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Comparative analyses of plasma amyloid-β levels in heterogeneous and monomerized states by interdigitated microelectrode sensor system.

Young Soo KimYong Kyoung YooHye Yun KimJee Hoon RohJinsik KimSeungyeop BaekJinny Claire LeeHye Jin KimMyung-Sic ChaeDahye JeongDongsung ParkSejin LeeHoChung JangKyeonghwan KimJeong Hoon LeeByung Hyun ByunSu Yeon ParkJeong Ho HaKyo Chul LeeWon Woo ChoJae-Seung KimJae-Young KohSang Moo LimKyo Seon Hwang
Published in: Science advances (2019)
Detection of amyloid-β (Aβ) aggregates contributes to the diagnosis of Alzheimer disease (AD). Plasma Aβ is deemed a less invasive and more accessible hallmark of AD, as Aβ can penetrate blood-brain barriers. However, correlations between biofluidic Aβ concentrations and AD progression has been tenuous. Here, we introduce a diagnostic technique that compares the heterogeneous and the monomerized states of Aβ in plasma. We used a small molecule, EPPS [4-(2-hydroxyethyl)-1-piperazinepropanesulfonic acid], to dissociate aggregated Aβ into monomers to enhance quantification accuracy. Subsequently, Aβ levels of EPPS-treated plasma were compared to those of untreated samples to minimize inter- and intraindividual variations. The interdigitated microelectrode sensor system was used to measure plasma Aβ levels on a scale of 0.1 pg/ml. The implementation of this self-standard blood test resulted in substantial distinctions between patients with AD and individuals with normal cognition (NC), with selectivity and sensitivity over 90%.
Keyphrases
  • small molecule
  • white matter
  • mild cognitive impairment
  • deep brain stimulation
  • blood brain barrier
  • protein protein
  • quantum dots
  • cerebral ischemia