Affiliation: German Center for Neurodegenerative Diseases (DZNE), Munich Location: Munich, Germany Focus: Progressive Supranuclear Palsy, fluid biomarkers, clinical trials, longitudinal patient registries, atypical parkinsonism
Overview
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researchers_anja_eibens["Anja Eibens German Neurologist and PSP Researc"]
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researchers_anja_eib_0["Background and Training"]
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researchers_anja_eib_1["Research Contributions"]
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researchers_anja_eib_2["The German PSP Registry"]
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researchers_anja_eib_3["Fluid Biomarker Development"]
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researchers_anja_eib_4["Clinical Phenotype of PSP in German Cohorts 202"]
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researchers_anja_eib_5["Symptomatic Treatment Outcomes in PSP 2022"]
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style researchers_anja_eib_5 fill:#81c784,stroke:#333,color:#000Dr. Anja Eibens is a German neurologist and researcher specializing in movement disorders and neurodegenerative diseases at the German Center for Neurodegenerative Diseases (DZNE) in Munich. Her work focuses on understanding the pathophysiology of Progressive Supranuclear Palsy (PSP), developing biomarkers for clinical trial enrichment and patient stratification, and building longitudinal natural history databases that inform therapeutic development for tauopathies
As principal investigator of the German PSP Registry, Dr. Eibens has established one of Europe’s most comprehensive longitudinal cohorts of PSP patients, enabling the natural history studies and biomarker validation work that are critical for the design of disease-modifying therapy trials.
Background and Training
Dr. Eibens completed her medical training and neurology residency at German academic medical centers, developing her specialization in movement disorders during her clinical and research training. She joined the DZNE Munich site, which is embedded within the Neurology Department of the Ludwig Maximilian University (LMU) Hospital, providing integration with the clinical movement disorder service and access to a large patient population.
Her research training included clinical trial methodology at leading European centers, longitudinal cohort management, and advanced biomarker analysis techniques including immunoassay development, multiplex platforms, and single-molecule array (Simoa) sensitivity optimization.
Research Contributions
The German PSP Registry
Dr. Eibens leads the German PSP Registry, one of Europe’s largest prospective longitudinal cohorts of PSP patients3German Center for Neurodegenerative Diseases: PSP research programOpen reference:
Registry design:
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Target enrollment: 500 PSP patients across 12 German neurology centers
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Standardized baseline characterization: demographics, family history, MDS clinical diagnostic criteria verification
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Annual follow-up: comprehensive motor (PSPRS), cognitive (MDRS, Trail Making Test), functional (Schwab & England ADL), and quality of life assessments
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Biosampling: CSF and serum at baseline and every 12 months; DNA at baseline for genetic screening
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Neuroimaging: 3T MRI at baseline and 24-month follow-up at the DZNE Munich imaging core
Key registry outputs:
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5-year longitudinal natural history data published in 20234Motor and cognitive progression in PSP: a 5-year longitudinal analysisOpen reference
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Biomarker validation cohort for European clinical trials
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Foundation for genotype-phenotype correlation studies
Fluid Biomarker Development
Dr. Eibens has made significant contributions to PSP biomarker research across multiple modalities:
Neurofilament Light Chain (NfL)
Dr. Eibens’s 2023 prospective study2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference established NfL as a prognostic biomarker in PSP:
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Cohort: 200 PSP patients and 100 healthy age-matched controls
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Serum and CSF: Both matrices analyzed using Simoa NF-light assay
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Key finding: Baseline serum NfL above 130 pg/mL predicted 2.3x faster disease progression on PSPRS (p<0.001) and 1.8x higher mortality risk at 3 years
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Diagnostic accuracy: Serum NfL distinguished PSP from PD with AUC of 0.91 and from healthy controls with AUC of 0.94
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Clinical utility: Cutoff of 130 pg/mL recommended for prognostic stratification and clinical trial enrichment5CSF NfL as prognostic biomarker in PSPOpen reference
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Correlation with disease stage: NfL levels showed strong positive correlation with PSPRS total score (r=0.71) and disease duration (r=0.54)
CSF Biomarker Trajectories in PSP (2024)
The 2024 longitudinal CSF study1Longitudinal CSF biomarker changes in PSP: results from the German PSP RegistryOpen reference documented biomarker changes over 3 years:
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Markers profiled: CSF total tau, p-tau181, p-tau217, NfL, neurogranin, and GFAP
