What question did this study set out to answer?

The study aims to determine if neuroinflammatory biomarkers can differentiate between hypertensive intracerebral hemorrhage and cerebral amyloid angiopathy.

February 2, 2026

Abstract WP280: Distinguishing Hypertensive Intracerebral Hemorrhage from Cerebral Amyloid Angiopathy: A Pilot Inflammatory Biomarker Approach

Key Points

The study aims to determine if neuroinflammatory biomarkers can differentiate between hypertensive intracerebral hemorrhage and cerebral amyloid angiopathy.
Enrolled 56 patients with acute intracerebral hemorrhage, split between hypertensive ICH and CAA.
Collected serum samples within 72 hours of onset for biomarker analysis.
Compared biomarker levels with healthy controls matched for age and sex.
Measured biomarkers using multiplex immunoassay.
CAA patients showed significantly elevated levels of CXCL13 and TREM2 compared to controls.
No significant differences were found for IL-34, MIF, RAGE, or YKL-40.
Trends indicated higher YKL-40 levels in CAA patients, though not statistically significant.
Biomarker patterns did not differentiate between hypertensive ICH and CAA in this cohort.

Abstract

Introduction: Distinguishing the etiology of intracerebral hemorrhage (ICH), whether due to hypertension or cerebral amyloid angiopathy (CAA), remains a critical clinical challenge, particularly as imaging often reveals overlapping pathologies in older adults. Inflammation is central to ICH pathophysiology and may provide diagnostic insights. We evaluated a panel of neuroinflammatory biomarkers to explore whether distinct profiles could help differentiate hypertensive ICH from CAA-related hemorrhage. Hypothesis: We hypothesized that circulating neuroinflammatory biomarkers could help distinguish hypertensive ICH from CAA. Methods: Fifty-six patients with acute ICH (mean age 74 ± 7.9) were enrolled: 28 with hypertensive ICH and 28 with CAA-related hemorrhage. Serum samples were obtained within 72 hours of onset. Twenty-four age- and sex-matched healthy controls (mean age 75 ± 12.8) without neurologic disease provided single time-point samples. Exclusion criteria included active cancer, recent blood transfusion, or active substance abuse. Biomarker levels (BLC/CXCL13, TREM2, IL-34, MIF, RAGE, YKL-40, ThermoFisher) were quantified using a multiplex immunoassay. Results: Compared with controls, patients with CAA demonstrated significantly elevated BLC (CXCL13) (p = 0.037) and TREM2 (p = 0.038). No significant differences were observed in IL-34, MIF, RAGE, or YKL-40. Biomarker patterns between hypertensive ICH and CAA did not differ significantly in this pilot cohort, although a trend was seen towards higher levels of YKL-40 in CAA patients. Conclusion: This pilot study suggests that selected neuroinflammatory biomarkers, particularly CXCL13 and TREM2, are elevated in CAA-related ICH compared with healthy aging controls. While these findings do not clearly distinguish CAA from hypertensive ICH, they highlight the potential of inflammatory profiling to enhance phenotyping of hemorrhagic stroke and guide future biomarker discovery. Further studies in larger cohorts are warranted to refine diagnostic signatures in ICH.

Abstract WP280: Distinguishing Hypertensive Intracerebral Hemorrhage from Cerebral Amyloid Angiopathy: A Pilot Inflammatory Biomarker Approach

Key Points

Abstract

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