Precision Chemoradiotherapy for HER2 Tumors Using Antibody Conjugates of an Auristatin Derivative with Reduced Cell Permeability

Hingorani, Dina V.; Doan, Matthew K.; Camargo, M. Fernanda; Aguilera, Joseph; Song, Seung Hun; Pizzo, Donald; Scanderbeg, Daniel J.; Cohen, Ezra E.W.; Lowy, Andrew M.; Adams, Stephen; Advani, Sunil J.

doi:10.1158/1535-7163.mct-18-1302

Cited by 22 publications

(24 citation statements)

References 50 publications

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“… 30 – 32 Conjugation of MMAF with several antibodies resulted in ADCs with potent anti-tumor activities. 33 – 36 The free carboxyl group of MMAF also facilitates synthesis of drug-linker conjugates with high potency. 37 Trastuzumab and MMAF were selected as a model targeting antibody and cytotoxic payload for synthesizing the PAR polymer-based ADC.…”

Section: Resultsmentioning

confidence: 99%

A poly-ADP-ribose polymer-based antibody-drug conjugate

et al. 2020

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Section: Resultsmentioning

confidence: 99%

A poly-ADP-ribose polymer-based antibody-drug conjugate

et al. 2020

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“…As a tubulin-binding molecule, dolastatin exerts its cytotoxic effect through the inhibition of microtubule assembly and tubulin-dependent GTP hydrolysis, leading to cell cycle arrest and apoptosis ( 21 ). MMAF differs from another auristatin derivative, monomethyl auristatin E (MMAE), for a C-terminal modification which is aimed to limit membrane permeability and reduce bystander and off-target toxicity ( 22 ). A phase 1 study (NCT01786135) demonstrated the safety of SGN-CD19A in the clinical setting of R/R B-cell NHL, with 30% of evaluable patients achieving a complete response ( 23 ).…”

Section: Antibody-drug Conjugatesmentioning

confidence: 99%

CD19-Targeted Immunotherapies for Diffuse Large B-Cell Lymphoma

et al. 2022

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Surgical resection, chemotherapy and radiotherapy were, for many years, the only available cancer treatments. Recently, the use of immune checkpoint inhibitors and adoptive cell therapies has emerged as promising alternative. These cancer immunotherapies are aimed to support or harness the patient’s immune system to recognize and destroy cancer cells. Preclinical and clinical studies, based on the use of T cells and more recently NK cells genetically modified with chimeric antigen receptors retargeting the adoptive cell therapy towards tumor cells, have already shown remarkable results. In this review, we outline the latest highlights and progress in immunotherapies for the treatment of Diffuse Large B-cell Lymphoma (DLBCL) patients, focusing on CD19-targeted immunotherapies. We also discuss current clinical trials and opportunities of using immunotherapies to treat DLBCL patients.

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“…F7-ADC consists of F7-Ab conjugated to the antimitotic drug, monomethyl auristatin E (MMAE), by cleavable MC-VC-PABC linkers (Figure 2A). An average of four MMAE molecules were conjugated to cysteine residues in the antibody hinge region, following reduction of disulfides (41,42). For non-invasive F7-ADC tracking, we also conjugated a Cy5 fluorophore to a hinge region disulfide via a non-cleavable maleimide linker.…”

Section: Antibody-drug Conjugate Septuximab Vedotin Binds Fzd7mentioning

confidence: 99%

“…F7-Ab-MMAE drug conjugate was synthesized using methods previously described (41,42). A solution (2 mL, 10.2 mg/mL) of F7-Ab was treated with sodium bicine buffer (200 μL, 1M pH 8.3) and sodium diethylenetriaminepentaacetic acid (20 μL, 100 mM pH 7).…”

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confidence: 99%

A FZD7-specific Antibody–Drug Conjugate Induces Ovarian Tumor Regression in Preclinical Models

Sonavane

et al. 2021

Molecular Cancer Therapeutics

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Though WNT signaling is frequently dysregulated in solid tumors, drugging this pathway has been challenging due to off-tumor effects. Current clinical pan-WNT inhibitors are non-specific and lead to adverse effects, highlighting the urgent need for more specific WNT-pathway targeting strategies. We identified elevated expression of the WNT receptor Frizzled class receptor 7 (FZD7) in multiple solid cancers in The Cancer Genome Atlas, particularly in the mesenchymal and proliferative subtypes of ovarian serous cystadenocarcinoma, which correlate with poorer median patient survival. Moreover, we observed increased FZD7 protein expression in ovarian tumors compared to normal ovarian tissue, indicating that FZD7 may be a tumorspecific antigen. We therefore developed a novel antibody-drug conjugate, septuximab vedotin (F7-ADC), which is composed of a chimeric human-mouse antibody to human FZD7 conjugated to the microtubule-inhibiting drug monomethyl auristatin E (MMAE). F7-ADC selectively binds human FZD7, potently kills ovarian cancer cells in vitro, and induces regression of ovarian tumor xenografts in murine models. To evaluate F7-ADC toxicity in vivo, we generated mice harboring a modified Fzd7 gene where the resulting Fzd7 protein is reactive with the humantargeting F7-ADC. F7-ADC treatment of these mice did not induce acute toxicities, indicating a potentially favorable safety profile in patients. Overall, our data suggest that the antibody-drug conjugate approach may be a powerful strategy to combat FZD7-expressing ovarian cancers in the clinic.

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Precision Chemoradiotherapy for HER2 Tumors Using Antibody Conjugates of an Auristatin Derivative with Reduced Cell Permeability

Cited by 22 publications

References 50 publications

A poly-ADP-ribose polymer-based antibody-drug conjugate

A poly-ADP-ribose polymer-based antibody-drug conjugate

CD19-Targeted Immunotherapies for Diffuse Large B-Cell Lymphoma

A FZD7-specific Antibody–Drug Conjugate Induces Ovarian Tumor Regression in Preclinical Models

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