Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia

Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia

The incidence of Down syndrome increases with maternal age, and its occurrence varies in different population (1 in 319 to 1 in 1000 live births). Currently, the use of cell-free fetal DNA (cffDNA) from maternal plasma was wide implemented as one of alternatives for non-invasive prenatal screening t...

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Main Authors: Zainuddin, Malaysia, Roslani, Annaliza, Ismail, Rozihan, Muhammad, Siti Aesah @ Naznin, Kaderi, Mohd Arifin, Abdul Ghafar, Nurul Fatehah
Format: Monograph
Language:English
Published: 2019
Subjects:
QH426 Genetics
RG Gynecology and obstetrics
Online Access:http://irep.iium.edu.my/75738/
http://irep.iium.edu.my/75738/1/NZ_Full%20Report_FRGS15-187-0428.pdf
id iium-75738
recordtype eprints
spelling iium-757382019-11-18T06:55:53Z http://irep.iium.edu.my/75738/ Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia Zainuddin, Malaysia Roslani, Annaliza Ismail, Rozihan Muhammad, Siti Aesah @ Naznin Kaderi, Mohd Arifin Abdul Ghafar, Nurul Fatehah QH426 Genetics RG Gynecology and obstetrics The incidence of Down syndrome increases with maternal age, and its occurrence varies in different population (1 in 319 to 1 in 1000 live births). Currently, the use of cell-free fetal DNA (cffDNA) from maternal plasma was wide implemented as one of alternatives for non-invasive prenatal screening test at certain healthcare facilities. This study aims to identify the DNA methylation differences in cffDNA for trisomy 21 detection using a previously developed prediction model based on differentially methylated regions. cffDNA was isolated from 16 pregnant women, including 10 from normal pregnancies, five possible high-risk pregnancies and a confirmed trisomy 21 pregnancy. Each cffDNA extracts were fragmented, immunoprecipitated and quantified by real-time qPCR using three pairs of specific primers for chromosome 21. The calculation of D-value with the cut-off point of zero will determine the status of samples by applying the formula D = -6.331 + 0.959XEP4 +1.188XEP5 +0.424XEP6 +0.621XEP7 +0.028XEP8 + 0.387XEP10– 0.683XEP11 +0.897XEP12, where XEPi = fraction value for each marker. Cases that give a D-value above the cutting point are classified as “trisomy 21” while those with values below the cutting point are classified as “normal”. Interestingly, all our cases were classified as normal, including the confirmed trisomy case. However, this could be due to small number of cases which prevents a better discrimination between the two groups. Hence, a larger number of cases were necessary to obtain statistically validated results. Apart from intervention research, this study aims to assess the knowledge and attitudes of pregnant women on cffDNA-based prenatal diagnosis of trisomy 21 in Kuantan, Pahang. A total of 189 respondents aged 18-45 years old (30.34 ± 0.38) participated. The mean pregnancy weeks was 29.61 ± 9.11. Approximately 53% of the respondents were able to answer correctly more than half of the questions (> 5 of 9) regarding the knowledge of Down Syndrome (mean score 5.6 ± 1.8). As for the knowledge on the prenatal screening, about 48% could answer correctly more than half of the questions (≥6 of 12) with a mean score of 5.5± 3.2. The level of knowledge of Down syndrome was found to be significantly associated with maternal education level (p<0.001) while maternal age was significantly associated with the level of knowledge of Down syndrome prenatal screening (p=0.004). Our results showed our respondents did not have adequate level of knowledge on Down syndrome and its prenatal screening tests. Hence, it is suggested that intervention 2019-10-30 Monograph NonPeerReviewed application/pdf en http://irep.iium.edu.my/75738/1/NZ_Full%20Report_FRGS15-187-0428.pdf Zainuddin, Malaysia and Roslani, Annaliza and Ismail, Rozihan and Muhammad, Siti Aesah @ Naznin and Kaderi, Mohd Arifin and Abdul Ghafar, Nurul Fatehah (2019) Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia. Project Report. UNSPECIFIED. (Unpublished)
repository_type Digital Repository
institution_category Local University
