Institute of Metabolic Disease, Baylor Research Institute, Dallas, TX 75226, USA.
J Inherit Metab Dis. 2010 Aug;33(4):373-9. doi: 10.1007/s10545-010-9047-0. Epub 2010 Feb 17.
Therapy of the central nervous system (CNS) manifestations of lysosomal storage diseases (LSDs) has remained a major challenge because of its inability to deliver therapeutic agents efficiently across the intact blood-brain barrier. Non-specific therapies such as hematopoietic stem cell transplantation have been useful in globoid cell leukodystrophy (Krabbe disease) and in some mucopolysaccharidoses. Anti-inflammatory agents also show promise as adjuvant therapy. High doses of replacement therapy with native or modified enzyme show renewed promise for correction of CNS cells. Alternatively, small molecules can enter the brain relatively easily and promote reduction of accumulated substrate or function as pharmacological chaperones to enhance the level of the deficient enzyme. Gene therapy is still being developed and tested in patients. It is therefore likely that, thanks to a better understanding of disease mechanism, a variety of therapeutic approaches, used alone or in combination, will be useful to treat the devastating neurological complications of LSDs.
中枢神经系统 (CNS) 溶酶体贮积症 (LSD) 的治疗仍然是一个主要挑战,因为它无法有效地将治疗剂穿过完整的血脑屏障递送到 CNS。非特异性治疗,如造血干细胞移植,在球形体脑白质营养不良(Krabbe 病)和一些黏多糖贮积症中是有用的。抗炎剂也显示出作为辅助治疗的潜力。用天然或修饰的酶进行高剂量的替代治疗,为纠正 CNS 细胞提供了新的希望。或者,小分子可以相对容易地进入大脑,促进积累底物的减少,或作为药理学伴侣,以增强缺陷酶的水平。基因治疗仍在患者中进行开发和测试。因此,由于对疾病机制的更好理解,各种治疗方法,单独或联合使用,都可能有助于治疗 LSD 的毁灭性神经并发症。