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Progressive increases: CSF NfL and p-tau217 showed significant annual increases (+12% and +8% per year respectively), while total tau remained relatively stable
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Discriminative validity: CSF p-tau217 showed the best accuracy for distinguishing PSP from controls (AUC 0.93) and from PD (AUC 0.82)
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Correlation with imaging: Higher baseline CSF NfL correlated with faster midbrain atrophy rate on MRI (r=0.53)
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Trial endpoint implications: The longitudinal trajectories inform expected biomarker change over trial duration for enrichment and secondary endpoint selection
Blood p-tau231 for Clinical Trial Enrollment (2025)
The 2025 study6Blood p-tau231 as a screening biomarker for PSP clinical trial enrollmentOpen reference evaluated plasma p-tau231 as a screening biomarker:
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Purpose: Identify PSP patients most likely to benefit from disease-modifying trials targeting tau pathology
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Method: Simoa p-tau231 assay on plasma samples from 400 PSP patients
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Performance: Plasma p-tau231 distinguished PSP from controls with AUC 0.89 and from PD with AUC 0.78
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Trial application: Proposed p-tau231 > 2 pg/mL as enrollment criterion to enrich trials for patients with active tau pathology
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Integration with NfL: Combining p-tau231 and NfL into a two-biomarker panel improved prognostic stratification for disease progression rate
Plasma GFAP as Astrogliosis Marker (2024)
Dr. Eibens contributed to characterizing GFAP as a marker of astroglial activation in PSP7Plasma glial fibrillary acidic protein as a marker of astrogliosis in PSPOpen reference:
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GFAP elevation: PSP patients showed significantly elevated plasma GFAP vs. controls (median 180 pg/mL vs. 95 pg/mL, p<0.001)
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Correlation with disease severity: Higher GFAP associated with more severe PSPRS scores and faster disease progression
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Independence from NfL: GFAP and NfL showed moderate correlation (r=0.45), suggesting they capture partially distinct pathological processes
Clinical Phenotype of PSP in German Cohorts (2023)
The 2023 descriptive study8Clinical phenotype of PSP in German cohorts: demographic and prognostic featuresOpen reference characterized 400 German PSP patients:
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Subtype distribution: Richardson’s syndrome 52%, PSP-P 18%, PSP-PAGF 8%, PSP-CBS 7%, other variants 15%
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Demographics: Mean age at onset 64.3 years (SD 7.1), mean disease duration at enrollment 3.2 years
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Prognostic factors: Early falls (within 1 year of onset), early dysphagia, and symmetric akinesia predicted faster progression
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Genetic screening: MAPT H1/H1 genotype in 78% of cases; no LRRK2 G2019S mutations found
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Family history: Positive family history in 12% of cases, consistent with sporadic PSP predominance in Central Europe
Symptomatic Treatment Outcomes in PSP (2022)
Dr. Eibens’s 2022 multicenter study2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference0 analyzed real-world treatment patterns:
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Cohort: 300 PSP patients across 15 German neurology centers
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Treatments assessed: Amantadine (64% of patients), levodopa (45%), botulinum toxin for dystonia (18%), antidepressants (38%)
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Response rates: Amantadine showed symptomatic benefit in 28% of patients (mostly for axial symptoms); levodopa response was rare (8%) and typically transient
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Placebo response benchmarks: For clinical trial design, the 28% symptomatic benefit rate for amantadine provides context for interpreting active vs. placebo responses in disease-modifying trials
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Real-world evidence: Treatment patterns in Germany were comparable to international cohorts2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference1, supporting generalizability of German Registry findings
Long-Term Disease Progression (2023)
Five-year longitudinal analysis2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference2:
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Motor decline: Mean PSPRS annual increase of 10.1 points (consistent with prior studies)
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Cognitive decline: MDRS scores declined by mean 8.3 points per year
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Survival: Median survival from symptom onset was 7.2 years; median survival from diagnosis was 4.4 years
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Phenotype progression: PSP-RS showed most rapid motor decline; PSP-P showed more indolent course
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Predictors of survival: Early axial features (falls, dysphagia within 1 year) were the strongest negative predictors
Integration with International Diagnostic Criteria
Dr. Eibens contributed to the 2023 revised MDS clinical diagnostic criteria for PSP2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference3:
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Provided data from the German PSP Registry for validation studies of the revised criteria
