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活性增强的祖先溶酶体酶具有治疗亨特综合征的治疗潜力。

Ancestral lysosomal enzymes with increased activity harbor therapeutic potential for treatment of Hunter syndrome.

作者信息

Hendrikse Natalie M, Sandegren Anna, Andersson Tommy, Blomqvist Jenny, Makower Åsa, Possner Dominik, Su Chao, Thalén Niklas, Tjernberg Agneta, Westermark Ulrica, Rockberg Johan, Svensson Gelius Stefan, Syrén Per-Olof, Nordling Erik

机构信息

Swedish Orphan Biovitrum AB, Stockholm 112 76, Sweden.

Science for Life Laboratory, School of Engineering Sciences in Chemistry, Biotechnology and Health, KTH Royal Institute of Technology, Solna 171 21, Sweden.

出版信息

iScience. 2021 Feb 6;24(3):102154. doi: 10.1016/j.isci.2021.102154. eCollection 2021 Mar 19.

Abstract

We show the successful application of ancestral sequence reconstruction to enhance the activity of iduronate-2-sulfatase (IDS), thereby increasing its therapeutic potential for the treatment of Hunter syndrome-a lysosomal storage disease caused by impaired function of IDS. Current treatment, enzyme replacement therapy with recombinant human IDS, does not alleviate all symptoms, and an unmet medical need remains. We reconstructed putative ancestral sequences of mammalian IDS and compared them with extant IDS. Some ancestral variants displayed up to 2-fold higher activity than human IDS in assays and cleared more substrate in experiments in patient fibroblasts. This could potentially allow for lower dosage or enhanced therapeutic effect in enzyme replacement therapy, thereby improving treatment outcomes and cost efficiency, as well as reducing treatment burden. In summary, we showed that ancestral sequence reconstruction can be applied to lysosomal enzymes that function in concert with modern enzymes and receptors in cells.

摘要

我们展示了祖先序列重建在增强艾杜糖醛酸-2-硫酸酯酶(IDS)活性方面的成功应用,从而提高了其治疗亨特综合征(一种由IDS功能受损引起的溶酶体贮积病)的潜力。目前的治疗方法是用重组人IDS进行酶替代疗法,但并不能缓解所有症状,仍存在未满足的医疗需求。我们重建了哺乳动物IDS的推定祖先序列,并将它们与现存的IDS进行比较。在测定中,一些祖先变体的活性比人IDS高出2倍,并且在患者成纤维细胞的实验中清除了更多的底物。这有可能在酶替代疗法中降低剂量或增强治疗效果,从而改善治疗结果和成本效益,并减轻治疗负担。总之,我们表明祖先序列重建可应用于与细胞中的现代酶和受体协同发挥作用的溶酶体酶。

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