Biopharmaceutical Manufacturing, Volume 1 Regulatory processes Biopharmaceutical Manufacturing, Volume 1 Regulatory processes Sarfaraz Niazi University of Illinois, Chicago, IL, USA Sunitha Lokesh Pharmaceutical Scientist LLC, Deerfield, IL, USA IOP Publishing, Bristol, UK ªIOPPublishingLtd2021 Allrightsreserved.Nopartofthispublicationmaybereproduced,storedinaretrievalsystem ortransmittedinanyformorbyanymeans,electronic,mechanical,photocopying,recording orotherwise,withoutthepriorpermissionofthepublisher,orasexpresslypermittedbylawor undertermsagreedwiththeappropriaterightsorganization.Multiplecopyingispermittedin accordancewiththetermsoflicencesissuedbytheCopyrightLicensingAgency,theCopyright ClearanceCentreandotherreproductionrightsorganizations. 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ISBN 978-0-7503-3175-3(ebook) ISBN 978-0-7503-3173-9(print) ISBN 978-0-7503-3176-0(myPrint) ISBN 978-0-7503-3174-6(mobi) DOI 10.1088/978-0-7503-3175-3 Version:20211201 IOPebooks BritishLibraryCataloguing-in-PublicationData:Acataloguerecordforthisbookisavailable fromtheBritishLibrary. PublishedbyIOPPublishing,whollyownedbyTheInstituteofPhysics,London IOPPublishing,TempleCircus,TempleWay,Bristol,BS16HG,UK USOffice:IOPPublishing,Inc.,190NorthIndependenceMallWest,Suite601,Philadelphia, PA19106,USA ToDrSarahYim,whosehumility,scientificwisdom,andvisionhelpmanymindsgrow at the FDA and in the biosimilars community. —Sarfaraz K Niazi Iamthankfultomyfatherforencouragingmetobeacuriousscientistandmyhusband for supporting me to practice my passion. —Sunitha Lokesh Contents Preface xvii Acknowledgments xxxi Author biographies xxxii 1 Introduction to biopharmaceuticals 1-1 1.1 Overview 1-1 1.1.1 Biosimilars 1-4 1.1.2 Intellectual property 1-4 1.1.3 Regulations 1-5 1.2 Biopharmaceutical molecules 1-7 1.2.1 Overview 1-7 1.2.2 Molecular mechanism 1-8 1.2.3 Therapeutic classification 1-9 1.2.4 Hormone peptide drugs 1-9 1.2.5 Human hematopoietic factor 1-10 1.2.6 Human cytokines 1-10 1.2.7 Human plasma protein factor 1-11 1.2.8 Human bone formation protein 1-11 1.2.9 Recombinant enzymes 1-11 1.2.10 Antibodies 1-11 1.3 Protein structure and properties 1-14 1.3.1 Primary structure 1-14 1.3.2 Secondary structure 1-18 1.3.3 Tertiary structure 1-22 1.3.4 Quaternary structure 1-23 1.3.5 Post-translational modification (PTM) 1-23 1.3.6 Association and aggregation 1-29 1.4 Pharmacokinetic manipulations 1-29 1.4.1 Protein modification to increase the duration of action 1-30 1.5 Immunogenicity 1-31 1.5.1 The immune system 1-31 1.5.2 Antibodies 1-33 1.5.3 Antigens 1-33 1.5.4 Biopharmaceutical immunogenicity 1-34 1.5.5 Immunogenicity testing 1-36 vii BiopharmaceuticalManufacturing,Volume1 1.6 Recombinant expression 1-36 1.6.1 Understanding DNA and RNA 1-37 1.7 Gene and cell therapy 1-40 1.7.1 Gene editing 1-40 1.8 Conclusion 1-42 2 Antibody biopharmaceuticals 2-1 2.1 Overview 2-1 2.1.1 Naming 2-2 2.1.2 Commercial antibodies 2-3 2.2 The immune system 2-3 2.2.1 Innate immune system 2-11 2.2.2 Adaptive immune system 2-11 2.3 Monoclonal antibodies 2-11 2.3.1 Mode of action 2-13 2.4 Types of antibodies 2-16 2.4.1 Bispecific (BsAbs) 2-17 2.4.2 Fab fragments and single-chain antibodies 2-18 2.4.3 Humanized and chimeric mAbs 2-19 2.4.4 Affinity maturation 2-21 2.4.5 Antigenized antibodies 2-21 2.4.6 IgG1 fusion proteins 2-22 2.4.7 Drug or toxin conjugation 2-22 2.5 Development of antibodies 2-23 2.5.1 Endogenous method: single B-cell 2-23 2.5.2 Exogenous methods 2-23 2.5.3 Mouse hybridoma 2-24 2.5.4 Transgenic mice 2-27 2.5.5 Surface display libraries 2-28 2.5.6 Recombinant expression 2-34 2.6 Conclusion 2-35 2.7 Databases relevant to antibodies 2-35 3 Gene and cell therapy 3-1 3.1 Overview 3-1 3.2 Gene therapy 3-2 3.2.1 Methodologies 3-2 viii BiopharmaceuticalManufacturing,Volume1 3.2.2 Risks of gene therapy 3-5 3.2.3 Gene-editing technologies 3-6 3.2.4 Vector manufacturing 3-7 3.2.5 DNA vaccines 3-14 3.2.6 mRNA vaccines 3-18 3.3 Cell therapy 3-21 3.3.1 Types of cell therapies 3-22 3.3.2 CAR-T treatment (cellular immunotherapy) 3-23 3.3.3 Allogenic cell therapy 3-24 3.4 Regulatory considerations 3-26 3.4.1 Development and characterization of cell populations for 3-27 administration 3.4.2 Characterization and release testing of cellular gene therapy 3-30 products 3.4.3 Additional possible applications: radioisotopes or toxins 3-31 added to cell preparations 3.4.4 Vector production, characterization, and release testing 3-32 for gene therapy 3.4.5 Construction and characterization of vectors 3-32 3.4.6 Vector manufacturing system 3-32 3.4.7 Viral master banks 3-33 3.4.8 Lot-to-lot distribution vector testing and specifications 3-33 3.4.9 Issues in gene therapy related to specific vector classes 3-34 3.5 Conclusion 3-35 4 Formulation of biopharmaceuticals 4-1 4.1 Overview 4-1 4.2 Structural instability 4-2 4.2.1 Basis 4-2 4.2.2 Physical degradation 4-4 4.2.3 Chemical degradation 4-8 4.3 Formulation composition 4-19 4.3.1 Route of administration 4-19 4.3.2 Excipients and properties 4-21 4.3.3 Liquid formulations 4-25 4.3.4 Lyophilized formulations 4-26 4.4 Delivery routes 4-28 4.4.1 Intravenous 4-28 ix