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Generation of mAb Variants with Less Attractive Self-Interaction but Preserved Target Binding by Well-Directed Mutation
被引:4
作者:

Domnowski, Martin
论文数: 0 引用数: 0
h-index: 0
机构:
Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany
MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Lo Presti, Ken
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h-index: 0
机构:
Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Binder, Jonas
论文数: 0 引用数: 0
h-index: 0
机构:
Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Reindl, Josef
论文数: 0 引用数: 0
h-index: 0
机构:
MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Lehmann, Lucille
论文数: 0 引用数: 0
h-index: 0
机构:
MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Kummer, Felix
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h-index: 0
机构:
MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Wolber, Meike
论文数: 0 引用数: 0
h-index: 0
机构:
MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Satzger, Marion
论文数: 0 引用数: 0
h-index: 0
机构:
MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Dehling, Marco
论文数: 0 引用数: 0
h-index: 0
机构:
MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Jaehrling, Jan
论文数: 0 引用数: 0
h-index: 0
机构:
MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany

Friess, Wolfgang
论文数: 0 引用数: 0
h-index: 0
机构:
Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany
机构:
[1] Ludwig Maximilians Univ Munchen, Dept Pharm Pharmaceut Technol & Biopharmaceut, D-81377 Munich, Germany
[2] MorphoSys AG, Dept Prot Sci Res, D-82152 Planegg, Germany
关键词:
self-interaction;
self-association;
protein engineering;
HDX-MS;
viscosity;
unspecificity;
CONCENTRATED MONOCLONAL-ANTIBODY;
CLUSTER FORMATION;
PROTEIN-PROTEIN;
ASSOCIATION;
VISCOSITY;
IGG1;
AFFINITY;
SPECIFICITY;
MECHANISMS;
MITIGATION;
D O I:
10.1021/acs.molpharmaceut.0c00848
中图分类号:
R-3 [医学研究方法];
R3 [基础医学];
学科分类号:
1001 ;
摘要:
Strongly attractive self-interaction of therapeutic protein candidates can impose challenges for manufacturing, filling, stability, and administration due to elevated viscosity or aggregation propensity. Suitable formulations can mitigate these issues to a certain extent. Understanding the self-interaction mechanism on a molecular basis and rational protein engineering provides a more fundamental approach, and it can save costs and efforts as well as alleviate risks at later stages of development. In this study, we used computational methods for the identification of aggregation-prone regions in a mAb and generated mutants based on these findings. We applied hydrogen-deuterium exchange mass spectrometry to identify distinct self-interaction hot spots. Ultimately, we generated mAb variants based on a combination of both approaches and identified mutants with low attractive self-interaction propensity, minimal off-target binding, and even improved target binding. Our data show that the introduction of arginine in spatial proximity to hydrophobic patches is highly beneficial on all these levels. For our mAb, variants that contain more than one aspartate residue flanking to the hydrophobic HCDR3 show decreased attractive self-interaction at unaffected off-target and target binding. The combined engineering strategy described here underlines the high potential of understanding self-interaction in the early stages of development to predict and reduce the risk of failure in subsequent development.
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页码:236 / 245
页数:10
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