Alyafee Yusra, Al Tuwaijri Abeer, Umair Muhammad, Alharbi Mashael, Haddad Shahad, Ballow Maryam, Alayyar Latifah, Alam Qamre, Althenayyan Saleh, Al Ghilan Nadia, Al Khaldi Aziza, Faden Majid S, Al Sufyan Hamad, Alfadhel Majid
Medical Genomics Research Department, King Abdullah International Medical Research Center (KAIMRC), King Saud Bin Abdulaziz University for Health Sciences, King Abdulaziz Medical City, Ministry of National Guard Health Affairs, Riyadh, Saudi Arabia.
Clinical Laboratory Sciences Department, College of Applied Medical Sciences, King Saud Bin Abdulaziz University for Health Sciences (KSAU-HS), Riyadh, Saudi Arabia.
Front Genet. 2022 Nov 3;13:1047474. doi: 10.3389/fgene.2022.1047474. eCollection 2022.
In pregnant women at risk of autosomal recessive (AR) disorders, prenatal diagnosis of AR disorders primarily involves invasive procedures, such as chorionic villus sampling and amniocentesis. We collected blood samples from four pregnant women in their first trimester who presented a risk of having a child with an AR disorder. Cell-free DNA (cfDNA) was extracted, amplified, and double-purified to reduce maternal DNA interference. Additionally, whole-genome amplification was performed for traces of residual purified cfDNA for utilization in subsequent applications. Based on our findings, we detected the fetal status with the family corresponding different genes, i.e., , , , , and , as homozygous affected, wild-type, and heterozygous carriers, respectively. Results were subsequently confirmed by prenatal amniocentesis. The results of AmpFLSTR™ Identifiler™ presented a distinct profile from the corresponding mother profile, thereby corroborating the result reflecting the genetic material of the fetus. Herein, we detected AR disease mutations in the first trimester of pregnancy while surmounting limitations associated with maternal genetic material interference. Importantly, such detection strategies would allow the screening of pregnant women for common AR diseases, especially in highly consanguineous marriage populations. This technique would open avenues for the early detection and prevention of recessive diseases among the population.
对于有常染色体隐性(AR)疾病风险的孕妇,AR疾病的产前诊断主要涉及侵入性操作,如绒毛取样和羊膜穿刺术。我们收集了四名孕早期有生育患AR疾病孩子风险的孕妇的血样。提取、扩增并对游离DNA(cfDNA)进行双重纯化以减少母体DNA干扰。此外,对痕量残留纯化cfDNA进行全基因组扩增以供后续应用。基于我们的发现,我们利用对应不同基因检测胎儿状态,即, , , ,和 ,分别为纯合患病、野生型和杂合携带者。随后通过产前羊膜穿刺术证实结果。AmpFLSTR™ Identifiler™的结果呈现出与相应母亲图谱不同的图谱,从而证实了反映胎儿遗传物质的结果。在此,我们在妊娠早期检测到AR疾病突变,同时克服了与母体遗传物质干扰相关的局限性。重要的是,这种检测策略将允许对孕妇进行常见AR疾病的筛查,尤其是在近亲结婚人群中。这项技术将为人群中隐性疾病的早期检测和预防开辟道路。
