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The antibody drug conjugates market is projected to grow at an annualized rate of over 20%, till 2030
The antibody drug conjugates market is projected to grow at an annualized rate of over 20%, till 2030
The antibody drug conjugates market is projected to grow at an annualized rate of over 20%, till 2030

The antibody drug conjugates market is projected to grow at an annualized rate of over 20%, till 2030

Key Market Insights

§  Eminentrepresentatives from different biopharmaceutical companies confirm thesustained interest in ADC therapeutics, highlighting the technologicalinnovation that is driving contemporary R&D initiatives

§  Presently, over 240 ADC therapy candidates are being evaluated inclinical / preclinical stages for treating a variety of solid tumors /hematologic cancers

§  The pipeline featuresproduct candidates that target a wide range of biological antigens and areequipped with different cytotoxic warheads; a number of companies are focused on developing novel drug conjugates

§  In order to gain acompetitive edge in the market, ADC developers are actively exploring newbiological targets, conducting clinical trials across different geographies totreat diverse disease indications

§  A number of eminent scientists from renowned universities, owing totheir involvement in clinical development efforts, have emerged as key opinionleaders within this market

§  Over the years, more than 16,000 patents related to ADCs have been filed/ granted across the world, indicative of the ongoing pace of R&D activityin this field of research

§  Several investors, having realized the opportunity within this upcomingsegment of targeted cancer therapeutics industry, have invested over USD 5billion, in the period between 2011 and 2019

§  The increasing interest in this field is also reflected in the partnershipactivity; deals inked in the recent past were mostly focused on licensing ofproducts / technologies, involving both international and indigenousstakeholders

§  In the recent years,several developer companies have initiated clinical trials to evaluate thetherapeutic potential of ADCs in combination with other drug / therapy classes

§  Anticipating the launch of several product candidates, stakeholders areexploring diverse commercialization strategies across different stages of thelaunch cycle along with the appropriate reimbursement strategies

§  Given thecomplexities associated with the development and production of ADCs, CMOs areindispensable to the R&D and manufacturing activity in this domain; someCMOs have even pioneered the novel ADC technology platforms

§  Case Study: In order to keep patients andhealthcare professionals informed and aware of the developments, companies aredeploying diverse promotional strategies for their respective products

§  With a promising development pipeline and encouraging clinical results,the global market is anticipated to witness growth at an annualized rate ofover 20% during the next decade

§  The anticipatedfuture opportunity is likely to be distributed across different types of linkers and target antigens as more late-stage drugs get commercialized andexisting marketing authorizations are expanded

 

For more information, please visit https://www.rootsanalysis.com/reports/view_document/antibody-drug-conjugates-market-5th-edition-2019-2030/270.html

 

Table of Contents

 

1. PREFACE

1.1. Scope of the Report

1.2. Research Methodology

1.3. Chapter Outlines

 

2. EXECUTIVE SUMMARY

 

3. INTRODUCTION

3.1. Chapter Overview

3.2. Evolution of Anticancer Therapy

3.3. Cancer Treatment Methods

3.3.1. Surgery

3.3.2. Radiation Therapy

3.3.3. Chemotherapy

3.3.4. Targeted Therapies

 

3.4. Monoclonal Antibody-BasedAnticancer Therapies

3.5. Components of Antibody DrugConjugates (ADCs)

3.5.1. Antibody

3.5.2. Cytotoxin

3.5.3. Linker

 

3.6. Advantages of ADC Therapeutics overTraditional Therapeutic Interventions

3.7. Differences Between Small MoleculeDrugs, Monoclonal Antibody Therapies and ADCs

3.8. Pharmacokinetic Properties of ADCs

3.8.1. Absorption

3.8.2. Distribution

3.8.3. Metabolism and Excretion

 

4. MARKET OVERVIEW

4.1. Chapter Overview

4.2. ADC Therapeutics: Clinical Pipeline

4.2.1. Analysis by Phase of Development

4.2.2. Analysis by Indication

4.2.3. Analysis by Line of Treatment

4.2.4. Analysis by Dosing Regimen

4.2.5. Analysis by Type of Therapy

4.2.6. Analysis by Target Antigen

4.2.7. Analysis by Antibody Origin

4.2.8. Analysis by Antibody Isotype

4.2.9. Analysis by Type of Linker

4.2.10. Analysis by Type of Payload /Warhead

4.2.11. Key Technology Providers

4.2.12. Discontinued Drugs

 

