis

JF - Bioanalysis

IS - 19

ER -

Bottom-up sample preparation for the LC-MS/MS quantification of anti-cancer monoclonal antibodies in bio matrices

Abstract

Keywords

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