# Mosaic Loss of Chromosome Y and Plasma Aβ42/p‐tau181 Ratio as Biomarkers for Alzheimer's Disease in the Midwestern Amish

**Authors:** Yeunjoo E. Song, Ping Wang, Renee A. Laux, Sarada L. Fuzzell, Sherri D. Hochstetler, Kristy L. Miskimen, Audrey Lynn, Weihuan Wang, Yining Liu, Noel C. Moore, Alex V. Gulyayev, Daniel A. Dorfsman, Laura J. Caywood, Jason E. Clouse, Sharlene D. Herington, Michael B. Prough, Susan H. Slifer, Larry D Adams, Patrice G Whitehead, Jeffery M Vance, Michael L Cuccaro, Paula K. Ogrocki, Alan J. Lerner, Margaret Pericak‐Vance, William K. Scott, William S Bush, Jonathan L Haines

PMC · DOI: 10.1002/alz70856_106620 · Alzheimer's & Dementia · 2026-01-08

## TL;DR

The study explores how two biomarkers, mLOY and APR, relate to Alzheimer's disease in Amish males, finding they help distinguish cognitive impairment.

## Contribution

The study identifies mLOY and APR as complementary biomarkers for Alzheimer's disease in a unique Amish population.

## Key findings

- mLOY was more common in cognitively impaired Amish males but not statistically significant.
- APR improved discrimination of Alzheimer's disease with an increased area under the curve.

## Abstract

In aging men, mosaic loss of chromosome Y (mLOY) is a possible biomarker for increased risk of disease, including Alzheimer disease (AD). We previously reported mLOY increased with age and carriers of mLOY had an increased risk of AD. We also found plasma Aβ42/p‐tau181 ratio (APR) was significantly lower among AD Amish individuals compared to cognitively‐unimpaired (CU) individuals. We now examine how these two biomarkers interplay with cognitive status in Amish males.

mLOY was determined using the Mosaic Chromosomal Alterations(MoChA) pipeline. Extensive QC was done for both mLOY and plasma biomarker measures. Consensus review of medical history and neuropsychological testing categorized individuals into AD, Mild‐cognitive‐impairment (MCI) or Cognitive‐impairment‐not‐AD (CINAD) or CU. The cognitively‐impaired (CI) group combined AD, MCI and CINAD. We compared 1) CI to CU and 2) AD to CU. Correlation between APR and mLOY were estimated accounting for relatedness. Receiver operating characteristic analysis was performed to evaluate the discriminatory ability of the two biomarkers compared to the baseline model with age and presence/absence of APOE ε4 alleles. p‐value <0.05 was noted as statistically significant.

249 males (mean age=82.89±5.57) had measurements for both biomarkers. Of these, a subset had consensus diagnoses AD (n = 30; mean age=85.63±5.31), CINAD, MCI or CU (n = 105; mean age=82.01±5.36). The mean age of 82 CI individuals was 84.34±4.73. mLOY was observed in 20.1% of CU vs. 29.3% of CI (p‐value=0.23). APR was significantly negatively correlated with CI and AD as expected, was positively correlated with mLOY but not significantly and remained positively correlated when stratified, with the stronger correlation in AD. For AD, the area under the curve (AUC) improved from 0.70 to 0.82 with the inclusion of APR, with mLOY showing little effect. For CI, AUC improved from 0.63 to 0.68 by including mLOY, with no independent effect of APR. When including both in the model, AUC improves from 0.63 to 0.69.

We observed two promising biomarkers of AD, mLOY and APR, both contribute discriminating AD and CI but differently. This and the stringer correlation in AD may indicate they are more specific to AD than non‐specific CI.

## Linked entities

- **Diseases:** Alzheimer disease (MONDO:0004975)

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Source: https://tomesphere.com/paper/PMC12780748