AI Article Synopsis
- The study focuses on developing a monoclonal antibody (HPC2 1-B3) to differentiate pancreatic ductal adenocarcinoma and precancerous lesions from benign tissues.
- During tests, this antibody effectively identified cancerous and precancerous tissue in various pancreatic biopsy samples while showing no positivity in chronic pancreatitis cases.
- Findings suggest that HPC2 1-B3 could improve early detection of pancreatic dysplasia, potentially reducing pancreatic cancer mortality through better screening methods.
Article Abstract
BACKGROUND.: Pancreatic ductal adenocarcinoma is rarely detected early enough for patients to be cured. The objective of the authors was to develop a monoclonal antibody to distinguish adenocarcinoma and precancerous intraductal papillary mucinous neoplasia (IPMN) from benign epithelium. METHODS.: Mice were immunized with human pancreatic adenocarcinoma cells and monoclonal antibodies were screened against a panel of archived pancreatic tissue sections, including pancreatitis (23 cases), grade 1 IPMN (16 cases), grade 2 IPMN (9 cases), grade 3 IPMN (13 cases), and various grades of adenocarcinoma (17 cases). One monoclonal antibody, human pancreatic cancer fusion 2 (HPC2) 1-B3, which specifically immunostained adenocarcinoma and all grades of IPMN, was isolated. Subsequently, HPC2 1-B3 was evaluated in a retrospective series of 31 fine-needle aspiration (FNA) biopsies from clinically suspicious pancreatic lesions that had long-term clinical follow-up. RESULTS.: HPC2 1-B3 was negative in all 31 cases of chronic pancreatitis that were tested. In contrast, HPC2 1-B3 immunostained the cytoplasm and luminal surface of all 16 well- to moderately differentiated pancreatic ductal adenocarcinomas. It demonstrated only weak focal staining of poorly differentiated carcinomas. All high-grade IPMNs were found to be positive for HPC2 1-B3. The majority of low-grade to intermediate-grade IPMNs were positive (66% of cases). Immunostaining a separate series of pancreatic FNA cell blocks for HPC2 1-B3 demonstrated that the relative risk for detecting at least low-grade dysplasia (2.0 [95% confidence interval, 1.23-3.26]) was statistically significant (P = .002 by the Fisher exact test). CONCLUSIONS.: To reduce the mortality of pancreatic cancer, more effective early screening methods are necessary. The data from the current study indicate that a novel monoclonal antibody, HPC2 1-B3, may facilitate the diagnosis of early pancreatic dysplasia.
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|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3524386 | PMC |
| http://dx.doi.org/10.1002/cncy.21223 | DOI Listing |
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Human pancreatic cancer fusion 2 (HPC2) 1-B3: a novel monoclonal antibody to screen for pancreatic ductal dysplasia.
Cancer Cytopathol
January 2013
Department of Pathology, Oregon Health and Science University, Portland, Oregon 97239, USA.
Article Synopsis
- The study focuses on developing a monoclonal antibody (HPC2 1-B3) to differentiate pancreatic ductal adenocarcinoma and precancerous lesions from benign tissues.
- During tests, this antibody effectively identified cancerous and precancerous tissue in various pancreatic biopsy samples while showing no positivity in chronic pancreatitis cases.
- Findings suggest that HPC2 1-B3 could improve early detection of pancreatic dysplasia, potentially reducing pancreatic cancer mortality through better screening methods.
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