4.3. ADC Therapeutics: PreclinicalPipeline

4.3.1. Analysis by Phase of Development

4.3.2. Analysis by Indication

4.3.3. Analysis by Target Antigen

4.3.4. Key Players: Analysis by Numberof ADC Therapeutics

 

4.4. ADC Therapeutics: DeveloperLandscape

4.4.1. Analysis by Year of Establishment

4.4.2. Analysis by Company Size

4.4.3. Analysis by Geographical Location

4.4.4. Logo Landscape: Analysis by Sizeand Target Indication

4.5. Novel Drug Conjugates

 

5. COMPANY AND DRUG PROFILES

5.1. Chapter Overview

5.2. AbbVie

5.2.1. Company Overview

5.2.2. Financial Information

5.2.3. Pipeline Overview

5.2.3.1. Rovalpituzumab Tesirine /ROVA-T

5.2.3.1.1 Drug Overview

5.2.3.1.2. Mechanism of Action

5.2.3.1.3. Clinical Development Status

5.2.3.1.4. Key Clinical Trial Results

 

5.2.3.2. Teliso-V / TelisotuzumabVedotin / ABBV-399

5.2.3.2.1 Drug Overview

5.2.3.2.2. Mechanism of Action

5.2.3.2.3. Clinical Development Status

5.2.3.2.4. Key Clinical Trial Results

5.2.4. Recent Developments and FutureOutlook

 

5.3. Astellas Pharma

5.3.1. Company Overview

5.3.2. Financial Information

5.3.3. Pipeline Overview

5.3.3.1. Enfortumab Vedotin

5.3.3.1.1. Drug Overview

5.3.3.1.2. Mechanism of Action

5.3.3.1.3. Clinical Development Status

5.3.3.1.4. Key Clinical Trial Results

 

5.3.3.2. ASG16-M8F

5.3.3.2.1. Drug Overview

5.3.3.2.2. Mechanism of Action

5.3.3.2.3. Clinical Development Status

5.3.3.2.4. Key Clinical Trial Results

5.3.4. Recent Developments and FutureOutlook

5.4. AstraZeneca

54.1. Company Overview

5.4.2. Financial Information

5.4.3. Pipeline Overview

5.4.3.1. LUMOXITI™

5.4.3.1.1. Drug Overview

5.4.3.1.2. Mechanism of Action

5.4.3.1.3. Clinical Development Status

5.4.3.1.4. Key Clinical Trial Results

5.4.4. Recent Developments and FutureOutlook

 

5.5. Daiichi Sankyo

5.5.1. Company Overview

5.5.2. Financial Information

5.5.3. Pipeline Overview

5.5.3.1. Trastuzumab deruxtecan /DS-8201a / DS 8201

5.5.3.1.1. Drug Overview

5.5.3.1.2. Mechanism of Action

5.5.3.1.3. Clinical Development Status

5.5.3.1.4. Key Clinical Trial Results

5.5.4. Recent Developments and FutureOutlook

 

5.6. ImmunoGen

5.6.1. Company Overview

5.6.2. Financial Information

5.6.3. Pipeline Overview

5.6.3.1. IMGN853 / Mirvetuximabsoravtansine

5.6.3.1.1. Drug Overview

5.6.3.1.2. Mechanism of Action

5.6.3.1.3. Clinical Development Status

5.6.3.1.4. Key Clinical Trial Results

5.6.4. Recent Developments and FutureOutlook

5.7. Immunomedics

5.7.1. Company Overview

5.7.2. Financial Information

5.7.3. Pipeline Overview

5.7.3.1. IMMU-130

5.7.3.1.1. Drug Overview

5.7.3.1.2. Mechanism of Action

5.7.3.1.3. Clinical Development Status

5.7.3.1.4. Key Clinical Trial Results

5.7.4. Recent Developments and FutureOutlook

 

