Affinity maturation of a novel antagonistic human monoclonal antibody with a long V<sub>H</sub>CDR3 targeting the Class A GPCR formyl-peptide receptor 1

Douthwaite, Julie A.; Sridharan, Sridha; Huntington, Catherine; Hammersley, Jayne; Marwood, Rose; Hakulinen, Jonna; Ek, Margareta; Sjögren, Tove; Rider, David A.; Privezentzev, Cyril V.; Seaman, Jonathan; Cariuk, Peter; Knights, Vikki; Young, Joyce L.; Wilkinson, Trevor; Sleeman, Matthew A.; Finch, Donna K.; Lowe, David C.; Vaughan, Tristan J.

doi:10.4161/19420862.2014.985158

Cited by 37 publications

(18 citation statements)

References 43 publications

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“…29) with recombinant human 5T4 using a 48-day rest/boost immunization protocol (30) and was identified from a biochemical assay of hybridoma supernatants for binding to 5T4. This antibody underwent affinity optimization by CDR-directed mutagenesis (31) and phage display selection (32,33).…”

Section: Generation Of the Lead Anti-5t4 Antibody 5t4_0108mentioning

confidence: 99%

Preclinical Evaluation of MEDI0641, a Pyrrolobenzodiazepine-Conjugated Antibody–Drug Conjugate Targeting 5T4

Harper¹,

Lloyd²,

Dimasi³

et al. 2017

Molecular Cancer Therapeutics

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Antibody-drug conjugates (ADC) are used to selectively deliver cytotoxic agents to tumors and have the potential for increased clinical benefit to cancer patients. 5T4 is an oncofetal antigen overexpressed on the cell surface in many carcinomas on both bulk tumor cells as well as cancer stem cells (CSC), has very limited normal tissue expression, and can internalize when bound by an antibody. An anti-5T4 antibody was identified and optimized for efficient binding and internalization in a target-specific manner, and engineered cysteines were incorporated into the molecule for site-specific conjugation. ADCs targeting 5T4 were constructed by site-specifically conjugating the antibody with payloads that possess different mechanisms of action, either a DNA cross-linking pyrrolobenzodiazepine (PBD) dimer or a microtubule-destabilizing tubulysin, so that each ADC had a drug:antibody ratio of 2. The resulting ADCs demonstrated significant target-dependent activity in vitro and in vivo; however, the ADC conjugated with a PBD payload (5T4-PBD) elicited more durable antitumor responses in vivo than the tubulysin conjugate in xenograft models. Likewise, the 5T4-PBD more potently inhibited the growth of 5T4-positive CSCs in vivo, which likely contributed to its superior antitumor activity. Given that the 5T4-PBD possessed both potent antitumor activity as well as anti-CSC activity, and thus could potentially target bulk tumor cells and CSCs in target-positive indications, it was further evaluated in non-GLP rat toxicology studies that demonstrated excellent in vivo stability with an acceptable safety profile. Taken together, these preclinical data support further development of 5T4-PBD, also known as MEDI0641, against 5T4 þ cancer indications. Mol Cancer Ther;16(8); 1576-87. Ó2017 AACR.

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Section: Generation Of the Lead Anti-5t4 Antibody 5t4_0108mentioning

confidence: 99%

Preclinical Evaluation of MEDI0641, a Pyrrolobenzodiazepine-Conjugated Antibody–Drug Conjugate Targeting 5T4

Harper¹,

Lloyd²,

Dimasi³

et al. 2017

Molecular Cancer Therapeutics

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“…These can be broadly divided into those obtained by XFEL, such as 5-HT 2B [75] and GCG [76], and X-ray crystallography, such as TSHR [77], GIP [78] and EP4 [79]. Other studies have conducted homology modeling in combination with intensive epitope mapping to identify putative important contact residues of functional antibodies, e.g., CXCR4 [80], or by obtaining a crystal structure of the Fab fragment and modeled in combination with a GPCR homology model, e.g., FPR1 [81], but the greatest accuracy is obtained from high-resolution crystallography approaches. The knowledge gained from such studies can inform decisionmaking in the drug discovery process.…”

Section: Expert Opinionmentioning

confidence: 99%

A review of antibody-based therapeutics targeting G protein-coupled receptors: an update

Hutchings

2020

Expert Opinion on Biological Therapy

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“…The third complementary determining region of the heavy chain (CDR H3) is particularly important in antibody molecules as it contains the greatest diversity and also usually makes the most extensive contact with antigen. Long CDR H3 regions are often found in broadly neutralizing antibodies targeting human immunodeficiency (HIV), influenza, and polio viruses[4–8], and are also thought to be important in binding challenging antigens like G-protein coupled receptors and protease active sites[9, 10]. Thus, genetic mechanisms to form long CDR H3s may be very important in immune responses against key antigens.…”

Section: Introductionmentioning

confidence: 99%

Formation of ultralong DH regions through genomic rearrangement

Smider

2019

Preprint

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Cow antibodies are very unusual in having exceptionally long CDR H3 regions. The genetic basis for this length largely derives from long heavy chain diversity (DH) regions, with a single “ultralong” DH, IGHD8-2, encoding over fifty amino acids. Most bovine IGHD regions are homologous but have several nucleotide repeating units that diversify their lengths. Genomically, most DH regions exist in three clusters that appear to have formed from DNA duplication events. The cluster containing IGHD8-2 underwent a rearrangement and deletion event in relation to the other clusters in the region corresponding to IGHD8-2, with possible fusion of two DH regions and expansion of short repeats to form the ultralong IGHD8-2 gene. Length heterogeneity within DH regions is a unique evolutionary genomic mechanism to create immune diversity, including formation of ultralong CDR H3 regions.

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Affinity maturation of a novel antagonistic human monoclonal antibody with a long V_HCDR3 targeting the Class A GPCR formyl-peptide receptor 1

Cited by 37 publications

References 43 publications

Preclinical Evaluation of MEDI0641, a Pyrrolobenzodiazepine-Conjugated Antibody–Drug Conjugate Targeting 5T4

Preclinical Evaluation of MEDI0641, a Pyrrolobenzodiazepine-Conjugated Antibody–Drug Conjugate Targeting 5T4

A review of antibody-based therapeutics targeting G protein-coupled receptors: an update

Formation of ultralong DH regions through genomic rearrangement

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Affinity maturation of a novel antagonistic human monoclonal antibody with a long VHCDR3 targeting the Class A GPCR formyl-peptide receptor 1

Cited by 37 publications

References 43 publications

Preclinical Evaluation of MEDI0641, a Pyrrolobenzodiazepine-Conjugated Antibody–Drug Conjugate Targeting 5T4

Preclinical Evaluation of MEDI0641, a Pyrrolobenzodiazepine-Conjugated Antibody–Drug Conjugate Targeting 5T4

A review of antibody-based therapeutics targeting G protein-coupled receptors: an update

Formation of ultralong DH regions through genomic rearrangement

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Product

Resources

About

Affinity maturation of a novel antagonistic human monoclonal antibody with a long V_HCDR3 targeting the Class A GPCR formyl-peptide receptor 1