DS-8201a, A Novel HER2-Targeting ADC with a Novel DNA Topoisomerase I Inhibitor, Demonstrates a Promising Antitumor Efficacy with Differentiation from T-DM1.

1. Daiichi Sankyo Co., Ltd., Tokyo, Japan.
Authors
Ogitani Y¹
Aida T¹
Hagihara K¹
Yamaguchi J¹
Ishii C¹
Harada N¹
Soma M¹
Okamoto H¹
Oitate M¹
Arakawa S¹
Atsumi R¹
Nakada T¹
Hayakawa I¹
Abe Y¹
Agatsuma T¹
(15 authors)
2. Clinical Development Department, Daiichi Sankyo RD Novare Co., Ltd., Tokyo, Japan.
Authors
Hirai T²
(1 author)

ORCIDs linked to this article

Hirai T | 0000-0002-0214-1056

Clinical Cancer Research : an Official Journal of the American Association for Cancer Research, 29 Mar 2016, 22(20):5097-5108
https://doi.org/10.1158/1078-0432.ccr-15-2822 PMID: 27026201

Abstract

Purpose

An anti-HER2 antibody-drug conjugate with a novel topoisomerase I inhibitor, DS-8201a, was generated as a new antitumor drug candidate, and its preclinical pharmacologic profile was assessed.

Experimental design

In vitro and in vivo pharmacologic activities of DS-8201a were evaluated and compared with T-DM1 in several HER2-positive cell lines and patient-derived xenograft (PDX) models. The mechanism of action for the efficacy was also evaluated. Pharmacokinetics in cynomolgus monkeys and the safety profiles in rats and cynomolgus monkeys were assessed.

Results

DS-8201a exhibited a HER2 expression-dependent cell growth-inhibitory activity and induced tumor regression with a single dosing at more than 1 mg/kg in a HER2-positive gastric cancer NCI-N87 model. Binding activity to HER2 and ADCC activity of DS-8201a were comparable with unconjugated anti-HER2 antibody. DS-8201a also showed an inhibitory activity to Akt phosphorylation. DS-8201a induced phosphorylation of Chk1 and Histone H2A.X, the markers of DNA damage. Pharmacokinetics and safety profiles of DS-8201a were favorable and the highest non-severely toxic dose was 30 mg/kg in cynomolgus monkeys, supporting DS-8201a as being well tolerated in humans. DS-8201a was effective in a T-DM1-insensitive PDX model with high HER2 expression. DS-8201a, but not T-DM1, demonstrated antitumor efficacy against several breast cancer PDX models with low HER2 expression.

Conclusions

DS-8201a exhibited a potent antitumor activity in a broad selection of HER2-positive models and favorable pharmacokinetics and safety profiles. The results demonstrate that DS-8201a will be a valuable therapy with a great potential to respond to T-DM1-insensitive HER2-positive cancers and low HER2-expressing cancers. Clin Cancer Res; 22(20); 5097-108. ©2016 AACR.

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