Redefining ALS: Large-scale proteomic profiling reveals a prolonged pre-diagnostic phase with immune, muscular, metabolic, and brain involvement

  1. Jan Homann
  2. Roxanna Korologou-Linden
  3. Vivian Viallon
  4. Sarah Morgan
  5. Valerija Dobricic
  6. Laura Deecke
  7. Julia P. Schessner
  8. Karl Smith-Byrne
  9. Daniel Birtles
  10. Yujia Zhao
  11. Joanne Wuu
  12. Fanny Artaud
  13. Fatema Hajizadah
  14. Jose Maria Huerta
  15. Olena Ohlei
  16. Mikhail Lebedev
  17. P. Martijn Kolijn
  18. Marcela Guevara
  19. Ana Jimenez-Zabala
  20. María José Sánchez
  21. Camino Trobajo-Sanmartín
  22. Sandra M. Colorado-Yohar
  23. Sonia Alonso-Martín
  24. Dafina Petrova
  25. Sabina Sieri
  26. Klaus Berger
  27. Susan Peters
  28. Nick Wareham
  29. Rudolph Kaaks
  30. Ruth C. Travis
  31. Roel C. H. Vermeulen
  32. The Global Neurodegeneration Proteomics Consortium (GNPC)
  33. Ioanna Tzoulaki
  34. Alexis Elbaz
  35. Matthias Mann
  36. Carlotta Sacerdote
  37. Giovanna Masala
  38. Verena Katzke
  39. Michael Benatar
  40. Lars Bertram
  41. Lefkos Middleton
  42. Elio Riboli
  43. Marc J. Gunter
  44. Pietro Ferrari
  45. Oliver Robinson
  46. Christina M. Lill
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Abstract

Background

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disorder with a largely unknown duration and pathophysiology of the pre-diagnostic phase, especially for the common non-monogenic form.

Methods

We leveraged the European Prospective Investigation into Cancer and Nutrition (EPIC) cohort with up to 30 years of follow-up to identify incident ALS cases across five European countries. Pre-diagnostic plasma samples from initially healthy participants underwent high-throughput proteomic profiling (7,285 protein markers, SomaScan). Cox proportional hazards models based on 4,567 participants (including 172 incident ALS cases) were used to identify protein biomarkers associated with future ALS diagnosis. Top results were indirectly validated in two independent case-control studies of prevalent ALS (n=417 ALS, 852 controls). Functional annotation included cross-disease comparisons, gene set and tissue enrichment testing, organ-specific proteomic clocks, and the application of large-language models (LLM).

Findings

Five proteins (SECTM1, CA3, THAP4, KLHL41, SLC26A7) were identified as significant pre-diagnostic ALS biomarkers (FDR=0.05), detectable approximately two decades before diagnosis. Of these, all except SECTM1 were indirectly validated in independent cohorts of prevalent ALS cases, supporting their clinical significance. Additionally, 22 nominally significant (p<0.05) pre-diagnostic biomarkers were FDR-significant in prevalent ALS with consistent effect directions. Cross-disease comparisons with pre-diagnostic Parkinson’s and Alzheimer’s disease suggested a largely specific pre-diagnostic ALS biomarker signature. Gene ontology and tissue enrichment highlighted early involvement of immune, muscle, metabolic, and digestive processes. Furthermore, analyses of proteomic clocks revealed accelerated aging in brain-cognition, immune, and muscle tissues before clinical diagnosis. Druggability and LLM analyses revealed possible therapeutic targets and novel strategies, emphasizing translational relevance.

Interpretation

Our study provides first evidence of ultra-early molecular changes in common ALS up to two decades prior to clinical onset, mainly affecting immune, muscle, metabolic, digestive, and cognitive systems. Our study nominates several compelling candidates for risk stratification studies and novel therapeutic targets for early intervention.

Funding

Clinical Research in ALS and Related Disorders for Therapeutic Development (CreATe) Consortium, Cure Alzheimer’s Fund, Michael J Fox Foundation, Interdisciplinary Centre for Clinical Research, University Münster

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  1. Version published to 10.1101/2025.08.20.25334061 on medRxiv