Guidelines and new directions in the therapy and monitoring of ATTRv amyloidosis

转甲状腺素 医学 淀粉样变性 临床试验 疾病 淀粉样蛋白(真菌学) 淀粉样疾病 肝移植 心脏淀粉样变性 心肌病 重症监护医学 生物信息学 移植 内科学 病理 淀粉样纤维 心力衰竭 生物 淀粉样β
作者
Yukio Ando,David Adams,Merrill D. Benson,John L. Berk,Violaine Planté‐Bordeneuve,Teresa Coelho,Isabel Conceição,Bo‐Göran Ericzon,Laura Obici,Claudio Rapezzi,Yoshiki Sekijima,Mitsuharu Ueda,Giovanni Palladini,Giampaolo Merlini
出处
期刊:Amyloid [Informa]
卷期号:29 (3): 143-155 被引量:76
标识
DOI:10.1080/13506129.2022.2052838
摘要

The recent approval of three drugs for the treatment of amyloid transthyretin (ATTR) amyloidosis, both hereditary and wild-type, has opened a new era in the care of these diseases. ATTR amyloidosis is embedded in its pathophysiology, and the drugs target critical steps of the amyloid cascade. In addition to liver transplant, which removes the pathogenic variants, the introduction of gene silencers has allowed the suppression of both wild type and mutant transthyretin (TTR), thus extending the potential therapeutic range to wild-type cardiac amyloidosis. The kinetic stabilisation of TTR using small molecules has proved to be clinically effective both for amyloid neuropathy and cardiomyopathy. Gene silencers and kinetic stabilizers were recently approved on the basis of the outcome of phase III trials; however, comparative trials have not been performed, making it difficult to draw recommendations. Indications for liver transplantation have narrowed considerably. Here, guidelines for therapy are proposed based on expert consensus, acknowledging that the several drugs currently undergoing clinical trials will probably change in the near future the therapeutic armamentarium and, consequently, the therapeutic strategy. Indications for monitoring disease progression and drug efficacy are also provided for the management of these complexes, but now very treatable, diseases.
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