5.8. Pfizer

5.8.1. Company Overview

5.8.2. Financial Information

5.8.3. Pipeline Overview

5.8.3.1. CMC-544 / BESPONSA® /Inotuzumab Ozogamicin

5.8.3.1.1. Drug Overview

5.8.3.1.2. Mechanism of Action

5.8.3.1.3. Clinical Development Status

5.8.3.1.4. Key Clinical Trial Results

 

5.8.3.2. MYLOTARG™ / GemtuzumabOzogamicin

5.8.3.2.1. Drug Overview

5.8.3.2.2. Mechanism of Action

5.8.3.2.3. Clinical Development Status

5.8.3.2.4. Key Clinical Trial Results

5.8.4. Recent Developments and FutureOutlook

 

5.9. Roche / Genentech

5.9.1. Company Overview

5.9.2. Financial Information

5.9.3. Pipeline Overview

5.9.3.1. KADCYLA®

5.9.3.1.1. Drug Overview

5.9.3.1.2. Mechanism of Action

5.9.3.1.3. Clinical Development Status

5.9.3.1.4. Key Clinical Trial Results

 

5.9.3.2. RG-7596

5.9.3.2.1. Drug Overview

5.9.3.2.2. Mechanism of Action

5.9.3.2.3. Clinical Development Status

5.9.3.2.4. Key Clinical Trial Results

5.9.4. Recent Developments and FutureOutlook

 

5.10. Seattle Genetics

5.10.1. Company Overview

5.10.2. Financial Information

5.10.3. Pipeline Overview

5.10.3.1. ADCETRIS®

5.10.3.1.1. Drug Overview

5.10.3.1.2. Mechanism of Action

5.10.3.1.3. Clinical Development Status

5.10.3.1.4. Key Clinical Trial Results

 

5.10.3.2. SGN- LIV1A

5.10.3.2.1. Drug Overview

5.10.3.2.2. Mechanism of Action

5.10.3.2.3. Clinical Development Status

5.10.3.2.4. Key Clinical Trial Results

5.10.4. Recent Developments and FutureOutlook

 

5.11. Synthon

5.11.1. Company Overview

5.11.2. Financial Information

5.11.3. Pipeline Overview

5.11.3.1. SYD985 / TrastuzumabDuocarmazine

5.11.3.1.1. Drug Overview

5.11.3.1.2. Mechanism of Action

5.11.3.1.3. Clinical Development Status

5.11.3.1.4. Key Clinical Trial Results

5.11.4. Recent Developments and FutureOutlook

 

5.12. Other Companies

5.12.1. Bayer HealthCare

5.12.1.1. Company Overview

5.12.1.2. Financial Information

5.12.1.3. Pipeline Overview

5.12.1.4. Recent Developments and FutureOutlook

 

5.12.2. Biotest Pharmaceuticals

5.12.2.1. Company Overview

5.12.2.2. Financial Information

5.12.2.3. Pipeline Overview

5.12.2.4. Recent Developments and FutureOutlook

 

6. KEY THERAPEUTIC AREAS

6.1. Chapter Overview

6.2. Hematological Malignancies

6.2.1. Leukemias and Lymphomas

6.2.1.1. Leukemia: Introduction andEpidemiology

6.2.1.1.1. Acute Myeloid Leukemia

6.2.1.1.2. Chronic Myeloid Leukemia

6.2.1.1.3. Acute Lymphocytic Leukemia

6.2.1.1.4. Chronic Lymphocytic Leukemia

6.2.1.2. Lymphoma: Introduction andEpidemiology

6.2.1.3. Current Treatment Landscape

6.2.1.4. ADC Therapeutics for Leukemia /Lymphoma

 

6.2.2. Multiple Myeloma

6.2.2.1. Introduction and Epidemiology

6.2.2.2. Current Treatment Landscape

6.2.2.3. ADC Therapeutics for MultipleMyeloma

 

6.3. Solid Tumors

6.3.1. Lung Cancer

6.3.1.1. Introduction and Epidemiology

6.3.1.2. Current Treatment Landscape

6.3.1.3. ADC Therapeutics for LungCancer

 

