Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability

Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability

Aim. To investigate the possible association of LIF gene polymorphism rs929271 with mild intellectual disability (ID). Methods. The group of patients with mild (IQ score between 50 and 70) idiopathic intellectual disability consisted of 64 individuals including 40 (62.5 %) males and 24 (47.5 %) fema...

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Hauptverfasser: Gulkovskyi, R.V., Volkova, L.S., Livshits, L.A.
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spelling nasplib_isofts_kiev_ua-123456789-1524312025-02-09T14:53:35Z Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability Асоціація поліморфізму rs929271 гена лейкемія-інгібуючого фактора з ідіопатичною легкою інтелектуальною недієздатністю Ассоциация полиморфизма rs929271 гена лейкемия-ингибирующего фактора с идиопатической легкой интеллектуальной недееспособностью Gulkovskyi, R.V. Volkova, L.S. Livshits, L.A. Biomedicine Aim. To investigate the possible association of LIF gene polymorphism rs929271 with mild intellectual disability (ID). Methods. The group of patients with mild (IQ score between 50 and 70) idiopathic intellectual disability consisted of 64 individuals including 40 (62.5 %) males and 24 (47.5 %) females. The control group consisted of 238 healthy volunteers from different regions of Ukraine. Polymorphic variants of LIF gene rs929271 were detected using PCR followed by Hinf1 RFLP analysis. Results. The data concerning LIF genotypes and allelic variants distribution in ID patients and control group were obtained. Statistical analysis shows significant differences at rs929271 for both genotype and allele frequency when comparing ID cases and controls (p = 0.01 and 0.02, respectively). Conclusions. Our results suggest that LIF gene polymorphism rs929271 is associated with idiopathic mild intellectual disability. Therefore, we propose LIF as a new marker of genetic susceptibility for intellectual disability. Мета. Дослідити можливу асоціацію поліморфізму rs929271 гена LIF з легкою інтелектуальною недієздатністю (ІН). Методи. Група пацієнтів з легкою (IQ між 50 і 70) ідіопатичною інтелектуальною недієздатністю складалася з 64 індивідів, включаючи 40 (62,5 %) чоловіків і 24 (47,5 %) жінки. Контрольна група складалася з 238 здорових добровольців з різних регіонів України. Поліморфні варіанти rs929271 гена LIF виявляли за допомогою ПЛР з подальшим Hinf1 ПДРФ аналізом. Результати. Були отримані дані про розподіл генотипів і алельних варіантів ге­на LIF в групі пацієнтів з ІН і в контрольній групі. Статистичний аналіз показує значимі відмінності по rs929271 як для частот генотипів, так і алельних варіантів при порівнянні досліджуваної та контрольної груп (р = 0,01 і 0,02, відповідно). Висновки. Наші результати показують, що поліморфізм rs929271гена LIF асоційований з легкою ідіопатичною інтелектуальною недієздатністю. Тому ми пропонуємо LIF в якості нового маркера генетичної схи­льності до інтелектуальної недієздатності. Цель. Исследовать возможную ассоциацию полиморфиз­ма rs929271 гена LIF с легкой интеллектуальной недее­спо­­собностью (ИН). Методы. Группа пациентов с легкой (IQ между 50 и 70) идиопатической интеллектуальной недееспособностью состояла из 64 индивидов, включая 40 (62,5 %) мужчин и 24 (47,5 %) женщины. Контрольная группа состояла из 238 здоровых добровольцев из разных регионов Украины. Полиморфные варианты rs929271 гена LIF выявляли посредством ПЦР с последующим Hinf1 ПДРФ анализом. Результаты. Были получены данные о распределении генотипов и аллельных вариантов гена LIF в группе пациентов с ИН и в контрольной группе. Статистический анализ показывает значимые различия по rs929271 как для частот генотипов, так и аллелей при сравнении исследуемой и контрольной групп (р = 0,01 и 0,02, соответственно). Выводы. Наши результаты показывают, что полиморфизм rs929271гена LIF ассоциирован с легкой идиопатической интеллектуальной недееспособностью. Поэтому мы предлагаем LIF в качестве нового маркера генетической предрасположенности к интеллектуальной недееспособности. 2015 Article Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability/ R.V. Gulkovskyi, L.S. Volkova, L.A. Livshits // Biopolymers and Cell. — 2015. — Т. 31, № 1. — С. 34-37 . — Бібліогр.: 23 назв. — англ. 0233-7657 DOI: http://dx.doi.org/10.7124/bc.0008CA https://nasplib.isofts.kiev.ua/handle/123456789/152431 575.1+577.11+577.21 en application/pdf
institution Digital Library of Periodicals of National Academy of Sciences of Ukraine
collection DSpace DC
language English
topic Biomedicine
Biomedicine
spellingShingle Biomedicine
Biomedicine
Gulkovskyi, R.V.
