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在特发性炎症性肠病中,乳腺丝抑蛋白的异常表达与疾病活动及肿瘤转化相关。

Aberrant expression of maspin in idiopathic inflammatory bowel disease is associated with disease activity and neoplastic transformation.

作者信息

Cao Dengfeng, Wilentz Robb E, Abbruzzese James L, Ho Linus, Maitra Anirban

机构信息

Department of Pathology, The Johns Hopkins Hospital, Baltimore, Maryland 21231, USA.

出版信息

Int J Gastrointest Cancer. 2005;36(1):39-46. doi: 10.1385/IJGC:36:1:039.

Abstract

BACKGROUND

Maspin is both overexpressed in tumors and inflammation, implicating a possible role in bridging inflammation and neoplasia. Idiopathic inflammatory bowel disease (IBD) and IBD-associated dysplasias and carcinomas represent a prototype for studying the relationship between chronic inflammatory states and neoplasia.

AIM OF STUDY

To investigate expression of maspin in IBD and IBD-associated dysplasia and colorectal carcinoma.

METHODS

Immunohistochemical labeling of maspin was examined using tissue microarrays constructed from archival biopsy and resection tissue from 90 patients with 125 histologically defined lesions including 30 with inactive chronic IBD, 51 with active chronic IBD, 4 IBD-associated foci with epithelial changes indefinite for dysplasia (IFD), 7 with IBD-associated low-grade epithelial dysplasia (LGD), 8 with IBD-associated high grade epithelial dysplasia (HGD), and 25 with IBD-associated invasive colorectal adenocarcinomas.

RESULTS

Maspin was expressed in 47/51 (92%) active chronic IBD lesions, which was significantly higher than both inactive chronic IBD (13/30, 43%) and normal mucosa (1 of 9, 11%) (p < 0.01); in particular, the diffuse pattern of maspin expression was significantly higher in active IBD (41/51, 80%), compared with inactive IBD (5/30, 17%) and normal mucosa (0%) (p < 0.01). In the multistage progression model of colitis-associated neoplasia, aberrant labeling was observed at the earliest stages, with 3/4 (75%) IFD foci, 6/7 (86%) LGD, and 8/8 (100%) HGD specimens expressing maspin, virtually always in a diffuse pattern. Expectedly, 22/25 (88%) of invasive IBD-associated cancers overexpressed maspin, including 21 with diffuse labeling.

CONCLUSIONS

Maspin is significantly overexpressed in both active IBD and colitis-associated dysplasia compared to either inactive IBD or normal colonic mucosa, suggesting a potential role in disease "flare" as well as neoplastic progression. Targeting maspin for control of disease activity and cancer prophylaxis may be a promising novel therapeutic strategy for IBD.

摘要

背景

抑癌蛋白Maspin在肿瘤和炎症中均有过表达,这暗示其在连接炎症和肿瘤形成过程中可能发挥作用。特发性炎症性肠病(IBD)以及IBD相关的发育异常和癌代表了研究慢性炎症状态与肿瘤形成之间关系的一个范例。

研究目的

研究Maspin在IBD、IBD相关发育异常及结直肠癌中的表达情况。

方法

使用组织芯片对Maspin进行免疫组化标记检测,该组织芯片由90例患者的存档活检及切除组织构建而成,包含125个组织学定义的病变,其中30例为非活动性慢性IBD,51例为活动性慢性IBD,4例IBD相关上皮改变不明确的发育异常灶(IFD),7例IBD相关低级别上皮发育异常(LGD),8例IBD相关高级别上皮发育异常(HGD),以及25例IBD相关浸润性结直肠癌。

结果

Maspin在51例活动性慢性IBD病变中的47例(92%)中表达,这显著高于非活动性慢性IBD(30例中的13例,43%)和正常黏膜(9例中的1例,11%)(p<0.01);特别是,Maspin表达的弥漫模式在活动性IBD中显著更高(41/51,80%),相比之下非活动性IBD(5/30,17%)和正常黏膜(0%)(p<0.01)。在结肠炎相关肿瘤的多阶段进展模型中,在最早阶段就观察到异常标记,3/4(75%)的IFD灶、6/7(86%)的LGD和8/8(100%)的HGD标本表达Maspin,几乎都是弥漫模式。不出所料,25例IBD相关浸润性癌中的22例(88%)过表达Maspin,其中21例为弥漫性标记。

结论

与非活动性IBD或正常结肠黏膜相比,Maspin在活动性IBD和结肠炎相关发育异常中均显著过表达,提示其在疾病“发作”以及肿瘤进展中可能发挥作用。针对Maspin来控制疾病活动和预防癌症可能是一种有前景的IBD新型治疗策略。

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