Feasibility and acceptance of screening for fragile X mutations in low-risk pregnancies

Ryynänen, Markku; Heinonen, Seppo; Makkonen, M.; Kajanoja, Elisa; Mannermaa, Arto; Kirkinen, Pertti

doi:10.1038/sj.ejhg.5200285

Cited by 68 publications

(102 citation statements)

References 21 publications

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“…Follow-up interviews with a sub-group of women from this study revealed, however, that women had trouble relating to the clinical information about FXS and wanted to know more about families' experiences of FXS (Archibald et al 2009). No harms to psychological wellbeing have been demonstrated to date, although only three studies have specifically investigated the impact of offering screening on psychological factors such as anxiety (Ryynanen et al 1999;Fanos et al 2006;Metcalfe et al 2008).…”

Section: Carrier Screening For Fragile X Syndromementioning

confidence: 79%

“…The majority were with pregnant women (Berkenstadt et al 2007;Cronister et al 2005;Fanos et al 2006;Huang et al 2003;Pesso et al 2000;Spence et al 1996;Ryynanen et al 1999;Toledano-Alhadef et al 2001;Kallinen et al 2001), while some included relatively smaller numbers of nonpregnant women (Pesso et al 2000;Spence et al 1996;Toledano-Alhadef et al 2001;Berkenstadt et al 2007;Geva et al 2000). Most studies essentially focused on the uptake of testing, with rates varying between 7.9% ) and 21% (Spence et al 1996) in the USA, 80% in Israel (Pesso et al 2000), and 85% (Ryynanen et al 1999) and 92% respectively in two Finnish studies (Kallinen et al 2001).…”

Section: Carrier Screening For Fragile X Syndromementioning

confidence: 99%

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Carrier screening in preconception consultation in primary care

Metcalfe

2011

J Community Genet

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Discussing carrier screening during preconception consultation in primary care has a number of advantages in terms of promoting autonomy and enabling the greatest range of reproductive choices. For those with a family history of an inherited condition, this ought to be a routine discussion; however, this can be expanded to include the wider population, especially for those conditions for which carrier frequencies are considered relatively common. There is published literature from around the world regarding experiences with carrier screening in primary care for cystic fibrosis, haemoglobinopathies, fragile X syndrome, Tay-Sachs disease and spinal muscular atrophy, although many of these have tended to focus on consultations during rather than before pregnancy. Overall, these studies reveal that population carrier screening is well received by the participants with apparent minimal psychosocial harms; however, challenges exist in terms of approaches to ensure couples receive adequate information to make personally relevant decisions and for ongoing health professional engagement.

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Section: Carrier Screening For Fragile X Syndromementioning

confidence: 79%

Section: Carrier Screening For Fragile X Syndromementioning

confidence: 99%

Carrier screening in preconception consultation in primary care

Metcalfe

2011

J Community Genet

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“…Dig-labeled DNA molecular weight Marker V (Roche Diagnostics) and a known size marker were used as size standards. Filters were hybridized overnight at 42°C in roller bottles (Isotemp; Fisher Scientific) in Dig Easy Hybridization Buffer (Roche Diagnostics) with a Dig-end-labeled oligonucleotide probe [(CGG) 10 ] and Dig-labeled pBR322 DNA. Filters were washed at room temperature, twice for 5 minutes with 2ϫ SSC/0.1% SDS (100 ml) and twice for 7 minutes in a larger volume (400 ml) with the same washing solution, followed by two washes of 25 minutes, each in 0.5ϫ SSC/0.1 SDS at 45°C.…”

Section: Southern Blot and Pcr Analysismentioning

confidence: 99%

A Rapid Polymerase Chain Reaction-Based Screening Method for Identification of All Expanded Alleles of the Fragile X (FMR1) Gene in Newborn and High-Risk Populations

Tassone

Pan

Amiri

et al. 2008

The Journal of Molecular Diagnostics

340

363

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Fragile X syndrome , the most common inherited cause of intellectual impairment and the most common single gene associated with autism , generally occurs for fragile X mental retardation 1 (FMR1) alleles that exceed 200 CGG repeats (full-mutation range). Currently, there are no unbiased estimates of the number of full-mutation FMR1 alleles in the general population; a major obstacle is the lack of an effective screening tool for expanded FMR1 alleles in large populations. We have developed a rapid polymerase chain reaction (PCR)-based screening tool for expanded FMR1 alleles. The method utilizes a chimeric PCR primer that targets randomly within the expanded CGG region , such that the presence of a broad distribution of PCR products represents a positive result for an expanded allele. The method is applicable for screening both males and females and for allele sizes throughout the premutation (55 to 200 CGG repeats) and full-mutation ranges. Furthermore , the method is capable of rapid detection of expanded alleles using as little as 1% of the DNA from a single dried blood spot. The methodology presented in this work is suitable for screening large populations of newborn or those at high risk (eg , autism , premature ovarian failure , ataxia , dementia) for expanded FMR1 alleles. The test described herein costs less than $5 per sample for materials; with suitable scale-up and automation , the cost should approach $1 per sample. (J Mol

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“…The need for appropriate education and genetic counseling has been emphasized as has the importance of research exploring psychosocial impacts of such screening (Finucane et al 2012;Sherman et al 2005). Research indicates that population screening for FXS is generally perceived favorably by families and healthcare providers (Acharya and Ross 2009;Archibald et al 2013;Ryynanen et al 1999;Skinner et al 2003) as well as individuals offered screening in research contexts (Anido et al 2005(Anido et al , 2007Archibald et al 2009;Fanos et al 2006;Metcalfe et al 2008;Sherman et al 2005), and there appears to be a preference for screening offered before pregnancy (Acharya and Ross 2009;Archibald et al 2013;Skinner et al 2003). As carrier screening approaches have varied, there is no clear consensus on how best to deliver population-based carrier screening for FXS.…”

Section: Introductionmentioning

confidence: 99%

“It gives them more options”: preferences for preconception genetic carrier screening for fragile X syndrome in primary healthcare

et al. 2016

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This study aims to explore stakeholder views about offering population-based genetic carrier screening for fragile X syndrome. A qualitative study using interviews and focus groups with stakeholders was undertaken to allow for an indepth exploration of views and perceptions about practicalities of, and strategies for, offering carrier screening for fragile X syndrome to the general population in healthcare settings. A total of 188 stakeholders took part including healthcare providers (n = 81), relatives of people with fragile X syndrome (n = 29), and members of the general community (n = 78). The importance of raising community awareness about screening and providing appropriate support for carriers was emphasized. There was a preference for preconception carrier screening and for providing people with the opportunity to make an informed decision about screening. Primary care was highlighted as a setting which would ensure screening is accessible; however, challenges of offering screening in primary care were identified including time to discuss screening, knowledge about the test and possible outcomes, and the health professionals' approach to offering screening. With the increasing availability of genetic carrier tests, it is essential that research now focuses on evaluating approaches for the delivery of carrier screening programs. Primary healthcare is perceived as an appropriate setting through which to access the target population, and raising awareness is essential to making genetic screening more accessible to the general community.

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Feasibility and acceptance of screening for fragile X mutations in low-risk pregnancies

Cited by 68 publications

References 21 publications

Carrier screening in preconception consultation in primary care

Carrier screening in preconception consultation in primary care

A Rapid Polymerase Chain Reaction-Based Screening Method for Identification of All Expanded Alleles of the Fragile X (FMR1) Gene in Newborn and High-Risk Populations

“It gives them more options”: preferences for preconception genetic carrier screening for fragile X syndrome in primary healthcare

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