6.3.2. Breast Cancer

6.3.2.1. Introduction and Epidemiology

6.3.2.2. Current Treatment Landscape

6.3.2.3. ADC Therapeutics for BreastCancer

 

6.3.3. Ovarian Cancer

6.3.3.1. Introduction and Epidemiology

6.3.3.2. Current Treatment Landscape

6.3.3.3. ADC Therapeutics for OvarianCancer

 

6.3.4. Bladder Cancer

6.3.4.1. Introduction and Epidemiology

6.3.4.2. Current Treatment Landscape

6.3.4.3. ADC Therapeutics for BladderCancer

 

6.3.5. Colorectal Cancer

6.3.5.1. Introduction and Epidemiology

6.3.5.2. Current Treatment Landscape

6.3.5.3. ADC Therapeutics for ColorectalCancer

 

6.3.6. Prostate Cancer

6.3.6.1. Introduction and Epidemiology

6.3.6.2. Current Treatment Landscape

6.3.6.3. ADC Therapeutics for ProstateCancer

 

6.3.7. Gastric Cancer

6.3.7.1. Introduction and Epidemiology

6.3.7.2. Current Treatment Landscape

6.3.7.3. ADC Therapeutics for ProstateCancer

 

7. KEY OPINION LEADERS

7.1. Chapter Overview

7.2. Methodology

 

7.3. Principal Investigators /Sub-Investigators / Study Directors Involved in Clinical Trials

7.3.1. Geographical Distribution of KeyOpinion Leaders

7.3.1.1. Experts on ADCETRIS®

7.3.1.2. Experts on KADCYLA®

7.3.1.3. Experts on MYLOTARG™

7.3.1.4. Experts on Other ADCs

 

7.4. Prominent Key Opinion Leaders(KOLs)

7.5. KOL Benchmarking: Roots Analysisversus Third Party Scoring (ResearchGate Score)

 

7.6. Most Active Key Opinion Leaders

7.6.1. Profile: KOL A (Celgene)

7.6.2. Profile: KOL B (Western RegionalMedical Center)

7.6.3. Profile: KOL C (MedStarWashington Hospital Center)

7.6.4. Profile: KOL D (Cancer Instituteand Hospital)

7.6.5. Profile: KOL E (ComprehensiveCancer Centers of Nevada)

7.6.6. Profile: KOL F (Hopital Tenon)

7.6.7. Profile: KOL G (Cleveland Clinic)

 

8. TARGET COMPETITIVENESS ANALYSIS

8.1. Chapter Overview

8.2. Scope and Methodology

8.3. Competitiveness Analysis: Key ClinicalTargets for ADCs

8.3.1. Four-Dimensional Bubble Analysis

8.3.2 Five-Dimensional Spider WebAnalysis

 

8.4. Competitiveness Analysis: KeyPreclinical Targets for ADCs

8.4.1. Two-Dimensional Scatter PlotAnalysis

 

9. PARTNERSHIPS AND COLLABORATIONS

9.1. Chapter Overview

9.2. Partnership Models

9.3. ADC Therapeutics: List ofPartnerships and Collaborations

9.3.1 Analysis by Year of Partnerships

9.3.2. Analysis by Type of Partnerships

9.3.3. Most Active Players: Analysis byNumber of Partnerships

 

9.3.4. Regional Analysis

9.3.4.1. Intercontinental andIntracontinental Agreements

 

10. FUNDING AND INVESTMENT ANALYSIS

10.1. Chapter Overview

10.2. Types of Funding

10.3. ADC Therapeutics: Funding andInvestment Analysis

10.3.1. Analysis by Number of Instances

10.3.2. Analysis by Amount Invested

10.3.3. High Value Deals: Analysis byYear

10.3.4. Analysis by Type of Funding

 

10.3.5. Most Active Players

10.3.5.1. Analysis by Number of FundingInstances

10.3.5.2. Analysis by Amount Invested

10.4. Concluding Remarks

 

