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Ampullary cancer of intestinal origin and duodenal cancer-A logical clinical and therapeutic subgroup in periampullary cancer 被引量:4
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作者 Manju D Chandrasegaram Anthony J Gill +4 位作者 Jas Samra Tim Price John Chen Jonathan Fawcett Neil D Merrett 《World Journal of Gastrointestinal Oncology》 SCIE CAS 2017年第10期407-415,共9页
Periampullary cancers include pancreatic, ampullary, biliary and duodenal cancers. At presentation, the majority of periampullary tumours have grown to involve the pancreas, bile duct, ampulla and duodenum. This can r... Periampullary cancers include pancreatic, ampullary, biliary and duodenal cancers. At presentation, the majority of periampullary tumours have grown to involve the pancreas, bile duct, ampulla and duodenum. This can result in difficulty in defining the primary site of origin in all but the smallest tumors due to anatomical proximity and architectural distortion. This has led to variation in the reported proportions of resected periampullary cancers. Pancreatic cancer is the most common cancer resected with a pancreaticoduodenectomy followed by ampullary(16%-50%), bile duct(5%-39%), and duodenal cancer(3%-17%). Patients with resected duodenal and ampullary cancers have a better reported median survival(29-47 mo and 22-54 mo) compared to pancreatic cancer(13-19 mo). The poorer survival with pancreatic cancer relates to differences in tumour characteristics such as a higher incidence of nodal, neural and vascular invasion. While small ampullary cancers can present early with biliary obstruction, pancreatic cancers need to reach a certain size before biliary obstruction ensues. This larger size at presentation contributes to a higher incidence of resection margin involvement in pancreatic cancer. Ampullary cancers can be subdivided into intestinal or pancreatobiliary subtype cancers with histomolecular staining. This avoids relying on histomorphology alone, as even some poorly differentiated cancers preserve the histomolecular profile of their mucosa of origin. Histomolecular profiling is superior to anatomic location in prognosticating survival. Ampullary cancers of intestinal subtype and duodenal cancers are similar in their intestinal origin and form a logical clinical and therapeutic subgroup of periampullary cancers. They respond to 5-FU based chemotherapeutic regimens such as capecitabine-oxaliplatin. Unlike pancreatic cancers, KRAS mutation occurs in only approximately a third of ampullary and duodenal cancers. Future clinical trials should group ampullary cancers of intestinal origin and duodenal cancers toge 展开更多
关键词 Periampullary cancer Pancreatobiliary subtype intestinal subtype Ampullary cancer Duodenal cancer Epidermal growth factor receptor Pancreatic cancer Chemotherapy PANCREATICODUODENECTOMY KRAS
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幽门螺杆菌相关性萎缩性胃炎分型与肠化关系 被引量:1
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作者 韩子岩 鲁重美 《山西临床医药》 1998年第5期294-296,共3页
目的:探讨幽门螺杆菌(HP)相关性萎缩性胃炎的分型与肠化类型(Ⅰ型和Ⅲ型)之间的关系,分析HP相关性萎缩性胃炎在肠化演变中的主要路径和作用。方法:137例萎缩性胃炎划分成A型、B型和AB型。Warthin-Stary... 目的:探讨幽门螺杆菌(HP)相关性萎缩性胃炎的分型与肠化类型(Ⅰ型和Ⅲ型)之间的关系,分析HP相关性萎缩性胃炎在肠化演变中的主要路径和作用。方法:137例萎缩性胃炎划分成A型、B型和AB型。Warthin-Stary染色判定HP。组化A1cianB1ue(PH2.5)/PAS/和PB/KOH/PAS做出小肠型肠化和结肠型肠化。胃镜及病理诊断萎缩性胃炎。资料处理采用了“病例对照研究”的病因学方法。结果:萎缩性胃炎AB型与HP显著相关(OR=4.3,95%CI=1.9~9.5),联系强度“强”。萎缩性胃炎B型与HP相关(OR=2.1,95%CI=1.0~4.1),联系强度“中等”。萎缩性胃炎三型中,AB型HP感染率最高达77.8%,B型次之,为62.5%;三型差异显著(P<0.05)。HP相关性萎缩性胃炎AB型结肠型肠化发生率显著高于B型(63.6%,21.4%,P<0.05)。结论:AB型萎缩性胃炎的发生与HP感染密切相关并伴有高发的结肠型肠化,应视为萎缩性胃炎在肠化演变中的主导途径和防治对象。 展开更多
关键词 幽门螺杆菌 萎缩性胃炎 肠化 分型
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