institution International Islamic University Malaysia
building IIUM Repository
collection Online Access
language English
topic QH426 Genetics
RG Gynecology and obstetrics
spellingShingle QH426 Genetics
RG Gynecology and obstetrics
Zainuddin, Malaysia
Roslani, Annaliza
Ismail, Rozihan
Muhammad, Siti Aesah @ Naznin
Kaderi, Mohd Arifin
Abdul Ghafar, Nurul Fatehah
Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia
description The incidence of Down syndrome increases with maternal age, and its occurrence varies in different population (1 in 319 to 1 in 1000 live births). Currently, the use of cell-free fetal DNA (cffDNA) from maternal plasma was wide implemented as one of alternatives for non-invasive prenatal screening test at certain healthcare facilities. This study aims to identify the DNA methylation differences in cffDNA for trisomy 21 detection using a previously developed prediction model based on differentially methylated regions. cffDNA was isolated from 16 pregnant women, including 10 from normal pregnancies, five possible high-risk pregnancies and a confirmed trisomy 21 pregnancy. Each cffDNA extracts were fragmented, immunoprecipitated and quantified by real-time qPCR using three pairs of specific primers for chromosome 21. The calculation of D-value with the cut-off point of zero will determine the status of samples by applying the formula D = -6.331 + 0.959XEP4 +1.188XEP5 +0.424XEP6 +0.621XEP7 +0.028XEP8 + 0.387XEP10– 0.683XEP11 +0.897XEP12, where XEPi = fraction value for each marker. Cases that give a D-value above the cutting point are classified as “trisomy 21” while those with values below the cutting point are classified as “normal”. Interestingly, all our cases were classified as normal, including the confirmed trisomy case. However, this could be due to small number of cases which prevents a better discrimination between the two groups. Hence, a larger number of cases were necessary to obtain statistically validated results. Apart from intervention research, this study aims to assess the knowledge and attitudes of pregnant women on cffDNA-based prenatal diagnosis of trisomy 21 in Kuantan, Pahang. A total of 189 respondents aged 18-45 years old (30.34 ± 0.38) participated. The mean pregnancy weeks was 29.61 ± 9.11. Approximately 53% of the respondents were able to answer correctly more than half of the questions (> 5 of 9) regarding the knowledge of Down Syndrome (mean score 5.6 ± 1.8). As for the knowledge on the prenatal screening, about 48% could answer correctly more than half of the questions (≥6 of 12) with a mean score of 5.5± 3.2. The level of knowledge of Down syndrome was found to be significantly associated with maternal education level (p<0.001) while maternal age was significantly associated with the level of knowledge of Down syndrome prenatal screening (p=0.004). Our results showed our respondents did not have adequate level of knowledge on Down syndrome and its prenatal screening tests. Hence, it is suggested that intervention
format Monograph
author Zainuddin, Malaysia
Roslani, Annaliza
Ismail, Rozihan
Muhammad, Siti Aesah @ Naznin
Kaderi, Mohd Arifin
Abdul Ghafar, Nurul Fatehah
author_facet Zainuddin, Malaysia
Roslani, Annaliza
Ismail, Rozihan
Muhammad, Siti Aesah @ Naznin
Kaderi, Mohd Arifin
Abdul Ghafar, Nurul Fatehah
author_sort Zainuddin, Malaysia
title Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia
title_short Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia
title_full Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia
title_fullStr Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia
title_full_unstemmed Identifying the DNA methylation differences in cell-free fetal DNA: an approach towards non-invasive prenatal diagnosis of trisomy 21 in Malaysia
title_sort identifying the dna methylation differences in cell-free fetal dna: an approach towards non-invasive prenatal diagnosis of trisomy 21 in malaysia
publishDate 2019
url http://irep.iium.edu.my/75738/
http://irep.iium.edu.my/75738/1/NZ_Full%20Report_FRGS15-187-0428.pdf
first_indexed 2023-09-18T21:47:09Z
last_indexed 2023-09-18T21:47:09Z
_version_ 1777413525677801472

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