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人类椎间盘老化与退变的分析。手术标本与正常对照的比较。

Analysis of aging and degeneration of the human intervertebral disc. Comparison of surgical specimens with normal controls.

作者信息

Gruber H E, Hanley E N

机构信息

Department of Orthopaedic Surgery, Carolinas Medical Center, Charlotte, North Carolina, USA.

出版信息

Spine (Phila Pa 1976). 1998 Apr 1;23(7):751-7. doi: 10.1097/00007632-199804010-00001.

Abstract

STUDY DESIGN

A prospective analysis of 33 control and 39 surgical human lumbar disc specimens from the anulus was undertaken to assess disc cell extracellular matrix production and cell function. The authors of this study analyzed immunohistochemical distributions of Types I, II, III and VI collagen, in situ localization of apoptotic disc cells, and tartrate-resistant acid phosphatase localization.

OBJECTIVES

To quantify the incidence of apoptotic cell death in the anulus; examine the collagen distribution in the pericellular, territorial, and interterritorial matrix; examine matrix cell degeneration; and compare diseased tissue with normal tissue from control individuals.

SUMMARY OF THE BACKGROUND DATA

Previous studies of disc histopathology have focused on extracellular matrix morphology and on biochemical synthetic and degenerative changes, but little is understood about the cell populations within the disc that are responsible for these changes.

METHODS

In this study light microscopy, immunohistochemistry, enzyme histochemistry, and in situ hybridization were used to examine 33 patient and 39 control specimens of human anulus obtained either via surgical procedures or from donors to the Cooperative Human Tissue Network.

RESULTS

The high incidence of apoptotic cell death was significantly greater in the control group (73.1 +/- 5.1% [mean +/- SEM]; n = 20) than among surgical specimens (53.5 +/- 5.6%; n = 20; P < 0.001); this was probably a result of the significantly greater average age in the control population (57.2 +/- 3.1 years) compared with that in the patient population (44.3 +/- 3.2 years; P < 0.001). Immunohistochemistry yielded findings that led to an expanded appreciation of the greatly modified extracellular domains that surrounded disc cells during aging and degeneration in both study groups. Enzyme histochemistry revealed the presence of tartrate-resistant acid phosphatase activity in human disc cells.

CONCLUSIONS

These findings reveal that there is a high incidence of apoptosis in the intervertebral disc. Surviving cells are not synthetically inactive but are, rather, producing inappropriate matrix products during aging and degeneration. In certain instances it appears that the matrix surrounding the cell may form an isolation barrier, which may influence individual cell activity and intercellular communication. These results point to the need to 1) more fully understand the cause of disc cell death via apoptosis and to determine whether this programmed cell death can be reversed or halted, and 2) more fully understand the dynamic relation between disc cells and the surrounding extracellular matrix, which they produce and remodel. The factors regulating extracellular matrix-disc cell homeostasis in the disc are unknown, as is the relation between extracellular matrix and disc cell functional modulation. The morphologic findings of this study suggest that these issues are important considerations in disc cell biology. The identification of tartrate-resistant acid phosphatase activity in disc cells allows for a new area of study of disc extracellular matrix remodelling. In summary, these new perspectives provide new parameters with which to assess disc cell health and function.

摘要

研究设计

对33个对照和39个手术获取的人腰椎间盘纤维环标本进行前瞻性分析,以评估椎间盘细胞外基质的产生及细胞功能。本研究的作者分析了I、II、III和VI型胶原的免疫组化分布、凋亡椎间盘细胞的原位定位以及抗酒石酸酸性磷酸酶的定位。

目的

量化纤维环中凋亡细胞死亡的发生率;检查周细胞、区域和区域间基质中的胶原分布;检查基质细胞退变情况;并将患病组织与对照个体的正常组织进行比较。

背景资料总结

以往关于椎间盘组织病理学的研究主要集中在细胞外基质形态以及生化合成和退变变化方面,但对于椎间盘内导致这些变化的细胞群体了解甚少。

方法

在本研究中,使用光学显微镜、免疫组化、酶组织化学和原位杂交技术,对通过手术程序或从合作人体组织网络的供体获取的33例患者和39个对照的人纤维环标本进行检查。

结果

对照组(73.1±5.1%[均值±标准误];n = 20)凋亡细胞死亡的发生率显著高于手术标本组(53.5±5.6%;n = 20;P < 0.001);这可能是由于对照人群的平均年龄(57.2±3.1岁)显著高于患者人群(44.3±3.2岁;P < 0.001)。免疫组化结果使人们对两个研究组中衰老和退变过程中围绕椎间盘细胞的细胞外区域的巨大改变有了更深入的认识。酶组织化学显示人椎间盘细胞中存在抗酒石酸酸性磷酸酶活性。

结论

这些发现表明椎间盘凋亡发生率很高。存活细胞并非合成无活性,而是在衰老和退变过程中产生不适当的基质产物。在某些情况下,细胞周围的基质似乎形成了一个隔离屏障,这可能会影响单个细胞的活性和细胞间通讯。这些结果表明需要:1)更全面地了解通过凋亡导致椎间盘细胞死亡的原因,并确定这种程序性细胞死亡是否可以逆转或停止;2)更全面地了解椎间盘细胞与其产生和重塑的周围细胞外基质之间的动态关系。调节椎间盘细胞外基质 - 椎间盘细胞稳态的因素尚不清楚,细胞外基质与椎间盘细胞功能调节之间的关系也不清楚。本研究的形态学发现表明这些问题是椎间盘细胞生物学中的重要考虑因素。在椎间盘细胞中鉴定出抗酒石酸酸性磷酸酶活性为椎间盘细胞外基质重塑研究开辟了一个新领域。总之,这些新观点提供了评估椎间盘细胞健康和功能的新参数。

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