Therapeutic Immunotoxins with Increased Half-Life and Anti-Tumor Activity
Recombinant Immunotoxins (RITs) are chimeric molecules composed of an antigen binding domain and toxin. The antigen binding domain component targets the cancer cell and delivers the toxin component to the cell. However, the efficacy of RITs is limited by their short half-life once they are in the patient. To address this problem, investigators at the National Cancer Institute (NCI) increased the half-life of RITs using polyethylene glycol (PEG).
In specific embodiments, the antigen-binding fragment targets mesothelin, and the toxin is a fragment of Pseudomonas exotoxin (PE). Mesothelin is highly expressed in many human cancers including mesotheliomas, ovarian cancers, squamous cell carcinoma and pancreatic cancers – making it an excellent candidate for targeted therapies. The resulting PEGylated RITs have an increased half-life while retaining cytotoxic activity, thus increasing anti-tumor activity in mouse models. This indicates that site-specific modification with PEG can improve the therapeutic utility of RITs. Furthermore, the ability of PEGylation to increase the half-life of RITs can be applied to other RITs directed against different targets.
The NCI Laboratory of Molecular Biology is seeking parties interested in co-development research collaborations and/or licensing of this technology for commercialization in the field of recombinant immunotoxins and cancer therapeutics.
Potential Commercial Applications: | Competitive Advantages: |
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Development Stage:
Pre-clinical (in vivo)
Related Invention(s):
E-292-2007
Inventors:
Ira Pastan (NCI) ➽ more inventions...
Zeliang Zheng (NCI) ➽ more inventions...
Intellectual Property:
Application No. 62/935,822
Publications:
Zheng Z, et al. Site-specific PEGylation of anti-mesothelin recombinant immunotoxins increases half-life and antitumor activity. PMID 31871266
Collaboration Opportunity:
Licensing and research collaboration
Licensing Contact:
John Hewes, Ph.D.
Email: John.Hewes@nih.gov
Phone: 240-276-5515
OTT Reference No: E-179-2019
Updated: Aug 17, 2020