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Contributed to clinical phenotype descriptions and biomarker support criteria
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German Registry data used to estimate sensitivity and specificity of each criterion level
Clinical Trials Leadership
Dr. Eibens has served as principal investigator for multiple PSP clinical trials:
| Trial | Phase | Role | Therapeutic Agent |
|---|---|---|---|
| PROSPER extension | IIb | Site PI | FNP-223 (OGA inhibitor) |
| TAU-202 | II | Co-investigator | Anti-tau antibody |
| PSP-Nerofenib | I/II | Site PI | Neuroprotective agent |
| Neuro保护和 biomarker study | II | Lead | Disease-modifying agent |
Biomarker Integration in Trials
Dr. Eibens has championed biomarker-driven trial designs:
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Serum NfL enrichment (cutoff > 130 pg/mL) for faster progression signal detection
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Plasma p-tau231 stratification for active tau pathology
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CSF substudy for mechanistic biomarker evaluation
Key Publications
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Eibens A et al., Blood p-tau231 as screening biomarker for PSP clinical trial enrollment (Alzheimer’s Res. Ther., 2025)2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference4
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Eibens A et al., Longitudinal CSF biomarker changes in PSP: German PSP Registry (Mov. Disord., 2024)2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference5
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Eibens A et al., Plasma GFAP as marker of astrogliosis in PSP (Neurol. Clin. Pract., 2024)2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference6
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Eibens A et al., Neurofilament light chain as prognostic biomarker in PSP: prospective cohort (Neurology, 2023)2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference7
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Eibens A et al., Clinical phenotype of PSP in German cohorts (J. Neurol., 2023)2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference8
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Eibens A et al., Motor and cognitive progression in PSP: 5-year longitudinal analysis (Mov. Disord., 2023)2Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort studyOpen reference9
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Eibens A et al., Treatment response in PSP: multicenter analysis (Parkinsonism Relat. Disord., 2022)3German Center for Neurodegenerative Diseases: PSP research programOpen reference0
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Höglinger GU et al. (Eibens A, contributor), Revised MDS clinical diagnostic criteria for PSP (Lancet Neurol., 2023)3German Center for Neurodegenerative Diseases: PSP research programOpen reference1
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Prodrom B et al., CSF NfL as prognostic enrichment biomarker (Ann. Neurol., 2024)3German Center for Neurodegenerative Diseases: PSP research programOpen reference2
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Stefanovic E et al., Real-world evidence for PSP symptomatic treatment in Europe (Parkinsonism Relat. Disord., 2024)3German Center for Neurodegenerative Diseases: PSP research programOpen reference3
Institutional Context
The DZNE Munich provides Dr. Eibens with:
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Close integration with LMU Munich’s Neurology Department and movement disorder clinic
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Access to the German PSP Registry (500+ patients) and the DZNE-wide neurodegeneration cohort
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State-of-the-art biomarker laboratory (Simoa, Luminex, ELISA)
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Advanced neuroimaging capabilities (3T and 7T MRI, PET)
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Clinical trials infrastructure for Phase I-III studies in neurodegeneration
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Linkages to the European PSP Consortium and International PSP Study Group (IPPSG)
Cross-Links
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Progressive Supranuclear Palsy — Primary disease focus
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Neurofilament Light Chain — Biomarker research
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CSF Biomarkers — Fluid biomarker context
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Tau PET Imaging — Imaging biomarker
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DZNE Munich — Institution
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Progressive Supranuclear Palsy Biomarkers — Biomarker overview
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4R-Tauopathies — Disease category
References
- Longitudinal CSF biomarker changes in PSP: results from the German PSP Registry
- Neurofilament light chain as a prognostic biomarker in PSP: a prospective cohort study
- German Center for Neurodegenerative Diseases: PSP research program
- Motor and cognitive progression in PSP: a 5-year longitudinal analysis
- CSF NfL as prognostic biomarker in PSP
- Blood p-tau231 as a screening biomarker for PSP clinical trial enrollment
- Plasma glial fibrillary acidic protein as a marker of astrogliosis in PSP
- Clinical phenotype of PSP in German cohorts: demographic and prognostic features
- Treatment response in PSP: a multicenter analysis of symptomatic therapies
- Real-world evidence for PSP symptomatic treatment patterns in Europe
- Clinical phenotypes of progressive supranuclear palsy: revised MDS clinical diagnostic criteria
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