Differentially Expressed MicroRNAs in Maternal Plasma for the Noninvasive Prenatal Diagnosis of Down Syndrome (Trisomy 21)

Kamhieh-Milz, Julian; Moftah, Reham; Bal, Gürkan; Futschik, Matthias E.; Sterzer, Viktor; Khorramshahi, Omid; Burow, Martin; Thiel, Gundula; Stuke-Sontheimer, Annegret; Chaoui, Rabih; Kamhieh-Milz, Sundrela; Salama, Abdulgabar

doi:10.1155/2014/402475

Cited by 25 publications

(24 citation statements)

References 47 publications

(46 reference statements)

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“…Methods for isolating individual fetal cells [188,189] or examining microRNA [190,191] as well as the isolation of trophoblast cells from cervical smears [187,192] or from embryonic cells after coelocentesis [193] have been described in small study series. Faster and cheaper sequencing techniques could provide new diagnostic possibilities even in the case of small cell numbers or fragments.…”

Section: Discussionmentioning

confidence: 99%

DEGUM, ÖGUM, SGUM and FMF Germany Recommendations for the Implementation of First-Trimester Screening, Detailed Ultrasound, Cell-Free DNA Screening and Diagnostic Procedures

Kozlowski¹,

Burkhardt

Gembruch³

et al. 2018

Ultraschall in Med

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First-trimester screening between 11 + 0 and 13 + 6 weeks with qualified prenatal counseling, detailed ultrasound, biochemical markers and maternal factors has become the basis for decisions about further examinations. It detects numerous structural and genetic anomalies. The inclusion of uterine artery Doppler and PlGF screens for preeclampsia and fetal growth restriction. Low-dose aspirin significantly reduces the prevalence of severe preterm eclampsia. Cut-off values define groups of high, intermediate and low probability. Prenatal counseling uses detection and false-positive rates to work out the individual need profile and the corresponding decision: no further diagnosis/screening - cell-free DNA screening - diagnostic procedure and genetic analysis. In pre-test counseling it must be recognized that the prevalence of trisomy 21, 18 or 13 is low in younger women, as in submicroscopic anomalies in every maternal age. Even with high specificities, the positive predictive values of screening tests for rare anomalies are low. In the general population trisomies and sex chromosome aneuploidies account for approximately 70 % of anomalies recognizable by conventional genetic analysis. Screen positive results of cfDNA tests have to be proven by diagnostic procedure and genetic diagnosis. In cases of inconclusive results a higher rate of genetic anomalies is detected. Procedure-related fetal loss rates after chorionic biopsy and amniocentesis performed by experts are lower than 1 to 2 in 1000. Counseling should include the possible detection of submicroscopic anomalies by comparative genomic hybridization (array-CGH). At present, existing studies about screening for microdeletions and duplications do not provide reliable data to calculate sensitivities, false-positive rates and positive predictive values.

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Section: Discussionmentioning

confidence: 99%

DEGUM, ÖGUM, SGUM and FMF Germany Recommendations for the Implementation of First-Trimester Screening, Detailed Ultrasound, Cell-Free DNA Screening and Diagnostic Procedures

Kozlowski¹,

Burkhardt

Gembruch³

et al. 2018

Ultraschall in Med

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“…However, placenta is not the only determinant of pregnancy-associated miRNA levels in maternal and fetal blood, another source or mechanism influencing these levels is probably involved [29]. Hypothesis that miRNAs are somehow transported from fetus into the maternal circulation and vice versa is still unproven [26].…”

Section: Discussionmentioning

confidence: 99%

“…3) four miRNAs which did not fulfil the above conditions but were reported in the literature as being possibly associated with Down syndrome pathophysiology [26,30,31].…”

Section: Selection Of the Mirna Set For The Validation Studymentioning

confidence: 99%

“…They compared 33 euploid and 23 trisomic pregnancies and found two miRNAs -miR-99a and miR-3156, which were elevated in DS pregnancies. The most comprehensive study so far has been carried out by Kamhieh-Milz et al [26]. A group of 1043 miRNAs were analyzed using high-throughput qPCR SmartChip Human miRNA Panel, nevertheless, a very small number of samples were included (7 DS fetuses; 7 controls).…”

Section: Several Articles Comparing Mirna Levels In Plasma Of Pregnanmentioning

confidence: 99%

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Genome-wide miRNA profiling in plasma of pregnant women with Down syndrome fetuses