Volkova, L.S.
Livshits, L.A.
Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability
description Aim. To investigate the possible association of LIF gene polymorphism rs929271 with mild intellectual disability (ID). Methods. The group of patients with mild (IQ score between 50 and 70) idiopathic intellectual disability consisted of 64 individuals including 40 (62.5 %) males and 24 (47.5 %) females. The control group consisted of 238 healthy volunteers from different regions of Ukraine. Polymorphic variants of LIF gene rs929271 were detected using PCR followed by Hinf1 RFLP analysis. Results. The data concerning LIF genotypes and allelic variants distribution in ID patients and control group were obtained. Statistical analysis shows significant differences at rs929271 for both genotype and allele frequency when comparing ID cases and controls (p = 0.01 and 0.02, respectively). Conclusions. Our results suggest that LIF gene polymorphism rs929271 is associated with idiopathic mild intellectual disability. Therefore, we propose LIF as a new marker of genetic susceptibility for intellectual disability.
format Article
author Gulkovskyi, R.V.
Volkova, L.S.
Livshits, L.A.
author_facet Gulkovskyi, R.V.
Volkova, L.S.
Livshits, L.A.
author_sort Gulkovskyi, R.V.
title Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability
title_short Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability
title_full Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability
title_fullStr Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability
title_full_unstemmed Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability
title_sort association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability
publishDate 2015
topic_facet Biomedicine
url https://nasplib.isofts.kiev.ua/handle/123456789/152431
citation_txt Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability/ R.V. Gulkovskyi, L.S. Volkova, L.A. Livshits // Biopolymers and Cell. — 2015. — Т. 31, № 1. — С. 34-37 . — Бібліогр.: 23 назв. — англ.
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fulltext 34 Biomedicine UDC 575.1+577.11+577.21 Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability R. V. Gulkovskyi1, 2, L. S. Volkova1, 2, L. A. Livshits1, 2 1 Institute of Molecular Biology and Genetics, NAS of Ukraine 150, Akademika Zabolotnoho Str., Kyiv, Ukraine, 03680 2 Educational and Scientifi c Center «Institute of Biology», Taras Shevchenko National University of Kyiv 64/13, Volodymyrska Str., Kyiv, Ukraine, 01601 livshits@imbg.org.ua Aim. To investigate the possible association of LIF gene polymorphism rs929271 with mild intellectual disability (ID). Methods. The group of patients with mild (IQ score between 50 and 70) idiopathic intel- lectual disability consisted of 64 individuals including 40 (62.5 %) males and 24 (47.5 %) females. The control group consisted of 238 healthy volunteers from different regions of Ukraine. Polymorphic variants of LIF gene rs929271 were detected using PCR followed by Hinf1 RFLP analysis. Results. The data con- cerning LIF genotypes and allelic variants distribution in ID patients and control group were obtained. Statistical analysis shows signifi cant differences at rs929271 for both genotype and allele frequency when comparing ID cases and controls (p = 0.01 and 0.02, respectively). Conclusions. Our results suggest that LIF gene polymorphism rs929271 is associated with idiopathic mild intellectual disability. Therefore, we propose LIF as a new marker of genetic susceptibility for intellectual disability. K e y w o r d s: LIF gene, intellectual disability, polymorphism, population. Introduction Intellectual disability is a neurodevelopmental disor- der, affecting about 3 % of the population, and is as- sociated with a series of social and medical handi- caps [1]. The causes of intellectual disability vary with the severity of the condition: moderate-to-se- vere intellectual disability (IQ less than 50) is much more likely to be due to a single pathological cause (genetic or environmental) whereas mild ID (defi ned as an IQ score between 50 and 70) is rather due to the complex condition in origin [2]. Leukemia inhibitory factor (LIF) is a member of the neuropoietic family of neurotrophins and was found to regulate the neuronal phenotype and coor- dinates astrocyte, oligodendrocyte, microglia, and