11. PATENT ANALYSIS

11 Patent Analysis

11.1. Chapter Overview

11.2. Scope and Methodology

11.3. ADC Therapeutics: Patent Analysis

11.3.1. Analysis by Publication Year

11.3.2. Analysis by GeographicalLocation

11.3.3. Analysis by CPC Classification

11.3.4. Emerging Focus Areas

11.3.5. Analysis by Type of Industry

11.3.6. Leading Players: Analysis byNumber of Patents

11.4. ADC Therapeutics: PatentBenchmarking Analysis (Industry Players)

11.4.1. Analysis by PatentCharacteristics

11.4.2. Analysis By GeographicalLocation

11.5. ADC Therapeutics: Patent ValuationAnalysis

 

12. ACADEMIC GRANTS

12.1. Chapter Overview

12.2. Scope and Methodology

12.3. ADC Therapeutics: List of AcademicGrants

12.3.1. Analysis by Number of Grants

12.3.2. Analysis by Type of Grant

12.3.3. Analysis by Grant Amount

12.3.4. Analysis by Focus Area

12.3.5. Analysis by Support Period

 

12.4. Leading Organizations: Analysis byNumber of Grants

12.5. Analysis by Type of RecipientOrganization

12.6. Analysis by AdministeringInstitute Center

12.7. Analysis by Funding InstituteCenter

12.8. Key Project Leaders: Analysis byNumber of Grants

 

13. KEY COMMMERCIALIZATION STRATEGIES

13.1. Chapter Overview

13.2. Successful Drug Launch Strategy:ROOTS Framework

13.3. Successful Drug Launch Strategy:Product Differentiation

13.4. Common CommercializationStrategies Adopted Based on Development Stage of Product

 

13.5. Approved Molecules for ADCs

13.5.1. ADCETRIS®

13.5.2. KADCYLA®

13.5.3. MYLOTARG™

13.5.4. BESPONSA®

13.5.5. LUMOXITI™

13.5.5. POLIVY™

 

13.6. Key Commercialization StrategiesAdopted by Companies Developing ADCs

13.6.1. Strategies Adopted Before DrugApproval

13.6.1.2. Collaboration with InternalStakeholders and Pharmaceutical Firms

 

13.6.2. Strategies Adopted During / PostDrug Approval

13.6.2.1. Geographical Expansion

13.6.2.2. Participation in Global Events

13.6.2.3. Awareness Through ProductWebsites

13.6.2.4. Collaboration with InternalStakeholders and Pharmaceutical Firms

13.7. Concluding Remarks

 

14. PROMOTIONAL ANALYSIS

14.1. Chapter Overview

14.2. Channels Used for PromotionalCampaigns

14.3. Summary of Product WebsiteAnalysis

14.4. Summary of Patient Brochure andInformative Downloads

 

14.5. ADCETRIS®: Promotional Analysis

14.5.1. Product Website Analysis

14.5.1.1. Messages for HealthcareProfessionals

14.5.1.2. Messages For Patients

14.5.2. Patient Support Services andInformative Downloads

14.5.3. Other Promotional Activities

14.5.3.1. Presence in Conferences

 

14.6. KADCYLA®: Promotional Analysis

14.6.1. Product Website Analysis

14.6.1.1. Messages for HealthcareProfessionals

14.6.1.2. Messages for Patients

14.6.2. Patient Support Services andInformative Downloads

14.6.3. Other Promotional Activities

14.6.3.1. Presence in Conferences

 

14.7. MYLOTARG™: Promotional Analysis

14.7.1. Product Website Analysis

14.7.1.1. Messages for HealthcareProfessionals

14.7.1.2. Messages for Patients

14.7.2. Patient Support Services andInformative Downloads

14.7.3. Other Promotional Activities

14.7.3.1. Presence in Conferences

 

14.8. BESPONSA®: Promotional Analysis

14.8.1. Product Website Analysis

14.8.1.1. Messages for HealthcareProfessionals

14.8.1.2. Messages for Patients

14.8.2. Patient Support Services andInformative Downloads

14.8.3. Other Promotional Activities

14.8.3.1. Presence in Conferences

 

