Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik

Zıvralı Yarar, Esra

doi:10.31682/ayna.734371

Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik

Esra ZIVRALI YARAR (Ankara Sosyal Bilimler Üniversitesi, Sosyal ve Beşerî Bilimler Fakültesi, Psikoloji Bölümü, Ankara, Türkiye)

AYNA Klinik Psikoloji Dergisi

3 0

Yıl: 2021 Cilt: 8 Sayı: 2 Sayfa Aralığı: 186 - 198 Metin Dili: Türkçe DOI: 10.31682/ayna.734371 İndeks Tarihi: 23-12-2021

Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik

Öz:

Otizm spektrum bozukluğu, sosyal etkileşimde ve iletişimde güçlükler ile kısıtlı/tekrarlayan davranışlar ve ilgi alanları temelinde tanımlanmaktadır. Otizmin etiyolojisini anlamak ve etkili müdahale yolları üretmek, bozukluğun karmaşık doğası ve belirtilerin farklı şekillerde görülebilmesi gibi sebeplerden dolayı zorlayıcı olabilmektedir. Konu hakkında kısıtlı ilerlemenin sebeplerinden biri birbirinden oldukça farklı belirti gruplarını açıklayan tek bir sebep aranması olabilir. Parçalanabilir otizm üçlemesi hipotezi, otizmi karakterize eden belirti gruplarının davranışsal, bilişsel ve genetik düzeylerde büyük ölçüde birbirinden bağımsız olabileceğini önermektedir. Bu makale, söz konusu hipoteze kanıt teşkil edebilecek nicel genetik yöntemler ile elde edilen bulguları değerlendirmeyi amaçlamaktadır. Söz konusu bulgular, otizm belirtilerinin genetik temellerinin farklılık gösterebildiğine işaret etmekte ve parçalanabilir otizm üçlemesi hipotezini desteklemektedir. Tek yumurta ikizlerinde görülen fenotipik varyanslar, belirti grupları arasında yeterli düzeyde anlamlı ilişkinin bulunamayışı ve hem genetik hem de çevresel faktörlerin etkisi açısından tespit edilen farklılıklar otizm belirtilerinin birbirinden bağımsız değerlendirilebileceğine işaret etmektedir. Belirli kısıtlılıklar ve bunlara yönelik öneriler ışığında tartışılan bulgular otizmin heterojen yapısını anlamayı kolaylaştırmakta ve etkili müdahale teknikleri geliştirilebilmesi için yol göstermektedir. Böylece, belirli belirti gruplarında daha çok güçlüğü bulunan otizm tanısı almış bireyler kadar tanı kriterini karşılayacak kadar çeşitli belirtilere sahip olmayan ancak yoğun güçlük yaşayan bireyler için faydalı olacak müdahale protokollerinin oluşturulabileceğine dikkat çekilmiştir.

Anahtar Kelime:

Re-understanding autism: Fractionable symptoms and quantitative genetics

Öz:

Autism spectrum disorder is diagnosed based on impairments in social interaction and communication and engagement in restricted and repetitive behaviors and interests. Understanding the etiology of autism and developing effective interventions can be challenging due to the disorder's complex and heterogeneous nature. The search for a single cause for autism may be the reason for limited progress in the relevant research. The “fractionable autism triad" hypothesis suggests that the symptom domains defining autism are largely independent of each other at behavioral, cognitive, neural, and genetic levels. This paper outlined the evidence for the hypothesis at the genetic level using quantitative genetic methods. Results suggested that genetic factors associated with autism symptoms may differ, giving support to the fractionable autism triad hypothesis. The phenotypical variance within monozygotic twin pairs, lack of plausible associations between the levels of core symptom domains, and differences in genetic and/or environmental factors contributing to different symptom groups indicated the independence of the triad. These findings, which were discussed with limitations and suggestions for future research, are illuminating the heterogeneity of the disorder and lead researchers to new directions for the development of interventions tailored to specific difficulties. This way, treatment protocols can be developed for individuals with difficulties in specific symptom groups and those who could not meet the diagnostic criteria but continue having related difficulties.

