混合型肝细胞癌-胆管癌临床病理特征分析

摘要/Abstract

摘要： 目的分析82例混合型肝细胞癌-胆管癌(cHCC-CCA)临床病理特征。方法回顾性分析82例cHCC-CCA患者病历资料,同时纳入同时期HCC患者50例、CCA患者30例,比较三组一般临床资料、病理资料,同时分析cHCC-CCA镜下病理表现。结果 CCA组发病年龄、AFP水平为(57.1±8.2)岁、(312.0±37.4)U/mL,分别与cHCC-CCA[(52.6±6.7)岁、(364.3±35.2)U/mL]、HCC[(53.0±7.0)岁、(382.4±44.9)U/mL]比,差异有统计学意义(P<0.05),而cHCC-CCA与HCC相比,发病年龄、AFP水平差异无统计学意义(P>0.05)。cHCC-CCA、HCC患者合并HBV感染为63例(76.8%)、46例(92.0%),均显著高于CCA患者[11例(36.7%),P<0.05],而cHCC-CCA、HCC患者差异无统计学意义(P>0.05)。HCC组肿瘤直径、低分化病例为(4.6±1.2)cm、42例(84.0%),分别与cHCC-CCA[(5.7±1.4)cm、51例(62.2%)]、CCA[(5.5±1.6)cm、19例(63.3%)]比,差异有统计学意义(P<0.05),而cHCC-CCA与HCC肿瘤直径、低分化病例比较差异无统计学意义(P>0.05)。CCA组肝硬化、淋巴结转移为7例(23.3%)、11例(36.7%),分别与cHCC-CCA[56例(68.3%)、7例(8.5%)]、HCC[41例(82.0%)、3例(6.0%)]比,差异有统计学意义(P<0.05),而cHCC-CCA与HCC肝硬化、淋巴结转移比较无统计学意义(P>0.05)。cHCC-CCA镜下包括HCC(80例,97.6%)、CCA(78例,95.1%)两种区域,HCC区域镜下表现为粗小梁索状和假腺样结构,组织呈肝细胞样分化,内含丰富嗜酸性胞质,细胞核呈圆形。CCA区域见中低分化异型腺体排列成不规则腺管状和实性条索结构,伴间质纤维组织增生。另有11例(13.4%)组织中存在细胆管癌(CLC)区域,镜下表现为腺体呈狭小腔隙状和“鹿角状”生长方式,伴显著间质纤维组织增生,细胞体积较小,胞质稀少呈嗜碱性,细胞核呈卵圆形,腺体周围富含透明间质。结论 cHCC-CCA与HCC、CCA患者在临床病理特征方面既存在着相同点,也有着差异,关注cHCC-CCA镜下HCC、CCA成分的构成比例可能会为临床诊治cHCC-CCA提供科学依据。

关键词: 混合型肝细胞癌-胆管癌, 肝细胞癌, 胆管癌, 细胆管癌

Abstract: Objective The clinicopathological features of 82 cases of combined hepatocellular-cholangiocarcinoma (cHCC-CCA) were analyzed. Methods The medical records of 82 cases with cHCC-CCA were analyzed retrospectively, including 50 HCC patients and 30 CCA patients in the same period. The general clinical data and pathological data of the three groups were compared, and the pathological manifestations under cHCC-CCA microscope were analyzed. Results The onset age and AFP level in CCA group were (57.1±8.2) years old and (312.0±37.4) U/mL, and the differences were statistically significant (P<0.05) when compared with cHCC-CCA [(52.6±6.7) years old, (364.3±35.2) U/mL] and HCC [(53.0±7.0) years old, (382.4±44.9) U/mL]. However, there was no significant difference among cHCC-CCA, HCC onset age and AFP level (P>0.05). HBV infection was found in 63 patients (76.8%) with cHCC-CCA and 46 patients (92.0%) with HCC. They were significantly higher than those of CCA patients [11 cases (36.7%), P<0.05], but there was no significant difference between cHCC-CCA and HCC patients (P>0.05). In HCC group, the tumor diameter and poorly differentiated cases were (4.6±1.2)cm and 42 cases (84.0%), the difference was statistically significant (P<0.05) when compared with cHCC-CCA [(5.7±1.4) cm, 51 cases (62.2%)] and CCA [(5.5±1.6) cm, 19 cases (63.3%)]. However, there was no significant difference in tumor diameter and poorly differentiated cases between cHCC-CCA and HCC (P>0.05). In CCA group, there were 7 cases (23.3%) of cirrhosis and 11 cases (36.7%) of lymph node metastasis. Compared with cHCC-CCA [56 cases (68.3%), 7 cases (8.5%)] and HCC [41 cases (82.0%), 3 cases (6.0%)], the difference was statistically significant (P<0.05). However, there was no statistically significant difference (P>0.05) in the cases of cirrhosis and lymph node metastasis between cHCC-CCA group and HCC group. Under the microscope of cHCC-CCA, HCC(80 cases, 97.6%) and CCA(78 cases, 95.1%) were included. The HCC region showed thick trabecular cord-like and pseudoglandular structures under the microscope, with hepatocyte-like differentiation and rich eosinophilic cytoplasm, and the nucleus was round. In the CCA region, the moderately and poorly differentiated atypical glands were arranged in irregular glandular tubular and solid cord structures, accompanied by interstitial fiber tissue. In another 11 cases (13.4%), there was a cholangiolocellular carcinoma (CLC) region in the tissues. Microscopically, the glands showed a narrow cavity-like and "staghorn" growth pattern, accompanied by obvious interstitial fibrous tissue proliferation. The cells were small, the cytoplasm was sparse and basophilic, the nucleus was oval, and transparent stroma was abundant around the glands. Conclusion There are similarities and differences in clinicopathological features among the cHCC-CCA and HCC and CCA patients. Paying attention to the composition ratio of HCC and CCA under cHCC-CCA microscope may provide scientific basis for clinical diagnosis and treatment of cHCC-CCA.

Key words: Combined hepatocellular-cholangiocarcinoma, Hepatocellular carcinoma, Cholangiocarcinoma, Cholangiolocellular carcinoma

聂熹, 吴肖洁, 桂仁捷, 段华新. 混合型肝细胞癌-胆管癌临床病理特征分析[J]. 肝脏, 2025, 30(11): 1507-1510.

NIE Xi, WU Xiao-jie, GUI Ren-jie, DUAN Hua-xin. Clinicopathological characteristics of combined hepatocellular-cholangiocarcinoma[J]. Chinese Hepatolgy, 2025, 30(11): 1507-1510.

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