infl ammatory cell responses [3–5]. Furthermore, LIF is shown to act as a survival factor for neurons and oligodendrocytes [6, 7]. Upon binding to the heterodimeric glycoprotein 130 (gp130)/LIF receptor (LIFR) complex, LIF acti- vates several major intracellular signaling pathways including ERK/MAPK signaling [8, 9]. It was discov- ered that ERK/MAPK pathway is important for nor- mal cognitive development and is required for cer- tain types of synaptic plasticity [10, 11]. It was shown that the mutations in genes coding for ERK/ MAPK pathway proteins and regulators such as SYNGAP1 and RPS6KA3 cause non-syndromic in- tellectual disability (NS-ID) and autism spect rum disorders [12–16]. The leukemia inhibitory factor gene is located on chromosome 22q12.1-q12.2 [17]. The T to G tran- sversion rs929271 is located in the 3 primed untrans- ISSN 0233-7657 Biopolymers and Cell. 2015. Vol. 31. N 1. P. 34–37 doi: http://dx.doi.org/10.7124/bc.0008CA © 2015 R. V. Gulkovskyi et al.; Published by the Institute of Molecular Biology and Genetics, NAS of Ukraine on behalf of Biopolymers and Cell. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited 35 Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability lated region of the LIF gene. This polymor phism is suggested to reduce mRNA stability and fi nally may have an effect on the amount of secreted LIF [18]. Previous reports have demonstrated that the LIF gene variant (rs929271) may produce susceptibility to vascular dementia, hebephrenic schi zophrenia and deterioration of working memory function [19, 20]. Aim of this study is to evaluate the possible asso- ciation of the LIF gene polymorphism rs929271 with mild intellectual disability. Materials and Methods DNA-samples were extracted from peripheral blo- od leucocytes of unrelated volunteers from differ- ent regions of Ukraine and ID patients by the stan- dard phenol-chloroform method. Informed consents we re obtained from all the individuals participating in our study. The group of patients with mild (IQ score between 50 and 70) idiopathic intellectual disability consisted of 64 individuals including 40 (62.5 %) males and 24 (47.5 %) females, where previous extensive genetic investigations have revealed no abnormalities. All pa- tients underwent physical and neurological examina- tion (test used for IQ: WISC III, WISC-R, WISC) and standard G-banding ka ryotype analysis. DNA tests to determine Fragile X status (FRAXA, FRAXE, FRAXF loci) and Prader Willi/Angelman syndromes (PW/ AS) were perfor med to rule out the known genetic causes of ID prior to further investigation. Array-CGH analysis (400K resolution) revealed no any pathologi- cal rearrangements in all patients. The control group consisted of 238 individuals in- cluding 128 (53.8 %) males and 110 (46.2 %) fe- males. This group may be considered representative for the estimation of DNA polymorphism frequency in autosomal genes [21, 22]. The presence of LIF polymorphism rs929271 was examined by PCR-RFLP (restriction fragment length polymorphism) analysis. Specifi c oligonucle- otides, designed and synthesized in accordance to corresponding sequences of LIF ge ne, were used as primers: forward: 5’-GGGGACACAGAAACAAG GACAGGG -3’ and reverse: 5’-AAGGGTCGGAT CTGAGAGAATGGG-3’. Pri mers were desig ned us- Fig. 1. RFLP analysis of rs929271 LIF gene variant (2 % agarose gel electrophoresis): M – molecular mass marker (Ladder 50 bp); 1, 2, – individuals with homozygous ge notype TT; 3, 4 – individuals with heterozygous genotype TG; 5 – individual with homozygous genotype GG, 6 – negative control Table 1. Distribution of genotypes and allele variants in investigated groups Control group, n = 238 ID patients, n =64 Genotype, n (%) TT 107 (45) 18 (28.1) TG 106 (44.5) 35 (54.7) GG 25 (10.5) 11 (17.2) TG+GG 131(55) 46(71.9)* Allele, n (frequency) T 320 (0.672) 71 (0.555) G 156 (0.328) 57 (0.445)* N o t e. N – number of individuals; * statistically reliable differ- ence (P < 0,05). 