在小鼠中对ADAMTS - 4和ADAMTS - 5进行双敲除可产生生理上正常的动物，并阻止骨关节炎的进展。

Double-knockout of ADAMTS-4 and ADAMTS-5 in mice results in physiologically normal animals and prevents the progression of osteoarthritis.

作者信息

Majumdar Manas K, Askew Roger, Schelling Scott, Stedman Nancy, Blanchet Tracey, Hopkins Bei, Morris Elisabeth A, Glasson Sonya S

机构信息

Wyeth Research, Cambridge, Massachusetts 02140, USA.

出版信息

Arthritis Rheum. 2007 Nov;56(11):3670-4. doi: 10.1002/art.23027.

DOI:10.1002/art.23027

PMID:17968948

Abstract

OBJECTIVE

To phenotypically characterize ADAMTS-4- and ADAMTS-5-double-knockout mice, and to determine the effect of deletion of ADAMTS-4 and ADAMTS-5 on the progression of osteoarthritis (OA) in mice.

METHODS

Mice lacking the catalytic domain of ADAMTS-4 and ADAMTS-5 were crossed to generate ADAMTS-4/5-double-knockout animals. Twelve-week-old and 1-year-old male and female ADAMTS-4/5-double-knockout mice were compared with age- and sex-matched wild-type (WT) mice by evaluating terminal body weights, organ weights, clinical pathology parameters, PIXImus mouse densitometry findings, and macroscopic and microscopic observations. ADAMTS-4/5-double-knockout mice were challenged by surgical induction of joint instability to determine the importance of these genes in the progression of OA. Articular and nonarticular cartilage explants from WT and ADAMTS-4/5-double-knockout mice were treated with interleukin-1 (IL-1) plus retinoic acid ex vivo, to examine proteoglycan degradation.

RESULTS

There were no genotype-related phenotype differences between ADAMTS-4/5-double-knockout and WT mice through 1 year of age, with the exception that female ADAMTS-4/5-double-knockout mice had a lower mean terminal body weight at the 12-week time point. Eight weeks after surgical induction of joint instability, OA was significantly less severe in ADAMTS-4/5-double-knockout mice compared with WT mice. Following stimulation of cartilage explants with IL-1 plus retinoic acid, aggrecanase-mediated degradation in ADAMTS-4/5-double-knockout mice was ablated, to a level comparable with that in ADAMTS-5-knockout mice.

CONCLUSION

Dual deletion of ADAMTS-4 and ADAMTS-5 generated mice that were phenotypically indistinguishable from WT mice. Deletion of ADAMTS-4/5 provided significant protection against proteoglycan degradation ex vivo and decreased the severity of murine OA. These effects in the ADAMTS-4/5-double-knockout mice were comparable with those observed with deletion of ADAMTS-5 alone.

摘要

目的

对含金属蛋白酶与凝血酶敏感素基元的蛋白聚糖酶-4（ADAMTS-4）和含金属蛋白酶与凝血酶敏感素基元的蛋白聚糖酶-5（ADAMTS-5）双敲除小鼠进行表型特征分析，并确定ADAMTS-4和ADAMTS-5缺失对小鼠骨关节炎（OA）进展的影响。

方法

将缺乏ADAMTS-4和ADAMTS-5催化结构域的小鼠进行杂交，以产生ADAMTS-4/5双敲除动物。通过评估终末体重、器官重量、临床病理学参数、PIXImus小鼠骨密度测定结果以及大体和显微镜观察，将12周龄和1岁的雄性和雌性ADAMTS-4/5双敲除小鼠与年龄和性别匹配的野生型（WT）小鼠进行比较。通过手术诱导关节不稳定来挑战ADAMTS-4/5双敲除小鼠，以确定这些基因在OA进展中的重要性。将来自WT和ADAMTS-4/5双敲除小鼠的关节软骨和非关节软骨外植体在体外用人白细胞介素-1（IL-1）加视黄酸处理，以检查蛋白聚糖降解情况。

结果

在1岁之前，ADAMTS-4/5双敲除小鼠与WT小鼠之间没有与基因型相关的表型差异，不过在12周龄时，雌性ADAMTS-4/5双敲除小鼠的平均终末体重较低。手术诱导关节不稳定8周后，与WT小鼠相比，ADAMTS-4/5双敲除小鼠的OA严重程度明显较低。在用IL-1加视黄酸刺激软骨外植体后，ADAMTS-4/5双敲除小鼠中由聚集蛋白聚糖酶介导的降解被消除，降至与ADAMTS-5敲除小鼠相当的水平。