Post-Translational Changes in Serum Albumin in Patients with Alcohol-Associated Hepatitis

Bibliographic info

  • Authors: Jonathan Montomoli, Maurizio Baldassarre, Thomas Damgaard Sandahl, Marina Naldi, Emilie Glavind, Enrico Pompili, Peter Jepsen, Francesco Palmese, Paolo Caraceni, Hendrik Vilstrup, Marco Domenicali
  • Journal: International Journal of Molecular Sciences (IJMS), 2026, vol. 27, art. 1503; Open Access (CC BY); Received 27 Nov 2025, Accepted 30 Jan 2026, Published 3 Feb 2026
  • Institutions: Aarhus University Hospital, Denmark; IRCCS AOU Bologna; University of Bologna, Italy; Infermi Hospital, Rimini, Italy

Key question

Do HSA post-translational changes — specifically the HMA/HNA1/HNA2 fractions and the full isoform profile including native, cysteinylated, glycated, and truncated forms — differ between survivors and non-survivors in patients with alcohol-associated hepatitis (AAH), and can they predict 90-day outcome?

Methods

  • Sample type: Human serum — baseline (admission) and day 14
  • Cohort: 49 patients with alcohol-associated hepatitis (AAH); 38 survivors at 90 days; 11 non-survivors at 90 days; 20 healthy subjects (comparison)
  • Clinical scoring: MELD (median = not shown), GAHS (Glasgow Alcohol-associated Hepatitis Score)
  • Technique: LC-MS (top-down; HPLC-ESI-MS) for HSA isoform quantification
  • Isoforms measured: Native HSA; HMA (total mercaptalbumin); HNA1; HNA2; HSA-DA (N-term truncated); HSA-L (C-term truncated); HSA+Cys-DA; HSA-DHA (dehydroalanine at Cys34)
  • Timepoints: Admission (D0) and day 14
  • Statistical: Wilcoxon rank-sum test; chi-squared; comparison AAH vs healthy subjects

Main findings

Cohort characteristics (at admission)

CharacteristicAH Population (N=49)90-Day Survivors (N=38)90-Day Non-Survivors (N=11)p-value
Age (median IQR)53 (48–58)52 (47–57)54 (48–58)0.611
Male sex34 (69%)27 (71%)7 (64%)0.638
Albumin (g/L)26 (22–30)26 (22–30)26 (23–31)0.622
CRP (mg/dL)32 (23–…)

HSA isoform fractions at admission (% median IQR)

IsoformAH (N=49)90-Day Survivors90-Day Non-Survivorsp-value
Native HSA34.2 (30.2–44.1)36.2 (30.4–46.4)32.6 (29.7–37.4)0.523
HMA62.3 (56.1–67.9)63.5 (57.3–68.3)59.6 (53.3–64.2)0.337
HNA132.6 (27.2–39.5)31.7 (26.8–39.1)34.79 (30.9–43.3)0.337
HNA24.4 (3.1–5.9)4.1 (3.2–5.9)4.8 (2.8–6.2)0.915

HSA isoform fractions at day 14 (% median IQR)

IsoformAH Population90-Day Survivors90-Day Non-Survivorsp-value
Native HSA39.3 (31.2–43.7)39.8 (32.0–43.7)38.9 (29.7–44.0)0.775
HMA62.2 (56.9–68.7)62.1 (57.0–67.6)68.7 (58.5–71.0)0.145
HNA132.4 (25.2–37.6)32.9 (26.4–38.2)26.2 (23.8–35.0)0.171
HNA24.9 (4.3–6.1)4.8 (4.2–6.1)5.0 (4.4–5.9)0.881

Key finding

  • No significant difference in HSA isoform fractions between 90-day survivors and non-survivors at admission or day 14 (all p > 0.05)
  • Trend: non-survivors had slightly lower native HSA and HMA, higher HNA1 at admission — but underpowered (N=11 non-survivors)
  • AAH patients showed different HSA isoform distribution vs healthy subjects (Figure 1 in paper)
  • ⚠️ HSA isoforms in AAH do not significantly predict 90-day survival in this cohort

PTMs characterized

IsoformModificationDetectionNotes
HMAReduced Cys34LC-MSDominant healthy/AAH form
HNA1Reversible oxidation Cys34 (+119 Da cysteinylation, or disulfide)LC-MSElevated in AAH vs healthy
HNA2Irreversible oxidationLC-MSLow but elevated in AAH
HSA-DHADehydroalanine conversion at Cys34LC-MSNovel isoform mentioned
HSA-DAN-term truncationLC-MSMeasured
HSA+Cys-DACYS + N-term truncationLC-MSMeasured

Clinical context

  • Disease: Alcohol-associated hepatitis (AAH) — acute-on-chronic alcohol-related liver disease; 49 patients
  • Cohort sites: Aarhus University Hospital (Denmark); Bologna (Italy) — Scandinavian + Italian cohort
  • Implication: HSA PTM profiling in AAH shows altered isoform distribution vs healthy but does not predict survival at 90 days in this small cohort. Underpowered for the 11 non-survivor group.

Limitations

  • Small sample (49 total; only 11 non-survivors) — major limitation for survival analysis
  • Relative quantification only (%)
  • No multivariate survival analysis reported in available pages — MELD and GAHS likely dominate
  • Day 14 timepoint provides additional information but no significant discrimination

Connections

  • HSA — isoform profiling in AAH; first data with day 14 timepoint
  • naldi-2016-ah — preceded this paper; smaller characterization study of HSA in AH
  • das-2017-sah — SAH albumin modulates neutrophils; provides mechanistic context
  • domenicali-2014 — established isoform profiling in stable cirrhosis; AAH is a different clinical context
  • el-balkhi-2025 — ALBOM study (stable CLD fibrosis); native HSA predicts fibrosis stage; AAH here is acute setting where this may not apply similarly

Take home notes

  • The null result (no survival prediction) is important to capture — it does not mean HSA isoforms are useless in AAH, but the n=11 non-survivors is severely underpowered. A larger study would be needed.
  • Montomoli is the first author — a clinician at Aarhus + Rimini. He is co-author on naldi-2016-ah too. This study is the clinical expansion of that earlier work.
  • The HSA-DHA (dehydroalanine) isoform is mentioned — this is a chemical conversion of Cys34 that can occur in alkaline conditions or as a PTM. Not typically quantified in the ALBOM panel — worth investigating.
  • The comparison of AAH vs healthy subjects confirms that AAH does alter the isoform distribution (HNA1 elevated, native HSA decreased relative to healthy) — the question is just about survival prediction, which requires larger cohorts.