2022
DOI: 10.1002/dad2.12307
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Plasma p217+tau versus NAV4694 amyloid and MK6240 tau PET across the Alzheimer's continuum

Abstract: Introduction We evaluated a new Simoa plasma assay for phosphorylated tau (P‐tau) at aa217 enhanced by additional p‐tau sites (p217+tau). Methods Plasma p217+tau levels were compared to 18 F‐NAV4694 amyloid beta (Aβ) positron emission tomography (PET) and 18 F‐MK6240 tau PET in 174 cognitively impaired (CI) and 223 cognitively unimpaired (CU) participants. Results Compared to Aβ− CU, the p… Show more

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Cited by 32 publications
(47 citation statements)
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“…3 To that end, our results are encouraging, as we observed strong relationships between plasma pTau 217 and concurrent brain imaging biomarkers of AD, with an AUC of approximately 0.91 for identifying PiB+ participants, and 0.95 for identifying those who were MK+. These values are similar to those seen for the easier task of discriminating AD A𝛽𝛽 + from CU A𝛽𝛽 − groups, and are high compared to other reports describing cognitively unimpaired elderly groups in AIBL, 11 MCSA, 24 and BioFINDER. 46 With our threshold for predicting PiB+, the PPV of pTau 217 was 0.58, which would reduce the number needed to screen to obtain a full sample.…”
Section: Discussionsupporting
confidence: 88%
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“…3 To that end, our results are encouraging, as we observed strong relationships between plasma pTau 217 and concurrent brain imaging biomarkers of AD, with an AUC of approximately 0.91 for identifying PiB+ participants, and 0.95 for identifying those who were MK+. These values are similar to those seen for the easier task of discriminating AD A𝛽𝛽 + from CU A𝛽𝛽 − groups, and are high compared to other reports describing cognitively unimpaired elderly groups in AIBL, 11 MCSA, 24 and BioFINDER. 46 With our threshold for predicting PiB+, the PPV of pTau 217 was 0.58, which would reduce the number needed to screen to obtain a full sample.…”
Section: Discussionsupporting
confidence: 88%
“…1,2 The utility and convenience of an accurate blood test has clear implications for accelerating and improving clinical research and practice. [1][2][3][4] Several candidate markers exist including massspectrometry [5][6][7] and immunoassay 8 measured A𝛽𝛽 42 and A𝛽𝛽 40 and their ratio, and phosphorylated tau at threonine 217 (pTau 217 ), 9 181 (pTau 181 ), 10 and other phosphorylated sites, 11 as well as non-specific markers of neurodegeneration and astrogliosis, including neurofilament light (NfL) 12,13 and glial fibrillary acidic protein (GFAP). [14][15][16] Recently, interest has turned to pTau 217 , as cerebrospinal fluid levels increase early in autosomal dominant AD 17 and better discriminate AD from non-AD subgroups of cognitively impaired adults, compared to pTau 181 .…”
Section: Introductionmentioning
confidence: 99%
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