298 bp 159 bp 139 bp M 1 2 3 4 5 6 ing a web-based PRIMER 3.0 program (http://work- bench.sdsc.edu). We used the «BLAST» program at http://www.ncbi.nlm.nih. gov/blast to check for the specifi city of the primers. Hypothetical RFLP results 36 R. V. Gulkovskyi, L. S. Volkova, L. A. Livshits were tested using NEB cutter V2.0 (http://tools.neb. com/NEBcutter2). The PCR amplifi cation was performed in a fi nal volume of 25 μl containing 1 × PCR buffer, 1.5 mM MgCl2, 200 μM of each dNTP, 1 μM of each pri mer, 0.2 units of Taq-DNA polymerase and 200 ng of the DNA template. The cycling conditions were as fol- lows: initial denaturation at 95 C for 5 min, 30 cy- cles consisting of denaturation at 94 C for 30 s, annealing at 63 C for 30 s, extension at 72 C for 30 s and a fi nal elongation step at 72 C for 3 min. The amplifi ed fragments were digested with HinfI. Di- gestion was performed in 15 μl reaction volume con- taining 1 X reaction buffer, 0.5 units of the restric- tion enzyme and 10 μl of purifi ed PCR product, in- cubated at 37 C overnight and analyzed in 2 % standard agarose electrophoresis. The results were statistically assessed using Ope- nEpi software and Fisher’s 2 by 2 exact test, as well as odd ratio (OR) calculation; p < 0.05 was consid- ered to be statistically signifi cant test [23]. Results and Discussion The designed primers successfully amplifi ed the cor responding fragment (298 bp) of the LIF gene. The T to G transition in rs929271 variant removes a restriction site for endonuclease HinfI. Thereby three different patterns could be observed for the rs929271 variant after the restriction digestion: a 298 bp band (for rs929271 T/T); a 298 bp, a 159 bp and a 139 bp bands (for rs929271 T/G); a 159 bp and a 139 bp bands (rs929271 G/G) (Fig. 1). Based on the RFLP analysis of the rs929271 vari- ant, the individuals were classifi ed into three groups: TT, TG and GG. Genotypes and allele frequencies of the rs929271 polymorphism are presented in Table 1. The observed genotype distributions showed no de- viations from Hardy-Weinberg expectations in gener- al population of Ukraine and in ID patients group. It was determined that total frequency of hetero- and homozygous carriers of the LIF gene rs929271 minor allele, in this case that of guanine (G), is reli- ably higher (p = 0.01) in the ID patients group (71.9 %) compared to the control group (55 %). The minor G-allele occurred less frequently in the control gro- up – 0.328 than in the ID patients gro up – 0.445 (p = = 0.02). It was shown that the risk of mild ID devel- opment increased for both hetero- and homozygous carriers of minor rs929271 G-allele and the odd ratio was 2.09 (95 % CI: 1.14–3.81). Our results suggest that the LIF gene polymor- phism rs929271 is associated with idiopathic mild intellectual disability. These data can be explained by a decrease of LIF levels in the LIF gene rs929271 minor allele G carriers that in turn, may affect the regulation of neurogenesis and neuroprotection at least via LIF/ERK/MAPK signaling. Therefore, we propose LIF as a new marker of genetic susceptibility for intellectual disability. Fu- ture investigations are necessary to explain the mo- lecular mechanisms of the LIF involvement in ID pathogenesis. Acknowledgements We thank the patients and volunteers for their coop- eration. REFERENCES 1. Leonard H, Wen X. The epidemiology of mental retardation: challenges and opportunities in the new millennium. Ment Retard Dev Disabil Res Rev. 2002;8(3):117–34. 2. Flint J. Genetic basis of cognitive disability. Dialogues Clin Neurosci. 2001;3(1):37–46. 3. Holmberg KH, Patterson PH. Leukemia inhibitory factor is a key regulator of astrocytic, microglial and neuronal re- sponses in a low-dose pilocarpine injury model. Brain Res. 2006;1075(1):26–35. 4. Kerr BJ, Patterson PH. Leukemia inhibitory factor pro- motes oligodendrocyte survival after spinal cord injury. Glia. 2005;51(1):73–9. 5. Sugiura S, Lahav R, Han J, et al. Leukaemia inhibitory fac- tor is required for normal infl ammatory responses to in jury in the peripheral and central nervous systems in vi vo and is chemotactic for macrophages in vitro. Eur J Neu rosci. 2000; 12(2):457–66. 6. Barres BA, Schmid R, Sendnter M, Raff MC. Multiple extra- cellular signals are required for long-term oligodendro cyte survival. Development. 1993;118(1):283–95. 7. Martinou JC, Martinou I, Kato AC. Cholinergic differentia- tion factor (CDF/LIF) promotes survival of isolated rat em bryonic motoneurons in vitro. Neuron. 1992;8(4): 737– 44. 8. Niwa H, Ogawa K, Shimosato D, Adachi K. A parallel cir cu- it of LIF signalling pathways maintains pluripotency of mouse ES cells. Nature. 2009;460(7251):118–22. 