Bernardini Francesca, Warburton Michael J
Department of Cellular Pathology, St. George's Hospital Medical School, Cranmer Terrace, London SW17 0RE, UK.
Biochem J. 2002 Sep 1;366(Pt 2):521-9. doi: 10.1042/BJ20020467.
Tripeptidyl peptidase-I (TPP-I) is a lysosomal exopeptidase which removes tripeptides from the N-terminus of small peptides. Mutations in the TPP-I gene result in a lethal neurodegenerative disease, classical late-infantile neuronal ceroid lipofuscinosis (CLN2). This disease is characterized by the accumulation of proteinaceous and autofluorescent material within the lysosomes of neurons, which undergo massive cell death during the course of the disease. The absence of TPP-I may result in the lysosomal accumulation of small peptides and proteins, which eventually compromises lysosomal functions critical to the survival of neurons. To investigate the metabolism of small peptides, we have studied the degradation of cholecystokinin-(29-33)-amide (GWMDF-NH2; cholecystokinin C-terminal pentapeptide) by lysosomal fractions isolated from mouse brain and several other tissues. GWMDF-NH2 is cleaved at only one peptide bond by brain lysosomes, to produce GWM and DF-NH2. Inhibitor studies demonstrate that this reaction is catalysed by TPP-I. In contrast, lysosomal fractions from other mouse tissues additionally cleave a second peptide bond to produce GW and MDF-NH2. Inhibitor studies indicate that this reaction is catalysed by dipeptidyl peptidase-I (DPP-I; cathepsin C). Inhibitors of TPP-I are sufficient to completely block the degradation of GWMDF-NH2 by brain, but inhibitors of both TPP-I and DPP-I are required to completely inhibit the degradation of GWMDF-NH2 by other mouse tissues. Enzyme assays confirm the low activity of DPP-I in brain. An unrelated neuropeptide, neuromedin B, is degraded by a pathway that is partially dependent on TPP-I. These results indicate that TPP-I is required for the partial or complete digestion of certain neuropeptides by brain lysosomes. In the absence of TPP-I, neuropeptides or their degradation products will accumulate in brain lysosomes and may contribute to the pathogenesis of CLN2. Other tissues are spared because they express another peptidase, DPP-I, which has extensive activity on peptides and can compensate for the loss of TPP-I.
三肽基肽酶-I(TPP-I)是一种溶酶体外肽酶,可从小肽的N端去除三肽。TPP-I基因突变会导致一种致命的神经退行性疾病,即经典的晚发性婴儿神经元蜡样脂褐质沉积症(CLN2)。这种疾病的特征是神经元溶酶体内蛋白质和自发荧光物质的积累,在疾病过程中神经元会大量死亡。TPP-I的缺失可能导致小肽和蛋白质在溶酶体中积累,最终损害对神经元存活至关重要的溶酶体功能。为了研究小肽的代谢,我们研究了从小鼠脑和其他几种组织中分离的溶酶体组分对胆囊收缩素-(29-33)-酰胺(GWMDF-NH2;胆囊收缩素C端五肽)的降解。GWMDF-NH2仅在一个肽键处被脑溶酶体切割,产生GWM和DF-NH2。抑制剂研究表明,该反应由TPP-I催化。相比之下,来自其他小鼠组织的溶酶体组分还会切割第二个肽键,产生GW和MDF-NH2。抑制剂研究表明,该反应由二肽基肽酶-I(DPP-I;组织蛋白酶C)催化。TPP-I抑制剂足以完全阻断脑对GWMDF-NH2的降解,但需要TPP-I和DPP-I的抑制剂才能完全抑制其他小鼠组织对GWMDF-NH2的降解。酶活性测定证实了脑中DPP-I的低活性。一种无关的神经肽神经介素B通过一条部分依赖于TPP-I的途径降解。这些结果表明,TPP-I是脑溶酶体对某些神经肽进行部分或完全消化所必需的。在没有TPP-I的情况下,神经肽或其降解产物会在脑溶酶体中积累,并可能导致CLN2的发病机制。其他组织不受影响,因为它们表达另一种肽酶DPP-I,该酶对肽具有广泛的活性,可以弥补TPP-I的缺失。