TY - JOUR
T1 - Plasma amyloid‐beta levels in a pre‐symptomatic dutch‐type hereditary cerebral amyloid angiopathy pedigree
T2 - A cross‐sectional and longitudinal investigation
AU - the Dominantly Inherited Alzheimer Network
AU - Chatterjee, Pratishtha
AU - Tegg, Michelle
AU - Pedrini, Steve
AU - Fagan, Anne M.
AU - Xiong, Chengjie
AU - Singh, Abhay K.
AU - Taddei, Kevin
AU - Gardener, Samantha
AU - Masters, Colin L.
AU - Schofield, Peter R.
AU - Multhaup, Gerhard
AU - Benzinger, Tammie L.S.
AU - Morris, John C.
AU - Bateman, Randall J.
AU - Greenberg, Steven M.
AU - van Buchem, Mark A.
AU - Stoops, Erik
AU - Vanderstichele, Hugo
AU - Teunissen, Charlotte E.
AU - Hankey, Graeme J.
AU - Wermer, Marieke J.H.
AU - Sohrabi, Hamid R.
AU - Martins, Ralph N.
PY - 2021/3/2
Y1 - 2021/3/2
N2 - Plasma amyloid‐beta (Aβ) has long been investigated as a blood biomarker candidate for Cerebral Amyloid Angiopathy (CAA), however previous findings have been inconsistent which could be attributed to the use of less sensitive assays. This study investigates plasma Aβ alterations between pre‐symptomatic Dutch‐type hereditary CAA (D‐CAA) mutation‐carriers (MC) and non-carriers (NC) using two Aβ measurement platforms. Seventeen pre‐symptomatic members of a D‐ CAA pedigree were assembled and followed up 3–4 years later (NC = 8;MC = 9). Plasma Aβ1‐40 and Aβ1‐42 were cross‐sectionally and longitudinally analysed at baseline (T1) and follow‐up (T2) and were found to be lower in MCs compared to NCs, cross‐sectionally after adjusting for covari-ates, at both T1(Aβ1‐40: p = 0.001; Aβ1‐42: p = 0.0004) and T2 (Aβ1‐40: p = 0.001; Aβ1‐42: p = 0.016) employing the Single Molecule Array (Simoa) platform, however no significant differences were observed using the xMAP platform. Further, pairwise longitudinal analyses of plasma Aβ1‐40 revealed decreased levels in MCs using data from the Simoa platform (p = 0.041) and pairwise longitudinal analyses of plasma Aβ1‐42 revealed decreased levels in MCs using data from the xMAP platform (p = 0.041). Findings from the Simoa platform suggest that plasma Aβ may add value to a panel of biomarkers for the diagnosis of pre‐symptomatic CAA, however, further validation studies in larger sample sets are required.
AB - Plasma amyloid‐beta (Aβ) has long been investigated as a blood biomarker candidate for Cerebral Amyloid Angiopathy (CAA), however previous findings have been inconsistent which could be attributed to the use of less sensitive assays. This study investigates plasma Aβ alterations between pre‐symptomatic Dutch‐type hereditary CAA (D‐CAA) mutation‐carriers (MC) and non-carriers (NC) using two Aβ measurement platforms. Seventeen pre‐symptomatic members of a D‐ CAA pedigree were assembled and followed up 3–4 years later (NC = 8;MC = 9). Plasma Aβ1‐40 and Aβ1‐42 were cross‐sectionally and longitudinally analysed at baseline (T1) and follow‐up (T2) and were found to be lower in MCs compared to NCs, cross‐sectionally after adjusting for covari-ates, at both T1(Aβ1‐40: p = 0.001; Aβ1‐42: p = 0.0004) and T2 (Aβ1‐40: p = 0.001; Aβ1‐42: p = 0.016) employing the Single Molecule Array (Simoa) platform, however no significant differences were observed using the xMAP platform. Further, pairwise longitudinal analyses of plasma Aβ1‐40 revealed decreased levels in MCs using data from the Simoa platform (p = 0.041) and pairwise longitudinal analyses of plasma Aβ1‐42 revealed decreased levels in MCs using data from the xMAP platform (p = 0.041). Findings from the Simoa platform suggest that plasma Aβ may add value to a panel of biomarkers for the diagnosis of pre‐symptomatic CAA, however, further validation studies in larger sample sets are required.
KW - Amyloid‐beta
KW - Blood biomarkers
KW - Cerebral amyloid angiopathy
KW - Early diagnosis
KW - Hereditary cerebral haemorrhage with amyloidosis—Dutch type
KW - Plasma amyloid‐beta
KW - Single molecule array platform
UR - http://www.scopus.com/inward/record.url?scp=85102388941&partnerID=8YFLogxK
U2 - 10.3390/ijms22062931
DO - 10.3390/ijms22062931
M3 - Article
C2 - 33805778
AN - SCOPUS:85102388941
SN - 1661-6596
VL - 22
SP - 1
EP - 12
JO - International Journal of Molecular Sciences
JF - International Journal of Molecular Sciences
IS - 6
M1 - 2931
ER -