: AL amyloidosis is a life-threatening disease caused by deposition of immunoglobulin light chains. While the mechanisms underlying light chains amyloidogenesis in vivo remain unclear, several studies have highlighted the role that tissue environment and structural amyloidogenicity of individual light chains have in the disease pathogenesis. AL natural deposits contain both full-length light chains and fragments encompassing the variable domain (VL) as well as different length segments of the constant region (CL), thus highlighting the relevance that proteolysis may have in the fibrillogenesis pathway. Here, we investigate the role of major truncated species of the disease-associated AL55 light chain that were previously identified in natural deposits. Specifically, we study structure, molecular dynamics, thermal stability, and capacity to form fibrils of a fragment containing both the VL and part of the CL (133-AL55), in comparison with the full-length protein and its variable domain alone, under shear stress and physiological conditions. Whereas the full-length light chain forms exclusively amorphous aggregates, both fragments generate fibrils, although, with different kinetics, aggregate structure, and interplay with the unfragmented protein. More specifically, the VL-CL 133-AL55 fragment entirely converts into amyloid fibrils microscopically and spectroscopically similar to their ex vivo counterpart and increases the amorphous aggregation of full-length AL55. Overall, our data support the idea that light chain structure and proteolysis are both relevant for amyloidogenesis in vivo and provide a novel biocompatible model of light chain fibrillogenesis suitable for future mechanistic studies.

Lavatelli, F., Natalello, A., Marchese, L., Ami, D., Corazza, A., Raimondi, S., et al. (2024). Truncation of the constant domain drives amyloid formation by immunoglobulin light chains. THE JOURNAL OF BIOLOGICAL CHEMISTRY, 300(4) [10.1016/j.jbc.2024.107174].

Truncation of the constant domain drives amyloid formation by immunoglobulin light chains

Natalello A.
Secondo
;
Ami D.;
2024

Abstract

: AL amyloidosis is a life-threatening disease caused by deposition of immunoglobulin light chains. While the mechanisms underlying light chains amyloidogenesis in vivo remain unclear, several studies have highlighted the role that tissue environment and structural amyloidogenicity of individual light chains have in the disease pathogenesis. AL natural deposits contain both full-length light chains and fragments encompassing the variable domain (VL) as well as different length segments of the constant region (CL), thus highlighting the relevance that proteolysis may have in the fibrillogenesis pathway. Here, we investigate the role of major truncated species of the disease-associated AL55 light chain that were previously identified in natural deposits. Specifically, we study structure, molecular dynamics, thermal stability, and capacity to form fibrils of a fragment containing both the VL and part of the CL (133-AL55), in comparison with the full-length protein and its variable domain alone, under shear stress and physiological conditions. Whereas the full-length light chain forms exclusively amorphous aggregates, both fragments generate fibrils, although, with different kinetics, aggregate structure, and interplay with the unfragmented protein. More specifically, the VL-CL 133-AL55 fragment entirely converts into amyloid fibrils microscopically and spectroscopically similar to their ex vivo counterpart and increases the amorphous aggregation of full-length AL55. Overall, our data support the idea that light chain structure and proteolysis are both relevant for amyloidogenesis in vivo and provide a novel biocompatible model of light chain fibrillogenesis suitable for future mechanistic studies.
Articolo in rivista - Articolo scientifico
AL amyloidosis; amyloidogenesis; cardiomyopathy; constant domain; immunoglobulin light chains; proteolysis;
English
16-mar-2024
2024
300
4
107174
open
Lavatelli, F., Natalello, A., Marchese, L., Ami, D., Corazza, A., Raimondi, S., et al. (2024). Truncation of the constant domain drives amyloid formation by immunoglobulin light chains. THE JOURNAL OF BIOLOGICAL CHEMISTRY, 300(4) [10.1016/j.jbc.2024.107174].
File in questo prodotto:
File Dimensione Formato  
Lavatelli-2024-J Biol Chem-VoR.pdf

accesso aperto

Tipologia di allegato: Publisher’s Version (Version of Record, VoR)
Licenza: Creative Commons
Dimensione 3.16 MB
Formato Adobe PDF
3.16 MB Adobe PDF Visualizza/Apri
SI_Lavatelli-2024-J Biol Chem-VoR.pdf

accesso aperto

Descrizione: dati supplementari
Tipologia di allegato: Publisher’s Version (Version of Record, VoR)
Licenza: Creative Commons
Dimensione 2.69 MB
Formato Adobe PDF
2.69 MB Adobe PDF Visualizza/Apri

I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.

Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/491879
Citazioni
  • Scopus 1
  • ???jsp.display-item.citation.isi??? 0
Social impact