Physicochemical and functional characterization of trastuzumab-dkst, a trastuzumab biosimilar

Author:

Goyal Parag1ORCID,Iyer Jyoti2,Adhikary Laxmi2,Vats Bhavesh3,Kabadi Pradeep2,Pai Harish2ORCID,Ranayhossaini Daniel1,Gouda Shankara3,Subbarao Malini2ORCID,Mehta Gaurav3,Saha Arindam2,Bera Arnab2,Sahu Abhilashi2,Kaur Maninder2,Singh Ankita2,Marwah Ashwani2,Reddy Moole Praveen Kumar2,Smith Jeffrey1,Melarkode Ramakrishnan2ORCID,Ullanat Rajesh3ORCID

Affiliation:

1. Viatris, Inc., 1000 Mylan Boulevard, Canonsburg, PA 15317, USA

2. Biocon Biologics Limited, Biocon Special Economic Zone, Plot No. 2&3, Phase IV-B.I.A, Bommasandra-Jigani Link Road, Bangalore, 560099, India

3. Viatris Inc, Plot No 564/A/22, Road No 92, Jubilee Hills, Hyderabad, 500034, India

Abstract

Aims: Preclinical comparative similarity studies of trastuzumab-dkst, a Herceptin® biosimilar, are reported. Materials & methods: Primary sequence and higher order structure and pharmacological mechanisms of action were compared using multiple techniques. Pharmacokinetics and repeat-dose toxicity were assessed in cynomolgus monkeys. Results: Primary structures were identical; secondary and tertiary structures were highly similar. Non-significant differences were observed for charge heterogeneity. Twelve of 13 glycan species were highly similar, with slightly higher total mannose levels in trastuzumab-dkst. FcγR and FcRn binding activity was highly similar. Each drug equally inhibited HER2+ cell proliferation, demonstrating equivalent relative potency in mediating HER2+ cell cytolysis by antibody-dependent cellular cytotoxicity. Pharmacokinetic and toxicological profiles in cynomolgus monkeys were similar. Conclusion: Trastuzumab-dkst, US-licensed trastuzumab and EU-approved trastuzumab demonstrate high structural and functional similarity.

Funder

Viatris, Inc.

Biocon

Publisher

Future Science Ltd

Subject

Drug Discovery,Pharmacology,Molecular Medicine

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