111In/125/131I-Labeled anti-mucin-1 murine, chimeric or humanized antibody hPAM4
- PMID: 21834178
- Bookshelf ID: NBK57127
111In/125/131I-Labeled anti-mucin-1 murine, chimeric or humanized antibody hPAM4
Excerpt
Mucins (MUC) are a distinct class of transmembrane glycoproteins (designated as MUC1, MUC3A, MUC3B, MUC4, etc.) that are expressed primarily by the glandular and ductal cells of the epithelium in the human body and are known to modulate the tumorigenicity, progression, and pathogenesis of different cancers (1). The structure, physiological function, and process of promoting the development of malignancies by MUCs, particularly MUC1 and MUC4, are discussed in detail by Bafna et al. (1). MUC1 has been shown to be characteristically overexpressed by pancreatic
The majority of individuals suffering from PAC do not survive for more than 1 year after diagnosis, and <1% of these patients live beyond 5 years (5). Although surgical resection of the cancer is a possible treatment for this disease, only 10%–25% of the patients are considered suitable for this treatment because, by the time that the neoplasm is detected, the malignancy has metastasized and the tumor load in the patient is too high to warrant surgery (5). Patients with nonresectable PAC are treated either with
More than a decade ago, a 131I-labeled murine monoclonal antibody, PAM4 ([131I]-mPAM4), directed against a mucin (later identified to be MUC1 (5)) was reported to detect human xenograft PAC tumors in mice with high specificity and, compared to controls, significantly extended the survival time of the animals when used for radiotherapy of the cancer (7-9). In a preliminary study, [131I]-PAM4 was demonstrated to detect the primary and the metastasized pancreatic carcinoma tumors in humans, and there was a low nonspecific uptake of the tracer in the liver, spleen, and bone marrow of the patients (10). In another study, a chimeric form of PAM4 (cPAM4) was labeled with 125I and 111In to obtain [125I]-cPAM4 and [111In]-cPAM4, respectively, and the biodistribution of these labeled mAbs was investigated in mice bearing human xenograft PAC tumors (11). Recently, Gulec et al. studied the biodistribution of 111In-labeled humanized PAM4 ( [111In]-hPAM4) in a phase I clinical trial (2).
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