Anahtar Kelime:

Belge Türü: Makale Makale Türü: Derleme Erişim Türü: Bibliyografik

American Psychiatric Association (APA). (2013). Diagnostic and statistical manual of mental disorders (5. Baskı). Washington, DC: Author.
Bailey, A., Le Couteur, A., Gottesman, I., Bolton, P., Simonoff, E., Yuzda, E. ve Rutter, M. (1995). Autism as a strongly genetic disorder: Evidence from a British twin study. Psychological Medicine, 25(01), 63–77. https://doi.org/10.1017/S0033291700028099
Bargiela, S., Steward, R. ve Mandy, W. (2016). The experiences of late-diagnosed women with autism spectrum conditions: An investigation of the female autism phenotype. Journal of Autism and Developmental Disorders, 46(10), 3281–3294. https://doi.org/10.1007/s10803-016-2872-8
Bolton, P., Macdonald, H., Pickles, A., Rios, P., Goode, S., Crowson, M., Bailey, A. ve Rutter, M. (1994). A case-control family history study of autism. Journal of Child Psychology and Psychiatry, and Allied Disciplines, 35(5), 877–900. https://doi.org/10.1111/j.1469-7610.1994.tb02300.x
Bruder, C. E., Piotrowski, A., Gijsbers, A. A., Andersson, R., Erickson, S., de Ståhl, T. D., ... Crowley, M. (2008). Phenotypically concordant and discordant monozygotic twins display different DNA copy-number-variation profiles. The American Journal of Human Genetics, 82(3), 763–771. https://doi.org/10.1016/j.ajhg.2007.12.011
Brunsdon, V. E. ve Happé, F. (2014). Exploring the ‘fractionation’of autism at the cognitive level. Autism, 18(1), 17–30. https://doi.org/10.1177/1362361313499456
DeFries, J. C. ve Fulker, D. W. (1985). Multiple regression analysis of twin data. Behavior Genetics, 15(5), 467–473. https://doi.org/10.1007/BF01066239
Dworzynski, K., Happé, F., Bolton, P. ve Ronald, A. (2009). Relationship between symptom domains in autism spectrum disorders: A population based twin study. Journal of Autism and Developmental Disorders, 39(8), 1197–1210. https://doi.org/10.1007/s10803-009-0736-1
Folstein, S. ve Rutter, M. (1977). Genetic influences and infantile autism. Nature, 265(5596), 726–728. https://doi.org/10.1038/265726a0
Frith, U. (2003). Autism explaining the enigma (3. Baskı). Oxford: Blackwell.
Happé, F. ve Frith, U. (2020). Annual research review: Looking back to look forward–changes in the concept of autism and implications for future research. Journal of Child Psychology and Psychiatry, 61(3), 218–232. https://doi.org/10.1111/jcpp.13176
Happé, F. ve Ronald, A. (2008). The “fractionable autism triad”: A review of evidence from behavioural, genetic, cognitive and neural research. Neuropsychology Review, 18(4), 287– 304. https://doi.org/10.1007/s11065-008-9076-8
Happé, F., Ronald, A. ve Plomin, R. (2006). Time to give up on a single explanation for autism. Nature Neuroscience, 9(10), 1218–1220. https://doi.org/10.1038/nn1770
Kim, S. H. ve Lord, C. (2012). Combining information from multiple sources for the diagnosis of autism spectrum disorders for toddlers and young preschoolers from 12 to 47 months of age. Journal of Child Psychology and Psychiatry, 53(2), 143–151. https://doi.org/10.1111/j.1469-7610.2011.02458.x
Kolevzon, A., Smith, C. J., Schmeidler, J., Buxbaum, J. D. ve Silverman, J. M. (2004). Familial symptom domains in monozygotic siblings with autism. American Journal of Medical Genetics. Part B, Neuropsychiatric Genetics: The Official Publication of the International Society of Psychiatric Genetics, 129(1), 76–81. https://doi.org/10.1002/ajmg.b.30011
Le Couteur, A., Bailey, A., Goode, S., Pickles, A., Gottesman, I., Robertson, S. ve Rutter, M. (1996). A broader phenotype of autism: The clinical spectrum in twins. Journal of Child Psychology and Psychiatry, and Allied Disciplines, 37(7), 785–801. https://doi.org/10.1111/j.1469- 7610.1996.tb01475.x
Loomes, R., Hull, L. ve Mandy, W. P. L. (2017). What is the male-to-female ratio in autism spectrum disorder? A systematic review and meta-analysis. Journal of the American Academy of Child and Adolescent Psychiatry, 56(6), 466–474. https://doi.org/10.1016/j.jaac.2017.03.013
