Display options
Cite
Lakshmikesari A, Radhakrishna R, Bhanumathi A, et al. Expression of epidermal and transforming growth factors in pancreatic cancer. Oncol Rep. 1996;3(5):963-6doi: 10.3892/or.3.5.963.
Lakshmikesari, A., Radhakrishna, R., Bhanumathi, A., Ravi, D., Srinivas, G., Nair, M., & Pillai, M. (1996). Expression of epidermal and transforming growth factors in pancreatic cancer. Oncology reports, 3(5), 963-6. https://doi.org/10.3892/or.3.5.963
Lakshmikesari, A, et al. "Expression of epidermal and transforming growth factors in pancreatic cancer." Oncology reports vol. 3,5 (1996): 963-6. doi: https://doi.org/10.3892/or.3.5.963
Lakshmikesari A, Radhakrishna R, Bhanumathi A, Ravi D, Srinivas G, Nair M, Pillai M. Expression of epidermal and transforming growth factors in pancreatic cancer. Oncol Rep. 1996 Sep;3(5):963-6. doi: 10.3892/or.3.5.963. PMID: 21594491.
Copy Download .nbib Format: NLM
Share it on

Oncol Rep. 1996 Sep;3(5):963-6. doi: 10.3892/or.3.5.963.

Expression of epidermal and transforming growth factors in pancreatic cancer.

Oncology reports

A Lakshmikesari, R Radhakrishna, A Bhanumathi, D Ravi, G Srinivas, M Nair, M Pillai

Affiliations

  1. REG CANC CTR,DIV LAB MED,TRIVANDRUM 695011,KERALA,INDIA. REG CANC CTR,DIV RADIAT ONCOL,TRIVANDRUM 695011,KERALA,INDIA. MED COLL HOSP,DEPT PATHOL,THANJAVUR,TAMIL NADU,INDIA.

PMID: 21594491 DOI: 10.3892/or.3.5.963

Abstract

Pancreatic cancer continues to be a major clinical problem and little is known of the various cellular and molecular events associated with this malignancy. Growth factors and their receptors have important functions in the process of tumor progression. We have examined by immunocytochemistry, the expression of epidermal growth factor (EGF), its receptor (EGFR) and the transforming growth factors alpha and beta (TGF alpha and beta) in various grades of pancreatic adenocarcinoma. Expression of the growth factors was compared to their distribution in apparently normal pancreas and chronic pancreatitis. EGF, TGF alpha and TGF beta was expressed in normal pancreatic tissue while the expression of EGFR was slight and restricted. In chronic pancreatitis, this expression of EGFR increased and was found to be moderate in intensity. Expression of EGF, TGF alpha and TGF beta was similar to that seen in normal pancreas. Moderate to intense expression of EGF and TGF alpha was evident in all grades of pancreatic cancer. Expression of EGFR was intense in all these lesions. However, the most significant finding was the absence of TGF beta in all pancreatic cancer lesions. These results may have significant implications for pancreatic tumor progression. EGF and TGF alpha are growth promoters influencing the expression of EGFR. TGF beta, on the other hand exerts an anti-proliferative effect and favours differentiation. It therefore appears that the balance between EGF and TGF alpha on the one hand and TGF beta on the other may be critical in the process of tumor progression, especially if one considers chronic pancreatitis as a pre-malignant condition and the growth factor expression associated with it.

Publication Types