Innovative Bioconjugation Technology for Antibody–Drug Conjugates: Proof of Concept in a CD30-Positive Lymphoma Mouse Model

Juen, Ludovic; Baltus, Christine B.; Gély, Camille; Feuillâtre, Ofelia; Desgranges, Audrey; Viaud‐Massuard, Marie‐Claude; Martin, Camille

doi:10.1021/acs.bioconjchem.1c00058

Cited by 14 publications

(22 citation statements)

References 29 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In the present study, the bioconjugation technology was devoid of a first‐generation maleimide motif, leading to the production of a homogeneous ADC with an optimal average DAR close to 4, which might result in stronger therapeutic activity and reduced toxicities. Moreover, ADC produced with our bioconjugation technology recently demonstrated enhanced stability under thermal stress conditions or in the presence of human serum albumin, when compared to first‐generation ADCs 42 . Thus, the use of site‐specific bioconjugation technology for the generation of Adcitmer ® is likely to improve the toxicity rates of Adcitmer ® over lorvotuzumab mertansine.…”

Section: Discussionmentioning

confidence: 95%

“…Moreover, ADC produced with our bioconjugation technology recently demonstrated enhanced stability under thermal stress conditions or in the presence of human serum albumin, when compared to first-generation ADCs. 42 Thus, the use of site-specific bioconjugation technology for the generation of Adcitmer â is likely to improve the toxicity rates of Adcitmer â over lorvotuzumab mertansine. Further toxicity studies, such as the determination of the maximum tolerated dose and optimization of the therapeutic scheme, have to be conducted during further development.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Adcitmer ^® , a new CD56‐targeting monomethyl auristatin E‐conjugated antibody, is a potential therapeutic approach in Merkel cell carcinoma*

Esnault

Leblond

Martin³

et al. 2021

Br J Dermatol

View full text Add to dashboard Cite

Summary Background Merkel cell carcinoma (MCC) is an aggressive skin cancer, whose tumour cells often express CD56. While immune checkpoint inhibitors constitute a major advance for treating patients with MCC with advanced disease, new therapeutic options are still urgently required. Objectives To produce and evaluate the therapeutic performance of a new antibody–drug conjugate (Adcitmer®) targeting CD56 in preclinical models of MCC. Methods CD56 expression was evaluated in a MCC cohort (immunohistochemistry on a tissue microarray of 90 tumour samples) and MCC cell lines. Interaction of an unconjugated CD56‐targeting antibody with CD56+ MCC cell lines was investigated by immunohistochemistry and imaging flow cytometry. Adcitmer® product was generated by the bioconjugation of CD56‐targeting antibody to a cytotoxic drug (monomethyl auristatin E) using the McSAF Inside® bioconjugation process. The chemical properties and homogeneity of Adcitmer® were characterized by hydrophobic interaction chromatography. Adcitmer® cytotoxicity was evaluated in vitro and in an MCC xenograft mice model. Results Similar to previous reports, CD56 was expressed by 66% of MCC tumours in our cohort, confirming its relevance as a therapeutic target. Specific binding and internalization of the unconjugated CD56‐targeting antibody was validated in MCC cell lines. The high homogeneity of the newly generated Adcitmer® was confirmed by hydrophobic interaction chromatography. The CD56‐mediated cytotoxicity of Adcitmer® was demonstrated in vitro in MCC cell lines. Moreover, Adcitmer® significantly reduced tumour growth in a MCC mouse model. Conclusions Our study suggests that Adcitmer® should be further assessed as a therapeutic option in patients with MCC, as an alternative therapy or combined with immune checkpoint inhibitors.

show abstract

Section: Discussionmentioning

confidence: 95%

Section: Discussionmentioning

confidence: 99%

Adcitmer ^® , a new CD56‐targeting monomethyl auristatin E‐conjugated antibody, is a potential therapeutic approach in Merkel cell carcinoma*

Esnault

Leblond

Martin³

et al. 2021

Br J Dermatol

View full text Add to dashboard Cite

show abstract

“…Indeed, site-specific conjugation of antibodies has been shown to improve the therapeutic index because it improves ADC pharmacokinetics by reducing the hydrophobicity of the linker-payload as well as prevent the release of payload in blood [48]. Moreover, site-specific conjugation with rebridging of antibody disulfide bonds results in stable and homogeneous ADCs with a controlled number and position of payload, and higher stability characteristics [50].…”

