Abstract

New immunotoxins (ITs) are being developed for clinical use. Laboratory efforts are focused on using phage display to identify new antibodies and to produce new ITs directed at various tumors (breast, ovary, prostate, lung, colon, mesothelioma, astrocytoma) and lymphomas and leukemias. 1. A mutant form of the EGF receptor is found in many glioblastomas, breast, lung and ovarian cancers. D. Bigner (Duke University) has made MAbs that recognize only the mutant receptor. Chemical conjugates of these with PE are cytotoxic to cells with mutant receptors but have low activity. Recombinant ITs with high activity could not be produced from these MAbs. Antibody phage display was used to generate a new antibody that produces a very stable and active recombinant IT which is being evaluated for clinical use. 2. Prostate cancer: MAb E4 reacts with normal prostate cells and differentiated prostate cancers. It has reactivity with other normal tissues. It has been chemically coupled to mutant PE (PE35) to make an IT that is very cytotoxic to prostate carcinoma cell lines. The genes of this antibody are being cloned to make a recombinant IT. 3. Melanoma: Melanomas and melanocytes contain a form of the MSH receptor (MCS-1) that is not present in other tissues. We are preparing antibodies to MCS-1 to examine their possible usefulness as ITs 4. Ovarian cancer: Most ovarian cancers and mesotheliomas contain a protein termed mesothelin. We are developing high affinity antibodies to mesothelin which can be used to direct toxins (or other cytotoxic agents) to these cells. We have cloned the mesothelin cDNA and created tumors that express large amounts of mesothelin. These tumors are used to evaluate targeted therapies with antibodies directed at mesothelin. Using phage display, new antibodies to mesothelin have been identified. 5. Epithelial tumors: LMB-1 has produced several clinical responses but it damages capillaries because its large size retards its exit from the circulation. LMB-7 is much smaller and damages epithelial cells of the stomach, because it rapidly leaves the circulation. We are constructing several ITs of different sizes with the goal of finding a size which will allow the IT to escape from the circulation into tumors, but will restrict access to stomach epithelial cells. We have designed ITs that do not require proteolytic processing by inserting a dsFv fragment either between domains II and III or at the end of domain III prior to the REDLK sequence, and two very active ITs were made with Fv fragments of MAbs B1 and e23 (anti-erbB2).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Intramural Research (Z01)
Project #
1Z01BC008753-14
Application #
2463748
Study Section
Special Emphasis Panel (LMB)
Project Start
Project End
Budget Start
Budget End
Support Year
14
Fiscal Year
1996
Total Cost
Indirect Cost

  Institution

Name
National Cancer Institute Division of Basic Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Kaplan, Gilad; Mazor, Ronit; Lee, Fred et al. (2018) Improving the In Vivo Efficacy of an Anti-Tac (CD25) Immunotoxin by Pseudomonas Exotoxin A Domain II Engineering. Mol Cancer Ther 17:1486-1493
Shancer, Zoe; Williams, Matthew; Igelman, Austin et al. (2018) Preclinical development of anti-BCMA immunotoxins targeting multiple myeloma. Antib Ther 1:19-25
Mazor, Ronit; Addissie, Selamawit; Jang, Youjin et al. (2017) Role of HLA-DP in the Presentation of Epitopes from the Truncated Bacterial PE38 Immunotoxin. AAPS J 19:117-129
Mazor, Ronit; Kaplan, Gilad; Park, Dong et al. (2017) Rational design of low immunogenic anti CD25 recombinant immunotoxin for T cell malignancies by elimination of T cell epitopes in PE38. Cell Immunol 313:59-66
Bera, Tapan K; Onda, Masanori; Kreitman, Robert J et al. (2014) An improved recombinant Fab-immunotoxin targeting CD22 expressing malignancies. Leuk Res 38:1224-9
Sathyanarayana, Bangalore K; Hahn, Yoonsoo; Patankar, Manish S et al. (2009) Mesothelin, Stereocilin, and Otoancorin are predicted to have superhelical structures with ARM-type repeats. BMC Struct Biol 9:1
Ochiai, Hidenobu; Archer, Gary E; Herndon 2nd, James E et al. (2008) EGFRvIII-targeted immunotoxin induces antitumor immunity that is inhibited in the absence of CD4+ and CD8+ T cells. Cancer Immunol Immunother 57:115-21
Du, Xing; Beers, Richard; Fitzgerald, David J et al. (2008) Differential cellular internalization of anti-CD19 and -CD22 immunotoxins results in different cytotoxic activity. Cancer Res 68:6300-5
Du, Xing; Nagata, Satoshi; Ise, Tomoko et al. (2008) FCRL1 on chronic lymphocytic leukemia, hairy cell leukemia, and B-cell non-Hodgkin lymphoma as a target of immunotoxins. Blood 111:338-43
Epel, Malka; Carmi, Irit; Soueid-Baumgarten, Sharon et al. (2008) Targeting TARP, a novel breast and prostate tumor-associated antigen, with T cell receptor-like human recombinant antibodies. Eur J Immunol 38:1706-20

Showing the most recent 10 out of 52 publications