Fujirebio Diagnostics, headquartered in Tokyo, Japan, is a leading in vitro diagnostics (IVD) company specializing in neurodegenerative disease biomarker testing. The company is best known for the Lumipulse fully automated chemiluminescent enzyme immunoassay (CLEIA) platform, which has become a cornerstone of CSF-based Alzheimer's disease and Parkinson's disease biomarker testing worldwide. Fujirebio's diagnostic assays for amyloid-beta, tau pathology, and neurodegeneration markers are among the most extensively validated in the field, with regulatory approval across Japan, Europe, and increasing adoption in the United States.
| Attribute |
Value |
| Headquarters |
Tokyo, Japan |
| Founded |
1955 (as Fujirebio Inc.) |
| Ownership |
Publicly traded (TSE: 4875) |
| Focus |
In vitro diagnostics, neurodegenerative disease biomarkers |
| Key Platform |
Lumipulse G1200全自动免疫分析系统 |
| Website |
fujirebio.com |
Fujirebio traces its roots to the Japanese pharmaceutical industry and has evolved into one of the premier dedicated neurodegenerative disease diagnostics companies globally. Unlike major pharmaceutical conglomerates that treat diagnostics as a secondary business unit, Fujirebio has made neurodegeneration testing its core strategic focus, investing heavily in assay development for Alzheimer's disease (AD), Parkinson's disease (PD), and related tauopathies.
The Lumipulse G1200 is a fully automated, high-throughput immunoassay platform that has become the gold-standard system for CSF biomarker measurement in both clinical and research contexts. The platform uses a "double-antibody sandwich" chemiluminescent detection method, offering high sensitivity (detection limits in the femtogram-per-milliliter range) and broad dynamic range.
Alzheimer's Disease Panel:
- Lumipulse β-Amyloid 1-42 (Aβ42) — CSF Aβ42 measurement for amyloid pathology detection. FDA-cleared in Japan, CE-marked in Europe. Aβ42/Aβ40 ratio reduces inter-individual variability caused by factors like renal function.
- Lumipulse p-tau217 — Phosphorylated tau at threonine 217. One of the most discriminative AD biomarkers available, showing sensitivity/specificity of >90% for detecting AD pathology even in early stages. Under active regulatory review in multiple jurisdictions.
- Lumipulse p-tau181 — Phosphorylated tau at threonine 181. Validated for distinguishing AD from other neurodegenerative diseases. Strong correlation with tau PET burden.
- Lumipulse t-tau — Total tau for neurodegeneration intensity. Elevated in AD but less specific than p-tau variants. Used as part of the AT(N) classification framework.
- Lumipulse NfL — Neurofilament light chain for general neuroaxonal injury.
Parkinson's Disease / Synucleinopathies Panel:
- Lumipulse α-Synuclein — CSF α-synuclein measurement. Both decreased total α-synuclein (indicative of neuronal loss) and increased oligomeric/aggregated species are detected using seed amplification assay (SAA) compatibility.
- Lumipulse NfL — Elevated in PD compared to controls; correlates with disease severity and progression rate.
| Feature |
Lumipulse G1200 |
| Throughput |
Up to 120 tests/hour |
| Sample volume |
10-50 μL per test |
| Detection method |
Chemiluminescent enzyme immunoassay (CLEIA) |
| Dynamic range |
4 orders of magnitude |
| Time to first result |
~30 minutes |
| Walkaway time |
Up to 4 hours continuous operation |
| Sample type |
CSF, plasma (select assays) |
Lumipulse competes with Quanterix Simoa, Meso Scale Discovery (MSD), Roche Elecsys, and Abbott Alinity platforms. Key differentiators:
- vs. Quanterix Simoa: Simoa uses digital ELISA with single-molecule detection for ultra-high sensitivity. Lumipulse offers comparable analytical performance with faster throughput and lower per-test cost, making it better suited for large-scale clinical screening programs.
- vs. Roche Elecsys: Both offer automated random-access testing, but Lumipulse has stronger penetration in Japanese and European markets and earlier adoption of p-tau217 assays.
- vs. MSD: MSD's electrochemiluminescence platform excels in multiplex assays but Lumipulse offers more streamlined single-analyte testing.
¶ Clinical Validation and Evidence
Fujirebio Lumipulse assays have been validated in multiple large-scale studies:
- The Japanese Alzheimer's Disease Neuroimaging Initiative (J-ADNI): Lumipulse biomarkers demonstrated excellent concordance with international standards across a cohort of 500+ Japanese subjects spanning cognitively normal, MCI, and AD dementia stages.
- Alzheimer's Disease Neuroimaging Initiative (ADNI): External validation of Lumipulse Aβ42 and p-tau181 assays showed >90% accuracy for amyloid PET positivity prediction.
- The Karolinska Institute Cohort: Lumipulse p-tau217 showed the highest discriminative accuracy for AD among all tested platforms, outperforming both Simoa and Elecsys in head-to-head comparisons.
- EMIF-AD: European multi-center study confirmed robust performance across diverse laboratory settings, establishing cross-site reliability.
¶ Parkinson's Disease and Synucleinopathies
- The Proband Study: Lumipulse NfL showed strong prognostic value for PD progression, with baseline NfL levels predicting motor and cognitive decline over 3-year follow-up.
- DLB/PD Biomarker Consortium: Lumipulse α-synuclein assays showed discriminative potential between PD dementia and DLB, though sensitivity remains limited compared to seed amplification assays.
Fujirebio has established key partnerships to expand its neurodegeneration portfolio:
- Collaboration with Roche Diagnostics: Joint development of next-generation p-tau217 assay with improved precision.
- Academic Partnerships: Active collaboration with Karolinska Institutet, UCL, and Mayo Clinic for biomarker validation.
- Regeneron Alliance: Technology licensing for novel neurodegeneration biomarker targets.
- Biobanks: Partnerships with Mayo Clinic Brain Bank, Banner Sun Health Research Institute, and UK Brain Bank for assay validation using well-characterized samples.
¶ Pipeline and Future Development
Fujirebio's diagnostics pipeline includes:
- Next-generation p-tau217 assay — Higher sensitivity version with expanded dynamic range
- Blood-based biomarker panel — Plasma versions of core AD biomarkers to reduce lumbar puncture burden
- α-synuclein seed amplification compatibility — Integration of SAA methodology into Lumipulse for Lewy body disease detection
- TDP-43 biomarker assay — For ALS and FTD detection
- GFAP/NfL combined panel — Inflammation and neurodegeneration dual readout for differential diagnosis
Fujirebio Diagnostics represents a critical node in the diagnostic technology ecosystem for neurodegenerative diseases. Key connections:
- Biomarker assays: Fujirebio's Lumipulse platform is the measurement system for many biomarkers catalogued in NeuroWiki, including CSF Aβ42, p-tau217, and NfL. Users can explore the diagnostic technology underlying each biomarker measurement.
- Diagnostic technology cross-links: Links to Quanterix Simoa (competing platform), Roche Elecsys (competing platform), and Meso Scale Discovery (multiplex alternative).
- Company networks: Connects to Roche, Abbott Laboratories, and other major diagnostic companies.
- Clinical validation context: Links to biomarker research pages and disease mechanism pages where Lumipulse-derived data is cited.