AI Article Synopsis

  • The three main types of systemic amyloidosis are transthyretin amyloidosis (ATTR), immunoglobulin amyloidosis (AL), and inflammatory amyloidosis (AA), each with distinct characteristics and causes.
  • ATTR has two forms: wild type, common in heart disease, and a rare genetic variant linked to peripheral neuropathy; advancements in treatment have focused on stabilizing transthyretin.
  • AL is a hematological condition causing toxicity from abnormal immunoglobulin light chains, mainly affecting the heart and kidneys, while AA is associated with chronic inflammatory diseases but is less common due to effective treatments.

Article Abstract

The three most common varieties of systemic amyloidosis are transthyretin amyloidosis (ATTR), immunoglobulin amyloidosis (AL) and inflammatory amyloidosis (AA). There are two forms of transthyretin amyloidosis: the wild type, the most common, represents approximately 15% of heart diseases and the genetic, or "mutated" form, which is a rare disease and manifests mainly by peripheral neuropathy and heart disease. Major therapeutic advances have been made in recent years thanks to molecules that stabilize transthyretin and/or prevent its translation by destroying messenger RNA. Immunoglobulin amyloidosis (AL) is a hematological disease whose severity is due to the toxicity of immunoglobulin light chains forming amyloid deposits that are toxic to tissues, particularly the heart and kidneys. Treatments for immunoglobulin amyloidosis are increasingly effective, and target the plasma cell, leading to an overall improvement in the prognosis, with cardiac involvement being the most worrying condition. Inflammatory amyloidosis (AA) complicates chronic inflammatory diseases less often due to the effectiveness of anti-inflammatory biotherapies in inflammatory rheumatism, chronic inflammatory bowel diseases and genetic auto-inflammatory diseases. The causes of inflammatory amyloidosis are now more diverse with an increase in cases of unknown cause associated or not with obesity.

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Source
http://dx.doi.org/10.1016/j.annpat.2024.09.015DOI Listing

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