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Journal of Genetic Counseling
Published in: Journal of Genetic Counseling 6/2014

01-12-2014 | Original Research

Client Views and Attitudes to Non-Invasive Prenatal Diagnosis for Sickle Cell Disease, Thalassaemia and Cystic Fibrosis

Authors: Melissa Hill, Cecilia Compton, Madhavi Karunaratna, Celine Lewis, Lyn Chitty

Published in: Journal of Genetic Counseling | Issue 6/2014

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Abstract

In the near future the availability of non-invasive prenatal diagnosis (NIPD) for single gene disorders will change the prenatal diagnosis options available to couples who are carriers of conditions such as cystic fibrosis, sickle cell disorder and thalassaemia. Client opinions about NIPD are needed to inform the implementation of NIPD for single gene disorders. This qualitative study used two focus groups (n = 12) and one-to-one interviews (n = 16) with carriers and support group representatives of sickle cell disease, thalassaemia and cystic fibrosis. Discussions were digitally recorded, transcribed verbatim and analysed using thematic analysis. Opinions about NIPD were very positive and participants valued the opportunity to have safe and early testing. Uptake of prenatal testing is likely to increase as women who had previously declined invasive testing expressed interest in having NIPD. Participant concerns about NIPD centred on the need for accuracy to be high to be used for subsequent decision making about termination of pregnancy. Participants also raised concerns that less thought may be given to having a blood test compared to an invasive test and that the perceived ease of a blood test may bring increased pressure to have testing. Participants thought NIPD should be offered through existing specialist services to ensure appropriate genetic counseling and support. Maintaining all testing options is important as some people may prefer invasive testing over NIPD if invasive testing was more accurate or if invasive testing could give information about other conditions such as Down syndrome.
Literature
Barrett, A. N., McDonnell, T. C., Chan, K. C., & Chitty, L. S. (2012). Digital PCR analysis of maternal plasma for noninvasive detection of sickle cell anemia. Clinical Chemistry, 58(6), 1026–1032.PubMedCrossRef
Braun, V., & Clarke, V. (2006). Using thematic analysis in psychology. Qualitative Research in Psychology, 3, 77–101.CrossRef
Bustamante-Aragones, A., Rodriguez de Alba, M., Perlado, S., Trujillo-Tiebas, M. J., Arranz, J. P., Diaz-Recasens, J., et al. (2012). Non-invasive prenatal diagnosis of single-gene disorders from maternal blood. Gene, 504(1), 144–149.PubMedCrossRef
Chitty, L. S., Griffin, D. R., Meaney, C., Barrett, A., Khalil, A., Pajkrt, E., et al. (2011). New aids for the non-invasive prenatal diagnosis of achondroplasia: dysmorphic features, charts of fetal size and molecular confirmation using cell-free fetal DNA in maternal plasma. Ultrasound in Obstetrics and Gynecology, 37(3), 283–289.PubMedCrossRef
Chitty, L. S., Khalil, A., Barrett, A. N., Pajkrt, E., Griffin, D. R., & Cole, T. J. (2013). Safe, accurate, prenatal diagnosis of thanatophoric dysplasia using ultrasound and free fetal DNA. Prenatal Diagnosis, 33(5), 416–423.PubMedCentralPubMedCrossRef
Clinical Molecular Genetics Society (CMGS) (2013). Audit 2011–2012. Available from http://www.cmgs.org/CMGS%20audit/2012%20audit/CMGSAudit11_12_FINAL.pdf, Accessed May 2013.
