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通过对特定疾病表型的成纤维细胞与组织活检进行比较分析,鉴定掌腱膜挛缩症中的生物标志物。

Identification of biomarkers in Dupuytren's disease by comparative analysis of fibroblasts versus tissue biopsies in disease-specific phenotypes.

作者信息

Shih Barbara, Wijeratne Dulharie, Armstrong Daniel J, Lindau Tommy, Day Philip, Bayat Ardeshir

机构信息

Plastic & Reconstructive Surgery Research, Manchester Interdisciplinary Biocentre, University of Manchester, Manchester, UK.

出版信息

J Hand Surg Am. 2009 Jan;34(1):124-36. doi: 10.1016/j.jhsa.2008.09.017.

Abstract

PURPOSE

Biomarkers are molecular mediators that can serve as indicators of normal biological processes, pathologic processes, and therapeutic interventions. This study aims to identify potential biomarkers in Dupuytren's disease (DD), a fibroproliferative benign tumor with an unknown etiology and high recurrence after surgery.

METHODS

Bioinformatic analytical techniques were employed to identify candidate genes that may be differentially expressed in DD, which included gene expression analysis of microarray data and thorough literature searches in genetic linkage and other related biomolecular studies. All DD cases were males with advanced DD (n = 5, 66 years +/- 14). RNA was extracted from biopsies and corresponding cultures of normal fascia (unaffected transverse palmar fascia), palmar nodule and cord from each patient. Real-time reverse transcription-polymerase chain reactions were performed to determine the gene expression levels for disease-related transcripts.

RESULTS

The bioinformatic analysis revealed 25 candidate genes, which were further short-listed to 6 genes via functional annotation. The 6 selected candidate genes included: A disintegrin and metalloproteinase domain (ADAM12), aldehyde dehydrogenase 1 family member (ALDH1) A1, Iroquois homeobox protein 6 (IRX6), proteoglycan 4 (PRG4), tenascin C (TNC), and periostin (POSTN). The culturing treatments were shown to have significant impact on the gene expression for ALDH1A1, PRG4, and TNC. In tissue biopsies, significant fold changes were observed for ADAM12, POSTN, and TNC in the cord and/or nodule when compared with that of normal fascia. ADAM12 and POSTN are associated with accelerated or abnormal cell growth, whereas TNC has been associated with fibrotic diseases and cell migration.

CONCLUSIONS

This study demonstrated differential gene expression results in DD tissue biopsies compared with that of their corresponding cultures. ADAM12, POSTN, and TNC were identified from the cord and nodule biopsy samples as potential biomarkers in relation to DD development.

摘要

目的

生物标志物是分子介质,可作为正常生物过程、病理过程和治疗干预的指标。本研究旨在确定掌腱膜挛缩症(DD)中的潜在生物标志物,这是一种病因不明且术后复发率高的纤维增生性良性肿瘤。

方法

采用生物信息分析技术来识别可能在DD中差异表达的候选基因,包括对微阵列数据进行基因表达分析以及在遗传连锁和其他相关生物分子研究中进行全面的文献检索。所有DD病例均为患有晚期DD的男性(n = 5,66岁±14岁)。从每位患者的活检组织以及相应的正常筋膜(未受影响的掌横筋膜)、掌结节和条索的培养物中提取RNA。进行实时逆转录-聚合酶链反应以确定疾病相关转录本的基因表达水平。

结果

生物信息分析揭示了25个候选基因,通过功能注释进一步筛选至6个基因。所选的6个候选基因包括:解整合素和金属蛋白酶结构域(ADAM12)、醛脱氢酶1家族成员(ALDH1)A1、腹直肌同源盒蛋白6(IRX6)、蛋白聚糖4(PRG4)、腱生蛋白C(TNC)和骨膜蛋白(POSTN)。培养处理显示对ALDH1A1、PRG4和TNC的基因表达有显著影响。在组织活检中,与正常筋膜相比,在条索和/或结节中观察到ADAM12、POSTN和TNC有显著的倍数变化。ADAM12和POSTN与细胞生长加速或异常有关,而TNC与纤维化疾病和细胞迁移有关。

结论

本研究表明,与相应培养物相比,DD组织活检中存在基因表达差异。从条索和结节活检样本中鉴定出ADAM12、POSTN和TNC作为与DD发展相关的潜在生物标志物。

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