KeyNeurotek Pharmaceuticals AG, Leipziger Str. 44, D-39120 Magdeburg, Germany.
J Neuroinflammation. 2012 Feb 28;9:44. doi: 10.1186/1742-2094-9-44.
Cerebral inflammation is a hallmark of neuronal degeneration. Dipeptidyl peptidase IV, aminopeptidase N as well as the dipeptidyl peptidases II, 8 and 9 and cytosolic alanyl-aminopeptidase are involved in the regulation of autoimmunity and inflammation. We studied the expression, localisation and activity patterns of these proteases after endothelin-induced occlusion of the middle cerebral artery in rats, a model of transient and unilateral cerebral ischemia.
Male Sprague-Dawley rats were used. RT-PCR, immunohistochemistry and protease activity assays were performed at different time points, lasting from 2 h to 7 days after cerebral ischemia. The effect of protease inhibitors on ischemia-dependent infarct volumes was quantified 7 days post middle cerebral artery occlusion. Statistical analysis was conducted using the t-test.
Qualitative RT-PCR revealed these proteases in ipsilateral and contralateral cortices. Dipeptidyl peptidase II and aminopeptidase N were up-regulated ipsilaterally from 6 h to 7 days post ischemia, whereas dipeptidyl peptidase 9 and cytosolic alanyl-aminopeptidase were transiently down-regulated at day 3. Dipeptidyl peptidase 8 and aminopeptidase N immunoreactivities were detected in cortical neurons of the contralateral hemisphere. At the same time point, dipeptidyl peptidase IV, 8 and aminopeptidase N were identified in activated microglia and macrophages in the ipsilateral cortex. Seven days post artery occlusion, dipeptidyl peptidase IV immunoreactivity was found in the perikarya of surviving cortical neurons of the ipsilateral hemisphere, whereas their nuclei were dipeptidyl peptidase 8- and amino peptidase N-positive. At the same time point, dipeptidyl peptidase IV, 8 and aminopeptidase N were targeted in astroglial cells. Total dipeptidyl peptidase IV, 8 and 9 activities remained constant in both hemispheres until day 3 post experimental ischemia, but were increased (+165%) in the ipsilateral cortex at day 7. In parallel, aminopeptidase N and cytosolic alanyl-aminopeptidase activities remained unchanged.
Distinct expression, localization and activity patterns of proline- and alanine-specific proteases indicate their involvement in ischemia-triggered inflammation and neurodegeneration. Consistently, IPC1755, a non-selective protease inhibitor, revealed a significant reduction of cortical lesions after transient cerebral ischemia and may suggest dipeptidyl peptidase IV, aminopeptidase N and proteases with similar substrate specificity as potentially therapy-relevant targets.
脑炎症是神经元变性的标志。二肽基肽酶 IV、氨基肽酶 N 以及二肽基肽酶 II、8 和 9 和胞质丙氨酰-氨基肽酶参与自身免疫和炎症的调节。我们研究了这些蛋白酶在大鼠大脑中动脉内皮素诱导闭塞后的表达、定位和活性模式,这是短暂性和单侧脑缺血的模型。
使用雄性 Sprague-Dawley 大鼠。在脑缺血后 2 小时至 7 天的不同时间点进行 RT-PCR、免疫组织化学和蛋白酶活性测定。使用 t 检验对 7 天后大脑中动脉闭塞后依赖于蛋白酶抑制剂的梗塞体积进行定量分析。
定性 RT-PCR 显示这些蛋白酶在同侧和对侧皮质中均有表达。二肽基肽酶 II 和氨基肽酶 N 从缺血后 6 小时到 7 天同侧上调,而二肽基肽酶 9 和胞质丙氨酰-氨基肽酶在第 3 天短暂下调。在对侧半球的皮质神经元中检测到二肽基肽酶 8 和氨基肽酶 N 免疫反应性。在同一时间点,在同侧皮质中鉴定到二肽基肽酶 IV、8 和氨基肽酶 N 在激活的小胶质细胞和巨噬细胞中。动脉闭塞后 7 天,在同侧半球存活的皮质神经元的胞体中发现二肽基肽酶 IV 免疫反应性,而其核为二肽基肽酶 8 和氨基肽酶 N 阳性。在同一时间点,二肽基肽酶 IV、8 和氨基肽酶 N 被靶向于星形胶质细胞。在实验性缺血后 3 天,两侧半球的总二肽基肽酶 IV、8 和 9 活性保持不变,但在第 7 天同侧皮质增加(+165%)。同时,氨基肽酶 N 和胞质丙氨酰-氨基肽酶活性保持不变。
脯氨酸和丙氨酸特异性蛋白酶的不同表达、定位和活性模式表明它们参与了缺血触发的炎症和神经退行性变。一致地,IPC1755,一种非选择性蛋白酶抑制剂,在短暂性脑缺血后显示出皮质病变的显著减少,并且可能表明二肽基肽酶 IV、氨基肽酶 N 和具有类似底物特异性的蛋白酶作为潜在的治疗相关靶点。
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