Mazefsky, C. A., Goin-Kochel, R. P., Riley, B. P. ve Maes, H. H. (2008). Genetic and environmental influences on symptom domains in twins and siblings with autism. Research in Autism Spectrum Disorders, 2(2), 320–331. https://doi.org/10.1016/j.rasd.2007.08.002
Mazefsky, C. A., Oswald, D. P., Day, T. N., Eack, S. M., Minshew, N. J. ve Lainhart, J. E. (2012). ASD, a psychiatric disorder, or both? Psychiatric diagnoses in adolescents with high-functioning ASD. Journal of Clinical Child and Adolescent Psychology, 41(4), 516–523. https://doi.org/10.1080/15374416.2012.686102
Newschaffer, C. J., Fallin, D. ve Nora, L. L. (2002). Heritable and nonheritable risk factors for autism spectrum disorders. Epidemiologic Reviews, 24(2), 137–153. https://doi.org/10.1093/epirev/mxf010
Pickles, A., Starr, E., Kazak, S., Bolton, P. ve Papanikolaou, K. (2000). Variable expression of the autism broader phenotype: Findings from extended pedigrees. Journal of Child Psychology and Psychiatry, and Allied Disciplines, 41(4), 491–502. https://doi.org/10.1111/1469-7610.00634
Plomin, R., DeFries, J. C., Knopik, V. S. ve Neiderhiser, J. M. (2013). Behavioral genetics (6. Baskı). New York: Worth.
Ritvo, E. R., Freeman, B. J., Mason-Brothers, A., Mo, A. ve Ritvo, A. M. (1985). Concordance for the syndrome of autism in 40 pairs of afflicted twins. American Journal of Psychiatry, 142(1), 74– 77. https://doi.org/10.1176/ajp.142.1.74
Robinson, E. B., Koenen, K. C., McCormick, M. C., Munir, K., Hallett, V., Happé, F., Plomin, R. ve Ronald, A. (2011). Evidence that autistic traits show the same etiology in the general population and at the quantitative extremes (5%, 2.5%, and 1%). Archives of General Psychiatry, 68(11), 1113–1121. https://doi.org/10.1001/archgenpsychiatry.2011.119
Robinson, E. B., Koenen, K. C., McCormick, M. C., Munir, K., Hallett, V., Happé, F., Plomin, R. ve Ronald, A. (2012). A multivariate twin study of autistic traits in 12-year-olds: Testing the fractionable autism triad hypothesis. Behavior Genetics, 42(2), 245–255. https://doi.org/10.1007/s10519-011-9500-3
Ronald, A., Happé, F., Bolton, P., Butcher, L. M., Price, T. S., Wheelwright, S., Baron-Cohen, S. ve Plomin, R. (2006a). Genetic heterogeneity between the three components of the autism spectrum: A twin study. Journal of the American Academy of Child and Adolescent Psychiatry, 45(6), 691–699. https://doi.org/10.1097/01.CHI.0000215325.13058.9D
Ronald, A., Happé, F. ve Plomin, R. (2005). The genetic relationship between individual differences in social and nonsocial behaviours characteristic of autism. Developmental Science, 8(5), 444– 458. https://doi.org/10.1111/j.1467-7687.2005.00433.x
Ronald, A., Happé, F., Price, T. S., Baron-Cohen, S. ve Plomin, R. (2006b). Phenotypic and genetic overlap between autistic traits at the extremes of the general population. Journal of the American Academy of Child and Adolescent Psychiatry, 45(10), 1206–1214. https://doi.org/10.1097/01.chi.0000230165.54117.41
Ronald, A. ve Hoekstra, R. A. (2011). Autism spectrum disorders and autistic traits: A decade of new twin studies. American Journal of Medical Genetics Part B: Neuropsychiatric Genetics. 156(3), 255–274. https://doi.org/10.1002/ajmg.b.31159
Ronald, A., Larsson, H., Anckarsäter, H. ve Lichtenstein, P. (2011). A twin study of autism symptoms in Sweden. Molecular Psychiatry, 16(10), 1039–1047. https://doi.org/10.1038/mp.2010.82
Steffenburg, S., Gillberg, C., Hellgren, L., Andersson, L., Gillberg, I. C., Jakobsson, G. ve Bohman, M. (1989). A twin study of autism in Denmark, Finland, Iceland, Norway and Sweden. Journal of Child Psychology and Psychiatry, 30(3), 405–416. https://doi.org/10.1111/j.1469- 7610.1989.tb00254.x
Szatmari, P., MacLean, J. E., Jones, M. B., Bryson, S. E., Zwaigenbaum, G. B., Mahoney, W. J. ve Tuff, L. (2000). The familial aggregation of the lesser variant in biological and nonbiological relatives of PDD probands: A family history study. Journal of Child Psychology and Psychiatry, 41(05), 579–586. https://doi.org/10.1111/1469-7610.00644

