Patterns of failure after curative resection of pancreatic carcinoma

Griffin, John F.; Smalley, Stephen R.; Jewell, William R.; Paradelo, Jorge C.; Reymond, Ralph D.; Hassanein, Ruth S.; Evans, Richard G.

doi:10.1002/1097-0142(19900701)66:1<56::aid-cncr2820660112>3.0.co;2-6

Cited by 404 publications

(188 citation statements)

References 17 publications

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“…It has also been reported that high doses of radiotherapy (55 Gy or greater) can improve local control in patients with pancreatic carcinoma, compared with radiotherapy at lower doses. 17 5-FU is used as a standard agent for chemoradiotherapy. When 5-FU is administered by bolus injection, it is essentially cleared from plasma in 1 hour.…”

mentioning

confidence: 99%

Intraoperative and conformal external‐beam radiation therapy with protracted 5‐fluorouracil infusion in patients with locally advanced pancreatic carcinoma

Furuse

Kinoshita

Kawashima

et al. 2003

Cancer

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mentioning

confidence: 99%

Intraoperative and conformal external‐beam radiation therapy with protracted 5‐fluorouracil infusion in patients with locally advanced pancreatic carcinoma

Furuse

Kinoshita

Kawashima

et al. 2003

Cancer

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“…2 Extended surgical resection, intensive chemotherapy, radiation therapy, or a combination of all 3 have been advocated in recent years, but none have prolonged patient survival significantly. New therapy for pancreatic cancer is needed.…”

Section: Discussionmentioning

confidence: 99%

“…1,2 The ability of tumor cells to degrade adjacent extracellular matrix is considered an essential step in the processes of invasion and metastasis. 3,4 Matrix metalloproteinases (MMPs) are a family of structurally related zymogens capable of degrading extracellular matrix, including basement membrane.…”

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confidence: 99%

Antitumor effect of a new selective matrix metalloproteinase inhibitor, MMI-166, on experimental pancreatic cancer

et al. 2001

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The antitumor effect of a new matrix metalloproteinase inhibitor, MMI-166, which is a selective inhibitor of MMP-2 and -9, was examined in the hamster pancreatic cancer cell line PGHAM-1. In vitro, MMI-166 inhibited the gelatinase activity of MMP-2 and -9 derived from PGHAM-1 cells, and dose-dependently inhibited invasion of PGHAM-1 through a basement membrane-like barrier. MMI-166 showed no apparent cytotoxicity to PGHAM-1 cells in culture at 100 g/ml. MMI-166 (200 mg/kg) or vehicle were administered orally, once daily, from day 1 until day 21 after implantation in the orthotopic implantation model of PGHAM-1. MMI-166 significantly reduced the incidence of liver surface metastasis from 66.7% to 20.0%, and it reduced the number of liver surface metastases per animal from 6.17 to 2.00, but this reduction was not significant. Key words: selective MMP inhibitor; pancreatic cancer; antitumor effectPancreatic cancer is characterized by extensive local invasion of adjacent structures, perineural invasion, early metastasis to liver and lymph nodes and a poor prognosis. 1,2 The ability of tumor cells to degrade adjacent extracellular matrix is considered an essential step in the processes of invasion and metastasis. 3,4 Matrix metalloproteinases (MMPs) are a family of structurally related zymogens capable of degrading extracellular matrix, including basement membrane. They are secreted by cancer cells and adjacent stromal cells in latent form and then converted into their active form. MMPs are crucial for tumor cell migration through the basement membrane and extracellular matrix, and for tumor cell intravasation and extravasation. 3,5 MMP-2-degrading type IV collagen, which is a main component of basement membranes, is expressed in pancreatic cancer 6 and plays an important role in invasion and metastasis. 7,8 MMPs also appear to be involved in angiogenesis, by mediating tissue remodeling and penetration of the extracellular matrix by activated endothelial cells. 4 Angiogenesis, which is essential for tumor growth and metastasis, is one of the important steps in the transition of tumors from small, harmless clusters of mutated cells to large, malignant growths, capable of spreading to other organs throughout the body. 9 When angiogenesis is blocked, tumor growth is suppressed, and tumor cell proliferation is balanced by apoptosis. 10 MMP-2 plays an especially important role in angiogenesis and tumor progression in some cancers. 11 Hamster pancreatic cancer cell line PGHAM-1 was derived from BOP (N-nitrosobis(2-oxopropyl)amine)-induced hamster pancreatic cancer cells as a result of repeated passage by subcutaneous implantation. It is a ductal adenocarcinoma that closely resembles human pancreatic carcinoma, and it often gives rise to liver metastasis shortly after implantation into the pancreas. [12][13][14] The PGHAM-1 cell line is useful for studying pancreatic cancer and liver metastasis by pancreatic cancer.Many studies have been conducted on the inhibitory effect of MMP inhibitors on invasion and metastasis in var...

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“…After 3 days, animals were killed and the livers were fixed with 2% formaldehyde in PBS (4°C). Tissues were cut evenly into three slices and incubated in a PBS solution containing 5 mm K 3 Fe(CN) 5 , 5 mm K 4 Fe(CN) 5 , 2 mm MgCl 2 , and 1 mg/ml of X-gal for 18 h at 37°C. 29 After staining, tissues were embedded in paraffin, sectioned, adhered to glass slides, and counter stained with hematoxylin and eosin.…”

Section: Liver Metastasis Modelmentioning

confidence: 99%

“…[1][2][3][4][5][6] In particular, liver metastasis frequently occurs (about 60%) after a surgical resection for pancreatic adenocarcinoma even if it is performed with a curative intent. 5 No effective therapeutic modality has been established to prevent liver metastasis or to treat it successfully. In human pancreatic cancer, point mutation of the c-K-ras protooncogene at codon 12/13 is frequently detected.…”

Section: Introductionmentioning

confidence: 99%

The dominant negative H-ras mutant, N116Y, suppresses growth of metastatic human pancreatic cancer cells in the liver of nude mice

et al. 2000

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In pancreatic cancer, the mutation of c-K-ras is a critical event of tumor growth and metastasis. We have previously demonstrated a dominant negative effect of N116Y on the growth of pancreatic cancer cells. To evaluate the potential of N116Y for suppressing the metastatic growth of pancreatic tumor cells, we made a replication-deficient recombinant N116Y adenovirus driven by the carcinoembryonic antigen (CEA) promoter (Ad CEA-N116Y). We demonstrated that the expression of N116Y, growth inhibition, and apoptotic death induction were all specific to pancreatic cancer cell lines (PCI-35 and PCI-43) that were promoter positive, whereas no growth retardation was observed in human embryonic pancreas-derived cell line 1C3D3 after Ad CEA-

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Patterns of failure after curative resection of pancreatic carcinoma

Cited by 404 publications

References 17 publications

Intraoperative and conformal external‐beam radiation therapy with protracted 5‐fluorouracil infusion in patients with locally advanced pancreatic carcinoma

Intraoperative and conformal external‐beam radiation therapy with protracted 5‐fluorouracil infusion in patients with locally advanced pancreatic carcinoma

Antitumor effect of a new selective matrix metalloproteinase inhibitor, MMI-166, on experimental pancreatic cancer

The dominant negative H-ras mutant, N116Y, suppresses growth of metastatic human pancreatic cancer cells in the liver of nude mice

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