An Antibody-Drug Conjugate for Multiple Myeloma Prepared by Multi-Arm Linkers

Overview

Journal Adv Sci (Weinh)

Specialty Biomedical Engineering

Date 2024 Mar 13

PMID 38477561

Authors

Yueh-Hsiang Yu

Wei-Ting Tian

Cedric Grauffel

Wei-Chen Lin

Ming-Yu Hsieh

Pei-Wen Wu

Hui-Ju Lee

Chi-Jiun Peng

Pei-Hsuan Lin

Hsing-Mao Chu

Carmay Lim

Tse Wen Chang

Affiliations

Soon will be listed here.

Abstract

First-line treatment of multiple myeloma, a prevalent blood cancer lacking a cure, using anti-CD38 daratumumab antibody and lenalidomide is often inadequate due to relapse and severe side effects. To enhance drug safety and efficacy, an antibody-drug conjugate, TE-1146, comprising six lenalidomide drug molecules site-specifically conjugated to a reconfigured daratumumab to deliver cytotoxic lenalidomide to tumor cells is developed. TE-1146 is prepared using the HighDAR platform, which employs i) a maleimide-containing "multi-arm linker" to conjugate multiple drug molecules creating a drug bundle, and ii) a designed peptide with a Zn-binding cysteine at the C-termini of a reconfigured daratumumab for site-specific drug bundle conjugation. It is shown that TE-1146 remains intact and effectively enters CD38-expressing tumor cells, releasing lenalidomide, leading to enhanced cell-killing effects compared to lenalidomide/daratumumab alone or their combination. This reveals the remarkable potency of lenalidomide once internalized by myeloma cells. TE-1146 precisely delivers lenalidomide to target CD38-overexpressing tumor cells. In contrast, lenalidomide without daratumumab cannot easily enter cells, whereas daratumumab without lenalidomide relies on Fc-dependent effector functions to kill tumor cells.

Citing Articles

An Antibody-Drug Conjugate for Multiple Myeloma Prepared by Multi-Arm Linkers.

Yu Y, Tian W, Grauffel C, Lin W, Hsieh M, Wu P Adv Sci (Weinh). 2024; 11(20):e2307852.

PMID: 38477561 PMC: 11132082. DOI: 10.1002/advs.202307852.

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