High-molecular-weight oligomer tau (HMWoTau) species are dramatically increased in Braak-stage dependent manner in the frontal lobe of human brains, demonstrated by a novel oligomer Tau ELISA with a mouse monoclonal antibody (APNmAb005)

Hiroaki Fukumoto; Tzu-Huei Kao; Chin-Yin Tai; Ming-Kuei Jang; Masaomi Miyamoto

doi:10.1096/fj.202401704R

High-molecular-weight oligomer tau (HMWoTau) species are dramatically increased in Braak-stage dependent manner in the frontal lobe of human brains, demonstrated by a novel oligomer Tau ELISA with a mouse monoclonal antibody (APNmAb005)

FASEB J. 2024 Nov 30;38(22):e70160. doi: 10.1096/fj.202401704R.

Authors

Hiroaki Fukumoto¹, Tzu-Huei Kao¹, Chin-Yin Tai², Ming-Kuei Jang², Masaomi Miyamoto¹

Affiliations

¹ Department of Preclinical Research Division, APRINOIA Therapeutics Inc., Tokyo, Japan.
² APRINOIA Therapeutics Inc., Taipei, China.

Abstract

Disease-specific oligomers Tau assay system is anticipated in Alzheimer disease (AD) to elucidate their etiological roles. We developed a highly sensitive and selective ELISA for high-molecular-weight oligomer tau (HMWoTau) with LLOQ of 0.3 pg/well for the first time, using a novel mouse monoclonal antibody APNmAb005. The target molecule was identified as HMWoTau with circa 2000 kD as a minimum size and the more oligomerized species (>5000 kD), in combination analysis with Size-Exclusion-Chromatography and Sucrose-Density-Gradient-Centrifugation for both recombinant human (rh) Tau-derived aggregates and AD brain-lysates in PBS(-). HMWoTau was labeled by Thioflavin S and visualized as a homogeneous globular particle (about 30 nm in diameter) by two different technologies of atomic force microscopy and dSTORM-Nanoimager. Specific quantitation was also confirmed by immune-absorption, rhHMWoTau-spiked, and cross-reactivity studies. APNmAb005 failed to detect the HMWoTau signal by treatment with DTT/SDS under no influence on the pan-tau antibody, indicating its conformation-specific recognition. APNmAb005-ELISA showed AD-specific and statistically significant ELISA signals from 1 ng brain lysate protein/well. Analysis of the frontal neocortex (N = 40, Braak stage I-VI) by ELISA revealed the detection-limit levels of HMWoTau species at stage I-III, and drastic and statistically significant increases at stage V/VI (AD). By contrast, total Tau and p181 Tau showed 1/4-1/5 levels of AD even at Stage I, while both tau species also showed a statistically significant increase in AD. In sum, our novel APNmAb005-ELISA clarified the disease-specific increase in HMWoTau species and will be useful for not only further etiological elucidation but also the potential diagnostics in AD and relevant tauopathy.

Keywords: APNmAb005; Alzheimer; Braak‐stage; ELISA; HMWoTau; conformation‐specific; globular oligomer; p181Tau; total Tau.

MeSH terms

Aged
Aged, 80 and over
Alzheimer Disease* / metabolism
Alzheimer Disease* / pathology
Animals
Antibodies, Monoclonal* / immunology
Enzyme-Linked Immunosorbent Assay* / methods
Female
Frontal Lobe* / metabolism
Frontal Lobe* / pathology
Humans
Male
Mice
Molecular Weight
tau Proteins* / immunology
tau Proteins* / metabolism

Substances

tau Proteins
Antibodies, Monoclonal

Abstract

MeSH terms

Substances

Grants and funding