Characterization of a Conformation-Restricted Amyloid β Peptide and Immunoreactivity of Its Antibody in Human AD brain

Yusuke Kageyama(Shiga University of Medical Science), Yumi Irie(Kyoto University), Yuka Matsushima(Kyoto University), Tatsuya Segawa(Medical & Biological Laboratories (Japan)), Jean‐Pierre Bellier(Shiga University of Medical Science), Kumi Hidaka(Kyoto University), Hiroshi Sugiyama(Kyoto University), Daita Kaneda(Fukushimura Hospital), Yoshio Hashizume(Fukushimura Hospital), Hiroyasu Akatsu(Nagoya City University), Kunio Miki(Kyoto University), Akiko Kita(Kyoto University), Douglas G. Walker(Shiga University of Medical Science), Kazuhiro Irie(Kyoto University), Ikuo Tooyama(Shiga University of Medical Science)
ACS Chemical Neuroscience
August 31, 2021
Cited by 18Open Access
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Abstract

. Thioflavin T binding assays, nondenaturing gel electrophoresis, and morphological analyses revealed that SS-Aβ42 maintained oligomeric structure, whereas wild-type Aβ42 and the highly aggregative Aβ42 mutant with E22P substitution (E22P-Aβ42) formed Aβ fibrils. In agreement with these observations, SS-Aβ42 was more cytotoxic compared to the wild-type and E22P-Aβ42 in cell cultures. Furthermore, we developed a monoclonal antibody, designated TxCo-1, using the toxic conformation of SS-Aβ42 as immunogen. X-ray crystallography of the TxCo-1/SS-Aβ42 complex, enzyme immunoassay, and immunohistochemical studies confirmed the recognition site and specificity of TxCo-1 to SS-Aβ42. Immunohistochemistry with TxCo-1 antibody identified structures resembling senile plaques and vascular Aβ in brain samples of AD subjects. However, TxCo-1 immunoreactivity did not colocalize extensively with Aβ plaques identified with conventional Aβ antibodies. Together, these findings indicate that Aβ with a turn at positions 22 and 23, which is prone to form Aβ oligomers, could show strong cytotoxicity and accumulated in brains of AD subjects. The SS-Aβ42 and TxCo-1 antibody should facilitate understanding of the pathological role of Aβ with toxic conformation in AD.


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