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1 ifying the pancreatic cancer as a functional glucagonoma.
2 nesium responsiveness of NIPAL1 in alpha-TC6 glucagonoma cells (a pancreatic alpha-cell line) were si
3 tryptic fragments derived from insulinoma or glucagonoma cells, blocks the immunoprecipitation of bot
4           Recently, we identified Insulinoma-Glucagonoma clone 20 (IG20) that can render cells more s
5 of the thyroid, and 1 each had a gastrinoma, glucagonoma, fibrolamellar cancer, and malignant histioc
6 y diarrhea, hypokalemia-achlorhydria [WDHA], glucagonoma [glucagonoma syndrome], and so forth).
7 rately successful, with minimal evidence for glucagonomas or metastatic spread.
8                                           In glucagonoma patients, amino acid turnover and ureagenesi
9 oss, as reflected by the wasting observed in glucagonoma patients.
10 imens, death-domain adaptor protein Insuloma-Glucagonoma protein 20 (IG20) is consistently aberrantly
11 ypokalemia-achlorhydria [WDHA], glucagonoma [glucagonoma syndrome], and so forth).
12  In patients with glucagon-producing tumors (glucagonomas), the most conspicuous signs are skin lesio