14.9. LUMOXITI™: Promotional Analysis

14.9.1. Product Website Analysis

14.9.1.1. Messages for HealthcareProfessionals

14.9.1.2. Messages for Patients

14.9.2. Patient Support Services andInformative Downloads

14.9.3. Other Promotional Activities

14.9.3.1. Presence in Conferences

 

14.10. POLIVY™: Promotional Analysis

14.10.1. Product Website Analysis

14.10.1.1. Messages for HealthcareProfessionals

14.10.1.2. Messages for Patients

14.10.2. Patient Support Services andInformative Downloads

14.10.3. Other Promotional Activities

14.10.3.1. Presence in Conferences

 

15. COMBINATION THERAPIES

15.1. Chapter Overview

15.2. Combination Therapy: History ofDevelopment

15.3. FDA-approved Combination Therapiesin Oncology

 

15.4. Combination Therapy: FDAGuidelines

15.4.1. Combinations of Marketed Drugs

15.4.2. Combinations of Marketed Drugswith New Molecular Entities

15.4.3. Combinations of New MolecularEntities

 

15.5. Combination Therapies: ADCs

15.5.1. Completed / Ongoing ClinicalStudies of ADCs

15.5.1.1. Analysis by Type of Therapy

15.5.2. Completed / Ongoing ClinicalStudies of ADC-based Combination Therapies

15.5.2.1. Analysis by Highest Phase of Development

15.5.2.2. Analysis by Current TrialStatus

15.5.2.3. Analysis by Type ofCombination

15.5.2.4. Analysis by Indication andType of Combination

 

16. NOVEL CONJUGATION TECHNOLOGY PLATFORMS

16.1. Chapter Overview

16.2. First Generation ADC Technologies

 

16.3. Second Generation ADC Technologies

16.3.1. Cysteine and SelenocysteineEngineering

16.3.2. Unnatural Amino Acid Engineering

16.3.3. Amino-Terminal Engineered Serine

 

16.4. Third Generation ADC Technologies

16.4.1. Enzyme-Assisted Ligation Approaches

16.4.2. Glycan Remodeling Approaches

16.4.3. Ligation at FabNucleotide-Binding Site

16.4.4. Cysteine Rebridging

16.4.5. Preventing / LimitingRetro-Michael Drug Deconjugation

16.5. Evolutionary Analysis ofConjugation Technologies

 

17. ASSESMENT OF NON-CLINICAL DATA, FIRST IN HUMAN DOSING

17.1. Chapter Overview

17.2. ADCs and Non-Clinical Studies

17.3. ICH S9 Guidelines

 

17.4. Investigational New Drug(IND)-Enabling Study Designs

17.4.1. Example Case: KADCYLA®

 

17.5. Toxicities in Animal Models

17.6. Prediction of Maximum ToleratedDosage (MTD) in Humans

17.7. Other Key Considerations for StudyDesign

 

18. COST PRICE ANALYSIS

18.1. Chapter Overview

18.2. Factors Contributing Towards theHigh Price of ADC Therapeutics

18.3. ADC Therapeutics Market: PricingModels

18.3.1. On the Basis of Associated Costs

18.3.2. On the Basis of Competition

18.3.3. On the Basis of Patient Segment

18.4. Reimbursement Considerations forADC Therapeutics

 

19. CASE STUDY: CONTRACT MANUFACTURING OF ADC

19.1. Chapter Overview

19.2. Key Steps for ADC Manufacturing

19.3. Technical Concerns Related to ADCManufacturing

19.4. Challenges Associated with SupplyChain and Method Transfer

19.5. Limitations of In-HouseManufacturing

19.6. Investments in ADC ManufacturingCapability Expansions

19.7. Collaborations Established for ADCManufacturing

19.8. Growing Demand for ContractManufacturing

19.9. Emergence of Start-Ups OfferingContract Services

19.10. CMOs with Linker ManufacturingCapabilities

19.11. CMOs with HPAPI / CytotoxicPayload Manufacturing Capabilities

19.12. CMOs with ConjugationCapabilities

19.13. ADC One Stop Shops

 

