Fucosylated haptoglobin is a novel marker for pancreatic cancer: A detailed analysis of the oligosaccharide structure and a possible mechanism for fucosylation

Noriko Okuyama(Zero to Three), Yoshihito Ide(Zero to Three), Miyako Nakano(The University of Osaka), Tsutomu Nakagawa(The University of Osaka), K Yamanaka(The University of Osaka), Kenta Moriwaki(The University of Osaka), Kohei Murata(Osaka International Cancer Institute), Hiroaki Ohigashi(Osaka International Cancer Institute), Shigekazu Yokoyama(Osaka International Cancer Institute), Hidetoshi Eguchi(Osaka International Cancer Institute), Osamu Ishikawa(Osaka International Cancer Institute), Toshifumi Ito(Kansai Rosai Hospital), Michio Kato(Osaka National Hospital), Akinori Kasahara(The University of Osaka), Sunao Kawano(The University of Osaka), Jianguo Gu(The University of Osaka), Naoyuki Taniguchi(The University of Osaka), Eiji Miyoshi(The University of Osaka)
International Journal of Cancer
December 29, 2005
Cited by 292

Abstract

Changes in oligosaccharide structures have been reported in certain types of malignant transformations and, thus, could be used for tumor markers in certain types of cancer. In the case of pancreatic cancer cell lines, a variety of fucosylated proteins are secreted into their conditioned media. To identify fucosylated proteins in the serum of patients with pancreatic cancer, we performed western blot analyses using Aleuria Aurantica Lectin (AAL), which is specific for fucosylated structures. An approximately 40 kD protein was found to be highly fucosylated in pancreatic cancer and an N-terminal analysis revealed that it was the beta chain of haptoglobin. While the appearance of fucosylated haptoglobin has been reported in other diseases such as hepatocellular carcinoma, liver cirrhosis, gastric cancer and colon cancer, the incidence was significantly higher in the case of pancreatic cancer. Fucosylated haptoglobin was observed more frequently at the advanced stage of pancreatic cancer and disappeared after an operation. A mass spectrometry analysis of haptoglobin purified from the serum of patients with pancreatic cancer and the medium from a pancreatic cancer cell line, PSN-1, showed that the alpha 1-3/alpha 1-4/alpha 1-6 fucosylation of haptoglobin was increased in pancreatic cancer. When a hepatoma cell line, Hep3B, was cultured with the conditioned media from pancreatic cancer cells, haptoglobin secretion was dramatically increased. These findings suggest that fucosylated haptoglobin could serve as a novel marker for pancreatic cancer. Two possibilities were considered in terms of the fucosylation of haptoglobin. One is that pancreatic cancer cells, themselves, produce fucosylated haptoglobin; the other is that pancreatic cancer produces a factor, which induces the production of fucosylated haptoglobin in the liver.


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