A biomimetic chip to assess subcutaneous bioavailability of monoclonal antibodies in humans

Author:

Chandran Suja Vineeth12,Qi Qin M12,Halloran Kevin3,Zhang Jifeng3,Shaha Suyog12,Prakash Supriya12,Kumbhojkar Ninad12,Deslandes Antoine4,Huille Sylvain4,Gokarn Yatin R3,Mitragotri Samir12

Affiliation:

1. School of Engineering and Applied Sciences, Harvard University , Boston, MA 02134 , USA

2. Wyss Institute for Biologically Inspired Engineering , 3 Blackfan Circle , Boston, MA 02115, USA

3. Sanofi , 350 Water St , Cambridge, MA 02141, USA

4. Sanofi R&D , Impasse Des Ateliers , Vitry-sur-Seine 94400 France

Abstract

Abstract Subcutaneous (subQ) injection is a common route for delivering biotherapeutics, wherein pharmacokinetics is largely influenced by drug transport in a complex subQ tissue microenvironment. The selection of good drug candidates with beneficial pharmacokinetics for subQ injections is currently limited by a lack of reliable testing models. To address this limitation, we report here a Subcutaneous Co-Culture Tissue-on-a-chip for Injection Simulation (SubCuTIS). SubCuTIS possesses a 3D coculture tissue architecture, and it allows facile quantitative determination of relevant scale independent drug transport rate constants. SubCuTIS captures key in vivo physiological characteristics of the subQ tissues, and it differentiates the transport behavior of various chemically distinct molecules. We supplemented the transport measurements with theoretical modeling, which identified subtle differences in the local absorption rate constants of seven clinically available mAbs. Accounting for first-order proteolytic catabolism, we established a mathematical framework to assess clinical bioavailability using the local absorption rate constants obtained from SubCuTIS. Taken together, the technology described here broadens the applicability of organs-on-chips as a standardized and easy-to-use device for quantitative analysis of subQ drug transport.

Publisher

Oxford University Press (OUP)

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