Abstract 2700: ORM-6151: A first-in-class CD33-antibody enabled GSPT1 degrader for AML

Palacino, James; Lee, Pedro; Jeong, Hangyeol; Kim, Yeonjoon; Song, Yoojin; Permpoon, Uttapol; Wong, Wesley P.; Chen, Bai; Fishkin, Nathan; Takouri, Khuloud; Yu, Eunjun; Yao, Yi; Skaletskaya, Anna; Kim, Min‐Soo; Kim, ﻿Dayeong; Choi, Dong-Jin; Park, Peter U.

doi:10.1158/1538-7445.am2023-2700

Cited by 1 publication

(2 citation statements)

References 0 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…ORM-6151, a CD33-targeted DAC for patients with AML, has been developed by the same company. This DAC has demonstrated antigen-dependent in vitro cytotoxicity comparable to that of the FDA-approved anti-CD33 ADC gemtuzumab ozogamicin with superior activity, including complete eradication of all tumour cells in nine of nine animals with a single dose at 3 mg/ kg in an MV4-11 subcutaneous mouse xenograft model of AML 238,239 . Notably, even a 0.1 mg/kg single dose demonstrated effective disease control in a disseminated version of the MV4-11 xenograft model.…”

Section: Review Articlementioning

confidence: 94%

See 1 more Smart Citation

Exploring the next generation of antibody–drug conjugates

Tsuchikama,

Anami,

et al. 2024

Nat Rev Clin Oncol

View full text Add to dashboard Cite

Antibody-drug conjugates (ADCs) are a promising cancer treatment modality that enables the selective delivery of highly cytotoxic payloads to tumours. However, realizing the full potential of this platform necessitates innovative molecular designs to tackle several clinical challenges such as drug resistance, tumour heterogeneity and treatment-related adverse effects. Several emerging ADC formats exist, including bispecific ADCs, conditionally active ADCs (also known as probody-drug conjugates), immune-stimulating ADCs, protein-degrader ADCs and dual-drug ADCs, and each offers unique capabilities for tackling these various challenges. For example, probody-drug conjugates can enhance tumour specificity, whereas bispecific ADCs and dual-drug ADCs can address resistance and heterogeneity with enhanced activity. The incorporation of immune-stimulating and protein-degrader ADCs, which have distinct mechanisms of action, into existing treatment strategies could enable multimodal cancer treatment. Despite the promising outlook, the importance of patient stratification and biomarker identification cannot be overstated for these emerging ADCs, as these factors are crucial to identify patients who are most likely to derive benefit. As we continue to deepen our understanding of tumour biology and refine ADC design, we will edge closer to developing truly effective and safe ADCs for patients with treatment-refractory cancers. In this Review, we highlight advances in each ADC component (the monoclonal antibody, payload, linker and conjugation chemistry) and provide more-detailed discussions on selected examples of emerging novel ADCs of each format, enabled by engineering of one or more of these components.• To address these challenges, several novel ADC formats have been developed, including bispecific ADCs, probody-drug conjugates, immune-stimulating ADCs, protein-degrader ADCs and dual-drug ADCs.• Probody-drug conjugates are expected to have improved tumour specificity, whereas bispecific ADCs and dual-drug ADCs have the potential to combat drug resistance and tumour heterogeneity.• Integrating immune-stimulating ADCs and protein-degrader ADCs with current treatment regimens might enable multimodal treatment, potentially through several distinct mechanisms of action.• Patient stratification and biomarker identification will be crucial to maximize the clinical benefits of these emerging ADCs.Springer Nature or its licensor (e.g. a society or other partner) holds exclusive rights to this article under a publishing agreement with the author(s) or other rightsholder(s); author self-archiving of the accepted manuscript version of this article is solely governed by the terms of such publishing agreement and applicable law.

show abstract

Section: Review Articlementioning

confidence: 94%

“…234) and the chromatin regulatory protein SMARCA2 (also known as BRM) 235 . Two DACs designed to degrade the G1 to S phase transition 1 (GSPT1) protein are showing early signs of clinical potential [236][237][238][239] . These DACs use a highly potent CC-885-derived GSPT1-CRBN degrader as the payload.…”

Section: Review Articlementioning

confidence: 99%

Exploring the next generation of antibody–drug conjugates

Tsuchikama,

Anami,

et al. 2024

Nat Rev Clin Oncol

View full text Add to dashboard Cite

show abstract

Abstract 2700: ORM-6151: A first-in-class CD33-antibody enabled GSPT1 degrader for AML

Cited by 1 publication

References 0 publications

Exploring the next generation of antibody–drug conjugates

Exploring the next generation of antibody–drug conjugates

Contact Info

Product

Resources

About