20. CASE STUDY: COMPANION DIAGNOSTICS FOR ADC THERAPEUTICS

20.1. Chapter Overview

20.1.1. Advantages of CompanionDiagnostics

20.1.2. Disadvantages of CompanionDiagnostics

 

20.2. Companion Diagnostics for ADCTherapeutics

20.3. ADC Therapeutics: List ofCompanion Diagnostics

20.3.1. Analysis by Type of Target

20.3.2. Analysis by Type of CancerIndication

20.4. Concluding Remarks

 

21. MARKET FORECAST AND OPPORTUNITY ANALYSIS

21.1. Chapter Overview

21.2. Scope and Limitations

21.3. Forecast Methodology

 

21.4. Overall ADC Therapeutics Market

21.4.1. ADC Therapeutics Market:Distribution by Target Indication

21.4.2. ADC Therapeutics Market:Distribution by Type of Linker

21.4.3. ADC Therapeutics Market:Distribution by Type of Payload

21.4.4. ADC Therapeutics Market:Distribution by Target Antigen

21.4.5. ADC Therapeutics Market:Distribution by Geography

21.4.6. ADC Therapeutics Market:Distribution by Technology Providers

 

21.5. ADC Therapeutics Market:Individual Drug Sales Forecasts

21.5.1. ADCETRIS® / Brentuximab Vedotin

21.5.1.1. Target Patient Population

21.5.1.2. Sales Forecast

 

21.5.2. KADCYLA® / Ado-trastuzumabEmtansine

21.5.2.1. Target Patient Population

21.5.2.2. Sales Forecast

 

21.5.3. MYLOTARG™ / GemtuzumabOzogamicin

21.5.3.1. Target Patient Population

21.5.3.2. Sales Forecast

 

21.5.4. BESPONSA® / InotuzumabOzogamicin

21.5.4.1. Target Patient Population

21.5.4.2. Sales Forecast

 

21.5.5. LUMOXITI™

21.5.5.1. Target Patient Population

21.5.5.2. Sales Forecast

 

21.5.6. POLIVYTM / Polatuzumabvedotin-piiq / RG7596

21.5.6.1. Target Patient Population

21.5.6.2. Sales Forecast

 

21.5.7. ASG-22ME / Enfortumab Vedotin

21.5.7.1. Target Patient Population

21.5.7.2. Sales Forecast

 

21.5.8. BAT8001

21.5.8.1. Target Patient Population

21.5.8.2. Sales Forecast

 

21.5.9. DS-8201a / DS 8201 / TrastuzumabDeruxtecan

21.5.9.1. Target Patient Population

21.5.9.2. Sales Forecast

 

21.5.10. IMMU-132 / SacituzumabGovitecan

21.5.10.1. Target Patient Population

21.5.10.2. Sales Forecast

 

21.5.11. IMGN853 / MirvetuximabSoravtansine

21.5.11.1. Target Patient Population

21.5.11.2. Sales Forecast

 

21.5.12. lpituzumab TesirineRova-T /Rova

21.5.12.1. Target Patient Population

21.5.12.2. Sales Forecast

 

21.5.13. SYD985 / TrastuzumabDuocarmazine

21.5.13.1. Target Patient Population

21.5.13.2. Sales Forecast

 

21.5.14. ABBV-399 / Teliso-V /Telisotuzumab Vedotin

21.5.14.1. Target Patient Population

21.5.14.2. Sales Forecast

 

21.5.15. ADCT-301 / HuMax-TAC-ADC /Camidanlumab Tesirine

21.5.15.1. Target Patient Population

21.5.15.2. Sales Forecast

 

21.5.16. ADCT-402 / LoncastuximabTesirine

21.5.16.1. Target Patient Population

21.5.16.2. Sales Forecast

 

21.5.17. AGS 16M8F / AGS 16C3F

21.5.17.1. Target Patient Population

21.5.17.2. Sales Forecast

 

21.5.18. AVID100

21.5.18.1. Target Patient Population

21.5.18.2. Sales Forecast

 

21.5.19. BAY 94-9343

21.5.19.1. Target Patient Population

21.5.19.2. Sales Forecast

 

