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一种治疗性小干扰RNA增强Janus激酶1调节作用以治疗犬类炎症性疾病。

A Therapeutic Small-Interfering RNA Potentiates Janus Kinase 1 Modulation for the Treatment of Dog Inflammatory Diseases.

作者信息

Tang Qi, Fakih Hassan H, Gross Katherine Y, Winter Sarah J, Bramato Brianna M, Yıldız-Altay Ümmügülsüm, Chang Benjamin K, Echeverria Dimas, Jackson Samuel O, McHugh Nicholas, Srnka Alyxandr, Alterman Julia F, Almela Ramón M, Kudej Raymond K, London Cheryl A, Richmond Jillian M, Harris John E, Khvorova Anastasia

机构信息

RNA Therapeutics Institute, University of Massachusetts Chan Medical School, Worcester, Massachusetts 01605, United States.

Department of Dermatology, University of Massachusetts Chan Medical School, Worcester, Massachusetts 01605, United States.

出版信息

ACS Pharmacol Transl Sci. 2025 Mar 24;8(6):1526-1535. doi: 10.1021/acsptsci.4c00594. eCollection 2025 Jun 13.

Abstract

Inflammatory cytokine signaling pathways share notable similarities between humans and dogs. Janus kinase (JAK) family enzymesJAK1, JAK2, JAK3, and tyrosine kinase 2 (TYK2) are popular therapeutic targets for inflammatory diseases in human clinics. While more than a dozen JAK inhibitors are available for human use, the only FDA-approved JAK inhibitor for dogs is oclacitinib. Oclacitinib targets multiple JAK subtypes (i.e., JAK1/2/3 and TYK2) and requires daily oral administration, raising concerns about its long-term safety. There is a growing demand for safer and longer-lasting JAK inhibitors to improve the treatment of dog inflammatory diseases. Small-interfering RNAs (siRNAs) are an emerging class of medicines that offer mRNA sequence-specific target selectivity and sustained durability. In this work, we developed a fully chemically modified siRNA that supports efficient gene silencing of dog JAK1. We show that dog JAK1 siRNA offers more than 90% target silencing . The partial homology of the siRNA targeting site between dog and mouse mRNAs allowed us to validate the compound's preclinical activity in mouse skin and muscle tissues. In models using surgically discarded dog tissues from veterinary clinics, we show that dog JAK1 siRNA supports approximately 65% JAK1 silencing in the skin after intradermal injection and about 51% silencing in the muscle after intramuscular injection. This siRNA potentiates the treatment of inflammatory skin conditions and myopathies in dogs. Further engineering of siRNA may extend its utility to additional tissues, opening up new avenues for the development of immunomodulatory therapies for dogs.

摘要

炎症细胞因子信号通路在人类和犬类之间有显著的相似性。Janus激酶(JAK)家族酶——JAK1、JAK2、JAK3和酪氨酸激酶2(TYK2)——是人类临床炎症性疾病常用的治疗靶点。虽然有十几种JAK抑制剂可供人类使用,但美国食品药品监督管理局(FDA)批准的唯一一种用于犬类的JAK抑制剂是奥克拉替尼。奥克拉替尼靶向多种JAK亚型(即JAK1/2/3和TYK2),需要每日口服,这引发了人们对其长期安全性的担忧。对更安全、作用更持久的JAK抑制剂的需求日益增长,以改善犬类炎症性疾病的治疗。小干扰RNA(siRNA)是一类新兴药物,具有mRNA序列特异性靶点选择性和持续耐久性。在这项研究中,我们开发了一种完全化学修饰的siRNA,它能有效沉默犬类JAK1基因。我们发现犬类JAK1 siRNA能实现超过90%的靶点沉默。犬类和小鼠mRNA之间siRNA靶向位点的部分同源性使我们能够在小鼠皮肤和肌肉组织中验证该化合物的临床前活性。在使用兽医诊所手术废弃犬类组织的模型中,我们发现犬类JAK1 siRNA在皮内注射后能使皮肤中的JAK1沉默约65%,在肌肉注射后能使肌肉中的JAK1沉默约51%。这种siRNA增强了犬类炎症性皮肤病和肌病的治疗效果。对siRNA的进一步改造可能会将其应用扩展到其他组织,为犬类免疫调节疗法的开发开辟新途径。

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