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Review
. 2016 Oct;38(10):1655-64.
doi: 10.1007/s10529-016-2160-x. Epub 2016 Jun 22.

Antibody drug conjugates

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Review

Antibody drug conjugates

Ray Bakhtiar. Biotechnol Lett. 2016 Oct.

Abstract

Antibody drug conjugates (ADCs) have emerged as a viable option in targeted delivery of highly potent cytotoxic drugs in treatment of solid tumors. At the time of writing, only two ADCs have received regulatory approval with >40 others in clinical development. The first generation ADCs suffered from a lack of specificity in amino acid site-conjugations, yielding statistically heterogeneous stoichiometric ratios of drug molecules per antibody molecule. For the second generation ADCs, however, site-specific amino acid conjugation using enzymatic ligation, introduction of unnatural amino acids, and site-specific protein engineering hold promise to alleviate some of the current technical limitations. The rapid progress in technology platforms and antibody engineering has introduced novel linkers, site-specific conjugation chemistry, and new payload candidates that could possibly be exploited in the context of ADCs. A search using the Clinical Trial Database registry ( www.clinicaltrials.gov ), using the keyword 'antibody drug conjugate', yielded ~270 hits. The main focus of this article is to present a brief overview of the recent developments and current challenges related to ADC development.

Keywords: Brentuximab vedotin; Chemical linkers; Conjugation; Cytotoxicity; Payload; Solid tumors; Transtuzumab emtansine.

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