Section: Linker-antibody Conjugationmentioning

confidence: 99%

Antibody–Drug Conjugates as an Emerging Therapy in Oncodermatology

Esnault

Schrama

Houben

et al. 2022

Cancers

Self Cite

View full text Add to dashboard Cite

Antibody–drug conjugates (ADCs) are an emerging class of therapeutics, with twelve FDA- and EMA-approved drugs for hematological and solid cancers. Such drugs consist in a monoclonal antibody linked to a cytotoxic agent, allowing a specific cytotoxicity to tumor cells. In recent years, tremendous progress has been observed in therapeutic approaches for advanced skin cancer patients. In this regard, targeted therapies (e.g., kinase inhibitors) or immune checkpoint-blocking antibodies outperformed conventional chemotherapy, with proven benefit to survival. Nevertheless, primary and acquired resistances as well as adverse events remain limitations of these therapies. Therefore, ADCs appear as an emerging therapeutic option in oncodermatology. After providing an overview of ADC design and development, the goal of this article is to review the potential ADC indications in the field of oncodermatology.

show abstract

“…Additional technology has been reported by Juen, Martin, and coworkers, who developed the McSAF Inside Technology based on a trifunctionalized di(bromomethyl)pyridine scaffold capable of bridging the antibody chains at reduced disulfide interchain bonds to incorporate the corresponding linker-drug complex [ 110 , 111 ]. This new strategy allows the control of the DAR and position of the linker-payload resulting in the formation of highly stable and homogeneous ADCs.…”

Section: Chemistry and Biology Of Marine Antibody-drug Conjugatesmentioning

confidence: 99%

Antibody-Drug Conjugates Containing Payloads from Marine Origin

et al. 2022

View full text Add to dashboard Cite

Antibody-drug conjugates (ADCs) are an important class of therapeutics for the treatment of cancer. Structurally, an ADC comprises an antibody, which serves as the delivery system, a payload drug that is a potent cytotoxin that kills cancer cells, and a chemical linker that connects the payload with the antibody. Unlike conventional chemotherapy methods, an ADC couples the selective targeting and pharmacokinetic characteristics related to the antibody with the potent cytotoxicity of the payload. This results in high specificity and potency by reducing off-target toxicities in patients by limiting the exposure of healthy tissues to the cytotoxic drug. As a consequence of these outstanding features, significant research efforts have been devoted to the design, synthesis, and development of ADCs, and several ADCs have been approved for clinical use. The ADC field not only relies upon biology and biochemistry (antibody) but also upon organic chemistry (linker and payload). In the latter, total synthesis of natural and designed cytotoxic compounds, together with the development of novel synthetic strategies, have been key aspects of the consecution of clinical ADCs. In the case of payloads from marine origin, impressive structural architectures and biological properties are observed, thus making them prime targets for chemical synthesis and the development of ADCs. In this review, we explore the molecular and biological diversity of ADCs, with particular emphasis on those containing marine cytotoxic drugs as the payload.

show abstract

Innovative Bioconjugation Technology for Antibody–Drug Conjugates: Proof of Concept in a CD30-Positive Lymphoma Mouse Model

Cited by 14 publications

References 29 publications

Adcitmer ^® , a new CD56‐targeting monomethyl auristatin E‐conjugated antibody, is a potential therapeutic approach in Merkel cell carcinoma*

Adcitmer ^® , a new CD56‐targeting monomethyl auristatin E‐conjugated antibody, is a potential therapeutic approach in Merkel cell carcinoma*

Antibody–Drug Conjugates as an Emerging Therapy in Oncodermatology

Antibody-Drug Conjugates Containing Payloads from Marine Origin

Contact Info

Product

Resources

About

Innovative Bioconjugation Technology for Antibody–Drug Conjugates: Proof of Concept in a CD30-Positive Lymphoma Mouse Model

Cited by 14 publications

References 29 publications

Adcitmer ® , a new CD56‐targeting monomethyl auristatin E‐conjugated antibody, is a potential therapeutic approach in Merkel cell carcinoma*

Adcitmer ® , a new CD56‐targeting monomethyl auristatin E‐conjugated antibody, is a potential therapeutic approach in Merkel cell carcinoma*

Antibody–Drug Conjugates as an Emerging Therapy in Oncodermatology

Antibody-Drug Conjugates Containing Payloads from Marine Origin

Contact Info

Product

Resources

About

Adcitmer ^® , a new CD56‐targeting monomethyl auristatin E‐conjugated antibody, is a potential therapeutic approach in Merkel cell carcinoma*

Adcitmer ^® , a new CD56‐targeting monomethyl auristatin E‐conjugated antibody, is a potential therapeutic approach in Merkel cell carcinoma*