Svobodová

Chylíková

Šeda

et al. 2019

Preprint

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Objective: Down syndrome (DS) belongs to the most common causes of mental retardation in men, therefore new approaches allowing its rapid and effective prenatal detection are being explored. In our study we focused on diagnostic potential of plasma microRNAs. We follow up on our previous study in DS placentas, where seven miRNAs were found as being significantly elevated.Methods: A total of 70 first-trimester plasma samples of pregnant women were included to the present study (35 samples with DS fetuses; 35 with euploid fetuses). The genome-wide miRNA profiling was performed in the preliminary study using Affymetrix GeneChip™ miRNA 4.1 Array Strips.Selected miRNAs were then included to the following validation study using qPCR. Results: Based on the current pilot study results (12 miRNAs), our previous research on CVS samples (7 miRNAs) and literature (4 miRNAs), the group of 23 miRNAs were selected for validation study. Although the results of the preliminary study were promising, the following validation step using more sensitive technology RT-PCR and larger group of samples revealed no significant differences in miRNA profiles between compared groups. Conclusion: Our results suggest that testing of the first trimester plasma miRNAs is not suitable for NIPT. Different results could be theoretically achieved at later gestational ages; however, such a result probably would have limited utilization in clinical practice.

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“…As the percentage of mosaicism does not correlate with the severity of congenital anomalies in PKS fetuses (Libotte et al ) other markers of severity and poor outcomes would be helpful. Recently, abnormal extracellular microRNAs (miRNAs) in maternal plasma have been showed early in Down syndrome pregnancies and in those pregnancies complicated by gestational diabetes, preeclampsia, fetal growth restriction (Chiofalo et al ; Kamhieh‐Milz et al ; Lagana’ et al ; Sebastiani et al ). As five miRNAs located on 12p have already been reported to be overexpressed in skin fibroblasts from PKS patients, further studies on maternal plasma miRNAs profile in PKS pregnancies might open a window to identify new potential diagnostic and prognostic biomarkers (Izumi et al ).…”

Section: Approach To Genetic Counseling and Conclusionmentioning

confidence: 99%

Prenatal profile of Pallister‐Killian syndrome: Retrospective analysis of 114 pregnancies, literature review and approach to prenatal diagnosis

Salzano

Raible

Kaur

et al. 2018

American J of Med Genetics Pt A

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Pallister‐Killian syndrome (PKS) is a tissue limited mosaic disorder, characterized by variable degrees of neurodevelopmental delay and intellectual disability, typical craniofacial findings, skin pigmentation anomalies and multiple congenital malformations. The wide phenotypic spectrum of PKS in conjunction with the mosaic distribution of the i(12p) makes PKS an underdiagnosed disorder. Recognition of prenatal findings that should raise a suspicion of PKS is complicated by the fragmentation of data currently available in the literature and challenges in diagnosing a mosaic diagnosis on prenatal testing. Ultrasound anomalies, especially congenital diaphragmatic hernia, congenital heart defects, and rhizomelic limb shortening, have been related to PKS, but they are singularly not specific and are not present in all affected fetuses. We have combined prenatal data from 86 previously published reports and from our cohort of 114 PKS probands (retrospectively reviewed). Summarizing this data we have defined a prenatal growth profile and identified markers of perinatal outcome which collectively provide guidelines for early recognition of the distinctive prenatal profile and consideration of a diagnosis of PKS as well as for management and genetic counseling.

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Differentially Expressed MicroRNAs in Maternal Plasma for the Noninvasive Prenatal Diagnosis of Down Syndrome (Trisomy 21)

Cited by 25 publications

References 47 publications

DEGUM, ÖGUM, SGUM and FMF Germany Recommendations for the Implementation of First-Trimester Screening, Detailed Ultrasound, Cell-Free DNA Screening and Diagnostic Procedures

DEGUM, ÖGUM, SGUM and FMF Germany Recommendations for the Implementation of First-Trimester Screening, Detailed Ultrasound, Cell-Free DNA Screening and Diagnostic Procedures

Genome-wide miRNA profiling in plasma of pregnant women with Down syndrome fetuses

Prenatal profile of Pallister‐Killian syndrome: Retrospective analysis of 114 pregnancies, literature review and approach to prenatal diagnosis

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