APA	Zıvralı Yarar E (2021). Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. , 186 - 198. 10.31682/ayna.734371
Chicago	Zıvralı Yarar Esra Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. (2021): 186 - 198. 10.31682/ayna.734371
MLA	Zıvralı Yarar Esra Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. , 2021, ss.186 - 198. 10.31682/ayna.734371
AMA	Zıvralı Yarar E Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. . 2021; 186 - 198. 10.31682/ayna.734371
Vancouver	Zıvralı Yarar E Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. . 2021; 186 - 198. 10.31682/ayna.734371
IEEE	Zıvralı Yarar E "Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik." , ss.186 - 198, 2021. 10.31682/ayna.734371
ISNAD	Zıvralı Yarar, Esra. "Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik". (2021), 186-198. https://doi.org/10.31682/ayna.734371

APA	Zıvralı Yarar E (2021). Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. AYNA Klinik Psikoloji Dergisi, 8(2), 186 - 198. 10.31682/ayna.734371
Chicago	Zıvralı Yarar Esra Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. AYNA Klinik Psikoloji Dergisi 8, no.2 (2021): 186 - 198. 10.31682/ayna.734371
MLA	Zıvralı Yarar Esra Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. AYNA Klinik Psikoloji Dergisi, vol.8, no.2, 2021, ss.186 - 198. 10.31682/ayna.734371
AMA	Zıvralı Yarar E Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. AYNA Klinik Psikoloji Dergisi. 2021; 8(2): 186 - 198. 10.31682/ayna.734371
Vancouver	Zıvralı Yarar E Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik. AYNA Klinik Psikoloji Dergisi. 2021; 8(2): 186 - 198. 10.31682/ayna.734371
IEEE	Zıvralı Yarar E "Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik." AYNA Klinik Psikoloji Dergisi, 8, ss.186 - 198, 2021. 10.31682/ayna.734371
ISNAD	Zıvralı Yarar, Esra. "Otizmi Yeniden Anlamak: Parçalanabilir Belirtiler ve Nicel Genetik". AYNA Klinik Psikoloji Dergisi 8/2 (2021), 186-198. https://doi.org/10.31682/ayna.734371