# Mosaicism for Autosomal Trisomies: A Comprehensive Analysis of 1266 Published Cases Focusing on Maternal Age and Reproductive History

**Authors:** Natalia V. Kovaleva, Philip D. Cotter

PMC · DOI: 10.3390/genes15060778 · Genes · 2024-06-13

## TL;DR

This study analyzes 1266 cases of mosaic autosomal trisomies, focusing on maternal age and reproductive history to better understand their clinical implications.

## Contribution

The first systematic analysis of demographic data in mosaic trisomy carriers, revealing unexpected patterns in maternal age and reproductive history.

## Key findings

- Advanced maternal age was more common in normal pregnancy outcomes compared to abnormal ones.
- Mothers of postnatally detected mosaicism had higher rates of previous fetal loss compared to prenatal cases.
- Mosaic carriers with uniparental disomy showed significantly higher advanced maternal age proportions than those with biparental disomy.

## Abstract

Mosaicism for autosomal trisomy is uncommon in clinical practice. However, despite its rarity among both prenatally and postnatally diagnoses, there are a large number of characterized and published cases. Surprisingly, in contrast to regular trisomies, no attempts at systematic analyses of mosaic carriers’ demographics were undertaken. This is the first study aimed to address this gap. For that, we have screened more than eight hundred publications on mosaic trisomies, reviewing data including gender and clinical status of mosaic carriers, maternal age and reproductive history. In total, 596 publications were eligible for analysis, containing data on 948 prenatal diagnoses, including true fetal mosaicism (TFM) and confined placental mosaicism (CPM), and on 318 cases of postnatally detected mosaicism (PNM). No difference was found in maternal age between normal pregnancy outcomes with appropriate birth weight and those with intrauterine growth restriction. Unexpectedly, a higher proportion of advanced maternal ages (AMA) was found in normal outcomes compared to abnormal ones (abnormal fetus or newborn) and fetal losses, 73% vs. 56% and 50%, p = 0.0015 and p = 0.0011, correspondingly. Another intriguing finding was a higher AMA proportion in mosaic carriers with concomitant uniparental disomy (UPD) for chromosomes 7, 14, 15, and 16 compared to carriers with biparental disomy (BPD) (72% vs. 58%, 92% vs. 55%, 87% vs. 78%, and 65% vs. 24%, correspondingly); overall figures were 78% vs. 48%, p = 0.0026. Analysis of reproductive histories showed a very poor reporting but almost two-fold higher rate of mothers reporting a previous fetal loss from PNM cohort (in which almost all patients were clinically abnormal) compared to mothers from the TFM and CPM cohorts (with a large proportion of normal outcomes), 30% vs. 16%, p = 0.0072. The occurrence of a previous pregnancy with a chromosome abnormality was 1 in 13 in the prenatal cohort and 1 in 16 in the postnatal cohort, which are five-fold higher compared to published studies on non-mosaic trisomies. We consider the data obtained in this study to be preliminary despite the magnitude of the literature reviewed since reporting of detailed data was mostly poor, and therefore, the studied cohorts do not represent “big data”. Nevertheless, the information obtained is useful both for clinical genetic counseling and for modeling further studies.

## Full-text entities

- **Diseases:** intrauterine growth restriction (MESH:D005317), Mosaicism (MESH:C537822), BPD (MESH:D024182), Autosomal Trisomies (MESH:D014314), chromosome abnormality (MESH:D002869), CPM (MESH:D010922), fetal loss (MESH:D005315)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Full text

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## References

43 references — full list in the complete paper: https://tomesphere.com/paper/PMC11202781/full.md

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Source: https://tomesphere.com/paper/PMC11202781