de Jong, A., Dondorp, W. J., de Die-Smulders, C. E., Frints, S. G., & de Wert, G. M. (2010). Non-invasive prenatal testing: ethical issues explored. European Journal of Human Genetics, 18(3), 272–277.PubMedCentralPubMedCrossRef
de Jong, A., Dondorp, W. J., Frints, S. G., de Die-Smulders, C. E., & de Wert, G. M. (2011). Advances in prenatal screening: the ethical dimension. Nature Reviews Genetics, 12(9), 657–663.PubMedCrossRef
Deans, Z., & Newson, A. J. (2011). Should non-invasiveness change informed consent procedures for prenatal diagnosis? Health Care Analysis, 19(2), 122–132.PubMedCrossRef
Deans, Z., Hill, M., Chitty, L. S., & Lewis, C. (2013). Non-invasive prenatal testing for single gene disorders: exploring the ethics. European Journal of Human Genetics, 21(7), 713–718.PubMedCentralPubMedCrossRef
Dormandy, E., Gulliford, M., Bryan, S., Roberts, T. E., Calnan, M., Atkin, K., et al. (2010). Effectiveness of earlier antenatal screening for sickle cell disease and thalassaemia in primary care: cluster randomised trial. BMJ, 341, c5132.PubMedCentralPubMedCrossRef
D'Souza, E., Sawant, P. M., Nadkarni, A. H., Gorakshakar, A., Ghosh, K., & Colah, R. B. (2013). Detection of fetal mutations causing hemoglobinopathies by non-invasive prenatal diagnosis from maternal plasma. Journal of Postgraduate Medicine, 59(1), 15–20.PubMedCrossRef
Hall, A., Bostanci, A., & Wright, C. F. (2010). Non-invasive prenatal diagnosis using cell-free fetal DNA technology: applications and implications. Public Health Genomics, 13(4), 246–255.PubMedCrossRef
Hill, M., Finning, K., Martin, P., Hogg, J., Meaney, C., Norbury, G., et al. (2011). Non-invasive prenatal determination of fetal sex: translating research into clinical practice. Clinical Genetics, 80(1), 68–75.PubMedCrossRef
Hill, M., Compton, C., Lewis, C., Skirton, H., & Chitty, L. S. (2012). Determination of foetal sex in pregnancies at risk of haemophilia: a qualitative study exploring the clinical practices and attitudes of health professionals in the United Kingdom. Haemophilia, 18(4), 575–583.PubMedCrossRef
Hill, M., Karunaratna, M., Lewis, C., Forya, F., & Chitty, L. (2013). Views and preferences for the implementation of non-invasive prenatal diagnosis for single gene disorders from health professionals in the United Kingdom. American Journal of Medical Genetics Part A, 161A(7), 1612–1618.PubMedCrossRef
Hodgson, J., & Spriggs, M. (2005). A practical account of autonomy: why genetic counseling is especially well suited to the facilitation of informed autonomous decision making. Journal of Genetic Counseling, 14(2), 89–97.PubMedCrossRef
Kelly, S. E., & Farrimond, H. R. (2012). Non-invasive preantal genetic testing: A study of public attitudes. Public Health Genomics, 15(2), 73–81.PubMedCrossRef
Kitzinger, J. (2006). Focus groups qualitative research in health care (3rd ed.). BMJ Books: C. Pope and N. Mays. London.
Lench, N., Barrett, A., Fielding, S., McKay, F., Hill, M., Jenkins, L., et al. (2013). The clinical implementation of non-invasive prenatal diagnosis for single gene disorders: challenges and progress made. Prenatal Diagnosis, 33(3), 555–562.PubMedCrossRef
Lerman, C., Croyle, R. T., Tercyak, K. P., & Hamann, H. (2002). Genetic testing: psychological aspects and implications. Journal of Consulting and Clinical Psychology, 70(3), 784–797.PubMedCrossRef
Lewis, C., Hill, M., Skirton, H., & Chitty, L. S. (2012a). Fetal sex determination using cell-free fetal DNA: service users’ experiences of and preferences for service delivery. Prenatal Diagnosis, 32(8), 735–741.PubMedCrossRef
