2023
DOI: 10.1159/000533866
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The Potential of Trastuzumab Deruxtecan as a Tissue Agnostic Drug

Jan Trøst Jørgensen

Abstract: Background: Many modern anticancer drugs are designed to target specific molecular alterations harbored by the cancer. If a specific drug is able to target these alterations, regardless of the organ or tissue in which the cancer originates, it will often be characterized as a tissue- or tumor agnostic drug. According to the Food and Drug Administration (FDA), a tissue-agnostic drug refers to a drug that targets a specific molecular alteration across multiple cancer types, as defined by organ, tissue, or tumor … Show more

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Cited by 5 publications
(3 citation statements)
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“… 97 Trastuzumab deruxtecan (DS‐8201; T‐DXd) is a novel humanized HER2‐directed ADC with a high DAR (8:1) that was approved by the US FDA in 2019. 98 The structure of T‐DXd includes an anti‐HER2 IgG1 antibody (trastuzumab), a stable tetrapeptide‐based cleavable linker, and the exatecan derivative MAAA‐1181a (DXd), a DNA topoisomerase I inhibitor with 10‐fold higher inhibitory potency than irinotecan. T‐DXd has shown antitumor activity not only on HER2‐positive tumor cells but also on neighboring tumor cells with or without HER2 expression through a bystander effect.…”
Section: Therapeutic Trialsmentioning
confidence: 99%
See 1 more Smart Citation
“… 97 Trastuzumab deruxtecan (DS‐8201; T‐DXd) is a novel humanized HER2‐directed ADC with a high DAR (8:1) that was approved by the US FDA in 2019. 98 The structure of T‐DXd includes an anti‐HER2 IgG1 antibody (trastuzumab), a stable tetrapeptide‐based cleavable linker, and the exatecan derivative MAAA‐1181a (DXd), a DNA topoisomerase I inhibitor with 10‐fold higher inhibitory potency than irinotecan. T‐DXd has shown antitumor activity not only on HER2‐positive tumor cells but also on neighboring tumor cells with or without HER2 expression through a bystander effect.…”
Section: Therapeutic Trialsmentioning
confidence: 99%
“…T‐DXd has shown antitumor activity not only on HER2‐positive tumor cells but also on neighboring tumor cells with or without HER2 expression through a bystander effect. 98 The efficacy of TDM1 and T‐DXd has been demonstrated in randomized trials as first‐line, second‐line, or later treatment for solid cancer. Disitamab vedotin (RC48) is composed of: (1) hertuzumab, a new generation anti‐HER2 humanized monoclonal antibody with high specificity and affinity for HER2; (2) a maleimide–cysteine–valine–citrulline–para‐aminobenzyloxycarbonyl linker that releases the cytotoxic payload; and (3) a cytotoxic payload, MMAE, which inhibits microtubule polymerization in actively dividing cells.…”
Section: Therapeutic Trialsmentioning
confidence: 99%
“…As noted above, the efficacy of HER2-targeted therapy has been thought to vary between tumors of different primary origin, but the results demonstrating efficacy in such a wide range of areas has raised expectations for the tumor-agnostic effects of T-DXd [49]. In 2023, the DESTINY-PanTumor02 study was initiated as a phase II trial of T-DXd enrolling HER2-positive (IHC 2+ or IHC 3+) solid tumors for which HER2-targeted therapies had rarely or never been evaluated, including biliary tract, bladder, cervical, endometrial, ovarian, pancreatic, and other tumors [50].…”
Section: The Mechanism Of Action and Clinical Efficacy Of T-dxdmentioning
confidence: 99%