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用于靶向人髓核细胞的细胞表面特异性标志物的鉴定:碳酸酐酶XII的表达随年龄和退变而变化。

Identification of cell surface-specific markers to target human nucleus pulposus cells: expression of carbonic anhydrase XII varies with age and degeneration.

作者信息

Power Karen A, Grad Sibylle, Rutges Joost P H J, Creemers Laura B, van Rijen Mattie H P, O'Gaora Peadar, Wall J Gerard, Alini Mauro, Pandit Abhay, Gallagher William M

机构信息

University College Dublin, Dublin, Ireland.

出版信息

Arthritis Rheum. 2011 Dec;63(12):3876-86. doi: 10.1002/art.30607.

Abstract

OBJECTIVE

Back pain is a major cause of disability, affecting millions of people worldwide. One cause of axial back pain is degeneration of the nucleus pulposus (NP) of the intervertebral disc. This study was undertaken to investigate associations of NP cells with cell surface-specific proteins that differ from proteins in closely related cell types, i.e., intervertebral disc anulus fibrosus (AF) cells and articular cartilage (AC) chondrocytes, in order to identify potential surface molecules for directed delivery of therapeutic agents.

METHODS

We conducted a complementary DNA microarray analysis of 16 human samples from 6 donors, followed by gene list reduction using a systematic approach. Genes that were more highly expressed in NP than AC cells, contained transmembrane domains, and appeared attractive for targeting were assessed by quantitative reverse transcription-polymerase chain reaction (RT-PCR). As a viable candidate, carbonic anhydrase XII (CAXII) was analyzed at the protein level by immunohistochemistry and functional study.

RESULTS

Microarray results demonstrated a clear divide between the AC and AF and between the AC and NP samples. However, the transcriptomic profile of AF and NP samples displayed a greater intersubject similarity. Of the 552 genes with up-regulated expression in NP cells, 90 contained transmembrane domains, and 28 were quantified by RT-PCR. Most intense CAXII labeling was observed in the NP of discs from young subjects and in degenerative tissue.

CONCLUSION

CAXII may be considered for detection or targeting of degenerating disc cells. Furthermore, CAXII may be involved in pH regulation of NP cells. Its potential for directed delivery of regenerative factors and its functional role in NP cell homeostasis warrant further investigation.

摘要

目的

背痛是导致残疾的主要原因,影响着全球数百万人。椎间盘髓核(NP)退变是轴向背痛的一个原因。本研究旨在调查NP细胞与细胞表面特异性蛋白之间的关联,这些蛋白不同于密切相关细胞类型中的蛋白,即椎间盘纤维环(AF)细胞和关节软骨(AC)软骨细胞,以确定用于治疗剂定向递送的潜在表面分子。

方法

我们对来自6名供体的16个人类样本进行了互补DNA微阵列分析,随后采用系统方法减少基因列表。通过定量逆转录-聚合酶链反应(RT-PCR)评估在NP中比AC细胞表达更高、含有跨膜结构域且看起来有靶向吸引力的基因。作为一个可行的候选基因,通过免疫组织化学和功能研究在蛋白质水平分析碳酸酐酶XII(CAXII)。

结果

微阵列结果显示AC与AF之间以及AC与NP样本之间有明显区分。然而,AF和NP样本的转录组谱显示出更大的个体间相似性。在NP细胞中表达上调的552个基因中,90个含有跨膜结构域,28个通过RT-PCR进行了定量分析。在年轻受试者椎间盘的NP和退变组织中观察到最强的CAXII标记。

结论

CAXII可考虑用于退变椎间盘细胞的检测或靶向。此外,CAXII可能参与NP细胞的pH调节。其在再生因子定向递送方面的潜力及其在NP细胞内环境稳定中的功能作用值得进一步研究。

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