37 Association of the leukemia inhibitory factor gene polymorphism rs929271 with idiopathic mild intellectual disability 9. Hirai H, Karian P, Kikyo N. Regulation of embryonic stem cell self-renewal and pluripotency by leukaemia inhibito ry fac- tor. Biochem J. 2011;438(1):11–23. 10. Zhu JJ, Qin Y, Zhao M, Van Aelst L, Malinow R. Ras and Rap control AMPA receptor traffi cking during synaptic plastici- ty. Cell. 2002;110(4):443–55. 11. Thomas GM, Huganir RL. MAPK cascade signalling and synaptic plasticity. Nat Rev Neurosci. 2004;5(3):173–83. 12. Hamdan FF, Gauthier J, Spiegelman D, et al. Mutations in SYNGAP1 in autosomal nonsyndromic mental retardati on. N Engl J Med. 2009;360(6):599–605. 13. Hamdan FF, Daoud H, Piton A, et al. De novo SYNGAP1 mutations in nonsyndromic intellectual disability and au- tism. Biol Psychiatry. 2011;69(9):898–901. 14. Krepischi AC, Rosenberg C, Costa SS, Crolla JA, Huang S, Vianna-Morgante AM. A novel de novo microdeletion span- ning the SYNGAP1 gene on the short arm of chromosome 6 associated with mental retardation. Am J Med Genet A. 2010;152A(9):2376–8. 15. Delaunoy JP, Dubos A, Marques Pereira P, Hanauer A. Iden- tifi cation of novel mutations in the RSK2 gene (RPS6KA3) in patients with Coffi n-Lowry syndrome. Clin Genet. 2006; 70(2):161–6. 16. Field M, Tarpey P, Boyle J, et al. Mutations in the RSK2 (RPS6KA3) gene cause Coffi n-Lowry syndrome and non- syndromic X-linked mental retardation. Clin Genet. 2006; 70(6):509–15. 17. Sutherland GR, Baker E, Hyland VJ, Callen DF, Stahl J, Gough NM. The gene for human leukemia inhibitory factor (LIF) maps to 22q12. Leukemia. 1989;3(1):9–13. 18. 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Волкова, Л. А. Лівшиць Асоціація поліморфізму rs929271 гена лейкемія-інгібуючого фактора з ідіопатичною легкою інтелектуальною недієздатністю Мета. Дослідити можливу асоціацію поліморфізму rs929271 гена LIF з легкою інтелектуальною недієздатністю (ІН). Мето- ди. Група пацієнтів з легкою (IQ між 50 і 70) ідіопатичною інте- лектуальною недієздатністю складалася з 64 індивідів, включа- ючи 40 (62,5 %) чоловіків і 24 (47,5 %) жінки. Контрольна група складалася з 238 здорових добровольців з різних регіонів Украї- ни. Поліморфні варіанти rs929271 гена LIF виявляли за допо- могою ПЛР з подальшим Hinf1 ПДРФ аналізом. Результати. Були отримані дані про розподіл генотипів і алельних варіантів ге на LIF в групі пацієнтів з ІН і в контрольній групі. Статистич- ний аналіз показує значимі відмінності по rs929271 як для частот генотипів, так і алельних варіантів при порівнянні досліджува- ної та контрольної груп (р = 0,01 і 0,02, відповідно). Висновки. Наші результати показують, що поліморфізм rs929271гена LIF асоційований з легкою ідіопатичною інтелектуальною недієз- датністю. Тому ми пропонуємо LIF в якості нового маркера ге- нетичної схи льності до інтелектуальної недієздатності. Ключові слова: ген LIF, інтелектуальна недієздат ність, поліморфізм, популяція. Р. В. Гулковский, Л. С. Волкова, Л. А. Лившиц Ассоциация полиморфизма rs929271 гена лейкемия-ингибирующего фактора с идиопатической легкой интеллектуальной недееспособностью Цель. Исследовать возможную ассоциацию полиморфиз ма rs929271 гена LIF с легкой интеллектуальной недее спо - собностью (ИН). Методы. Группа пациентов с легкой (IQ меж- ду 50 и 70) идиопатической интеллектуальной недееспособ- ностью состояла из 64 индивидов, включая 40 (62,5 %) мужчин и 24 (47,5 %) женщины. Контрольная группа состояла из 238 здоровых добровольцев из разных регионов Украины. Поли- морфные варианты rs929271 гена LIF выявляли посредством ПЦР с последующим Hinf1 ПДРФ анализом. Результаты. Были получены данные о распределении генотипов и аллель- ных вариантов гена LIF в группе пациентов с ИН и в контроль- ной группе. Статистический анализ показывает значимые раз- личия по rs929271 как для частот генотипов, так и аллелей при сравнении исследуемой и контрольной групп (р = 0,01 и 0,02, соответственно). Выводы. Наши результаты показывают, что полиморфизм rs929271гена LIF ассоциирован с легкой идиопа- тической интеллектуальной недееспособностью. Поэтому мы предлагаем LIF в качестве нового маркера генетической пред- расположенности к интеллектуальной недееспособности. Ключевые слова: ген LIF, интеллектуальная недее спо- собность, полиморфизм, популяция. Received 10.01.2015

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