Actinium Highlights First-In-Class HER3 Targeted Radiotherapy Data Demonstrating Potent Anti-Cancer Activity of in Ovarian and Colorectal Cancer Models at the AACR Annual Meeting
Actinium Pharmaceuticals presented groundbreaking preclinical data on HER3-targeted radiotherapy at the AACR 2023 Annual Meeting, reporting a significant reduction in tumor volume (p<0.0001) for ovarian cancer when conjugated to Actinium-225 or Lutetium-177, outperforming bevacizumab.
The HER3 target is frequently overexpressed in various solid tumors and linked to poor survival rates. The results indicated effective target engagement and cytotoxic activity in preclinical models for both ovarian and colorectal cancers.
Actinium aims to address high unmet medical needs, highlighting the potential for broad application in different oncology indications. The data showcases Actinium's innovative approach, reaffirming its commitment to developing efficient targeted therapies.
- Significant reduction in tumor volume (p<0.0001) in ovarian cancer model with HER3-ARC conjugated to Actinium-225 or Lutetium-177 compared to bevacizumab.
- HER3-ARC demonstrated strong anti-cancer effects in preclinical models of high unmet need cancers.
- Broad utility of HER3-targeted agents indicated due to consistent overexpression in various solid tumors.
- None.
- Highly significant (p<0.0001) reduction in tumor volume in ovarian cancer model when using HER3-ARC conjugated to either Actinium-225 or Lutetium-177 compared to bevacizumab (Avastin)
- HER3 is expressed at high levels within multiple solid tumors and has been linked to poor survival and drug resistance, providing strong rationale for HER3 targeted radiotherapy in a clinical setting
Highlights from the AACR poster titled, "Novel HER3 targeting antibody radioconjugates, 225Ac-HER3 ARC and 177Lu-HER3 ARC, exhibit potent antitumor efficacy in HER3-positive solid tumors" include:
- Actinium's HER3-targeted radiotherapy displayed strong anticancer activity when conjugated to either alpha-emitting Actinium-225 or beta-emitting Lutetium-177 in models of two high unmet need cancers, highlighting its therapeutic potential for HER3+ malignancies
- HER3-ARC showed strong target engagement and efficient cellular internalization with compelling cytotoxic activity against established in vitro cellular models
- A single dose of HER3-ARC, conjugated to either Actinium-225 (p<0.0001) or Lutetium-177 (p<0.0001) showed highly significant reductions in tumor burden in a preclinical ovarian cancer model compared to bevacizumab, an anti-VEGF monoclonal antibody indicated in ovarian cancer
- Promising antitumor activity displayed in a preclinical model of colorectal cancer, a highly aggressive malignancy, including a significant reduction in tumor volume (p<0.0001) when dosed with 225Ac-HER3-ARC
- The consistent overexpression of HER3 in multiple solid tumor types including ovarian, renal, prostate, urothelial, breast, and lung cancers suggests broad utility of a HER3-targeted agent across oncology indications
"Actinium is committed to developing targeted radiotherapies for patients with unmet needs and our program targeting HER3, a validated, pan-cancer target, is a strong representation of our R&D capabilities", said
HER3 is a member of the EGFR family, a highly validated cancer target for which there are several approved therapies directed against EGFR and/or HER2. However, there are no approved therapeutics targeting HER3, which is upregulated in response to EGFR and HER2 therapies as part of acquired resistance and is associated with poor survival in multiple solid tumors including breast, colorectal, lung, ovarian and others.
The poster will be available on the presentations page of Actinium's investor relations page of its website: https://ir.actiniumpharma.com/presentations-webinars.
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