Lewis, C., Hill, M., Skirton, H., & Chitty, L. S. (2012b). Non-invasive prenatal diagnosis for fetal sex determination: benefits and disadvantages from the service users’ perspective. European Journal of Human Genetics, 20(11), 1127–1133.PubMedCentralPubMedCrossRef
Lewis, C., Hill, M., Chitty, L. S. (2014). Non-invasive prenatal diagnosis for single gene disorders: experience of patients. Clinical Genetics, 85(4), 336–342.
Lo, Y., Chan, K., Sun, H., Chen, E., Jiang, P., Lun, F., et al. (2010). Maternal plasma DNA sequencing reveals the genome-wide genetic and mutational profile of the fetus. Science Translational Medicine, 2(61), 61ra91.PubMedCrossRef
Lun, F. M., Tsui, N. B., Chan, K. C., Leung, T. Y., Lau, T. K., Charoenkwan, P., et al. (2008). Noninvasive prenatal diagnosis of monogenic diseases by digital size selection and relative mutation dosage on DNA in maternal plasma. Proceedings of the National Academy of Sciences of the United States of America, 105(50), 19920–19925.PubMedCentralPubMedCrossRef
Michie, S., Smith, J. A., Senior, V., & Marteau, T. M. (2003). Understanding why negative genetic test results sometimes fail to reassure. American Journal of Medical Genetics Part A, 119A(3), 340–347.PubMedCrossRef
Pergament, E., & Pergament, D. (2012). Reproductive decisions after fetal genetic counselling. Best Practice and Research Clinical Obstetrics and Gynaecology, 26(5), 517–529.PubMedCrossRef
Ropka, M. E., Wenzel, J., Phillips, E. K., Siadaty, M., & Philbrick, J. T. (2006). Uptake rates for breast cancer genetic testing: a systematic review. Cancer Epidemiology, Biomarkers and Prevention, 15(5), 840–855.PubMedCrossRef
Sanderson, S. C., O’Neill, S. C., Bastian, L. A., Bepler, G., & McBride, C. M. (2010). What can interest tell us about uptake of genetic testing? Intention and behavior amongst smokers related to patients with lung cancer. Public Health Genomics, 13(2), 116–124.PubMedCrossRef
Sayres, L. C., Allyse, M., Norton, M. E., & Cho, M. K. (2011). Cell-free fetal DNA testing: a pilot study of obstetric healthcare provider attitudes toward clinical implementation. Prenatal Diagnosis, 31(11), 1070–1076.PubMedCentralPubMedCrossRef
Sayres, L. C., Allyse, M., & Cho, M. K. (2012). Integrating stakeholder perspectives into the translation of cell-free fetal DNA testing for aneuploidy. Genome Medicine, 4(6), 49.PubMedCentralPubMedCrossRef
Skirton, H., & Patch, C. (2013). Factors affecting the clinical use of non-invasive prenatal testing: a mixed methods systematic review. Prenatal Diagnosis, 33(6), 532–541.PubMedCrossRef
Tabor, A., & Alfirevic, Z. (2010). Update on procedure-related risks for prenatal diagnosis techniques. Fetal Diagnosis and Therapy, 27(1), 1–7.PubMedCrossRef
Tischler, R., Hudgins, L., Blumenfeld, Y. J., Greely, H. T., & Ormond, K. E. (2011). Noninvasive prenatal diagnosis: pregnant women’s interest and expected uptake. Prenatal Diagnosis, 31(13), 1292–1299.PubMedCentralPubMedCrossRef
Yotsumoto, J., Sekizawa, A., Koide, K., Purwosunu, Y., Ichizuka, K., Matsuoka, R., et al. (2012). Attitudes toward non-invasive prenatal diagnosis among pregnant women and health professionals in Japan. Prenatal Diagnosis, 32(7), 674–679.PubMedCrossRef
Metadata
Title
Client Views and Attitudes to Non-Invasive Prenatal Diagnosis for Sickle Cell Disease, Thalassaemia and Cystic Fibrosis
Authors
Melissa Hill
Cecilia Compton
Madhavi Karunaratna
Celine Lewis
Lyn Chitty
Publication date
01-12-2014
Publisher
Springer US
Published in
Journal of Genetic Counseling / Issue 6/2014
Print ISSN: 1059-7700
Electronic ISSN: 1573-3599
DOI
https://doi.org/10.1007/s10897-014-9725-4

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