21.5.20. GSK 2857916 / Anti-BCMA ADC

21.5.20.1. Target Patient Population

21.5.20.2. Sales Forecast

 

21.5.21. HuMax-TF-ADC / TisotumabVedotin

21.5.21.1. Target Patient Population

21.5.21.2. Sales Forecast

 

21.5.22. IMGN529 / Debio 1562 /Naratuximab Emtansine

21.5.22.1. Target Patient Population

21.5.22.2. Sales Forecast

 

21.5.23. IMMU-130 / SacituzumabGovitecan

21.5.23.1. Target Patient Population

21.5.23.2. Sales Forecast

 

21.5.24. RC48

21.5.24.1. Target Patient Population

21.5.24.2. Sales Forecast

 

21.5.25. SGN-LIV1A / LadiratuzumabVedotin

21.5.25.1. Target Patient Population

21.5.25.2. Sales Forecast

 

22. SWOT ANALYSIS

22.1. Chapter Overview

22.2. Strengths

22.3. Weaknesses

22.4. Opportunities

22.5. Threats

22.6. Comparison of SWOT Factors

22.7. Concluding Remarks

 

23. CONCLUSION

23.1. Chapter Overview

23.2. Key Takeaways

 

24. EXECUTIVE INSIGHTS

24.1. Chapter Overview

24.2. Abzena

24.2.1. Company Snapshot

24.2.2. Interview Transcript: John Burt,Chief Executive Officer

 

24.3. Ajinomoto Bio-Pharma Services

24.3.1. Company Snapshot

24.3.2. Interview Transcript: TatsuyaOkuzumi, Associate General Manager

 

24.4. BSP Pharmaceuticals

24.4.1. Company Snapshot

24.4.2. Interview Transcript: AldoBraca, President and Chief Executive Officer and Giorgio Salciarini, TechnicalBusiness Development Senior Manager

 

24.5. Catalent Pharma Solutions

24.5.1. Company Snapshot

24.5.2. Interview Transcript: JenniferL. Mitcham, Director, SMARTag ADCs and Bioconjugates, and Stacy McDonald, GroupProduct Manager

 

24.6. Cardiff University

24.6.1. Company Snapshot

24.6.2. Interview Transcript: AlanBurnett, Professor, School of Medicine

 

24.7. Cerbios-Pharma

24.7.1. Company Snapshot

24.7.2. Interview Transcript: DenisAngioletti, Chief Commercial Officer

 

24.8. Eisai

24.8.1. Company Snapshot

24.8.2. Interview Transcript: ToshimitsuUenaka, Executive Director and Takashi Owa, Chief Innovation Officer

 

24.9. Lonza

24.9.1. Company Snapshot

24.9.2. Interview Transcript: LaurentDucry, Head of Bioconjugates Commercial Development

 

24.10. NBE-Therapeutics

24.10.1. Company Snapshot

24.10.2. Interview Transcript: WouterVerhoeven, Chief Business Officer

 

24.11. Oxford BioTherapeutics

24.11.1. Company Snapshot

24.11.2. Interview Transcript: ChristianRohlff, Chief Executive Officer and Founder

 

24.12. Pierre Fabre

24.12.1. Company Snapshot

24.12.2. Interview Transcript: ChristianBailly, Director of CDMO

 

24.13. Piramal Healthcare

24.13.1. Company Snapshot

24.13.2. Interview Transcript: MarkWright, Site Head, Grangemouth

 

24.14. Synaffix

24.14.1. Company Snapshot

24.14.2. Interview Transcript: AnthonyDeBoer, Director, Business Development

 

24.15. Syndivia

24.15.1. Company Snapshot

24.15.2. Interview Transcript: SashaKoniev, Chief Executive Officer and Co-Founder

 

24.16. Anonymous, Director, BusinessDevelopment, Leading CMO

24.17. Anonymous, Chief ExecutiveOfficer, Leading CMO

 

25. APPENDIX 1: TABULATED DATA

 

Contact Details

Gaurav Chaudhary

+1 (415) 800 3415

gaurav.chaudhary@rootsanalysis.com