Cloning and Expression Analysis of FTO Gene in Yak (Bos grunniens)
GU Ya-Rong1,2, MA Lan-Hua1, WANG Fu-Bin1,2, ZHANG Yong-Feng2, Yan Ping2, Pan He-Ping1,*
1 College of Life Science and Engineering, Northwest Minzu University, Lanzhou 730030, China; 2 Lanzhou Institute of Husbandry and Pharmaceutical Sciences of Chinese Academy of Agricultural Sciences, Lanzhou 730050, China
Abstract:Fat mass and obesity associated gene (FTO) belongs to the non-heme plus dioxygenase superfamily and plays an important role in mammalian fat development. This study takes Qinghai Datong yak (Bos grunniens) as the research object, the CDS region of FTO gene was amplified by RT-PCR, and its function and structure were predicted by bioinformatics online softwares. At the same time, the expression of FTO gene in different stages (18 and 30 months old), different tissues (heart, liver, spleen, lung, kidney, longissimus dorsi muscle, subcutaneous adipose) and different stages of yak preadipocyte differentiation (0, 4, 8 and 12 d) were analyzed by qPCR. The results showed that the full length of FTO (GenBank No. OM640141) coding region was 1 518 bp, encoding 505 amino acids. The FTO protein mainly consisted of α-helix (44.36%), irregularly coiled (38.42%), extended chain (10.89%) and β-turned (6.34%), without transmembrane structure and signal peptide, belonging to an unstable hydrophilic protein. The results of phylogenetic tree showed that the amino acid sequence of FTO was 99.80% homologous to cattle (Bos taurus) with the closest genetic distance, and was closely related to zebu (B. indicus) and wild yak (B. mutus), and most distantly related to horse (Equus przewalskii). The results of qPCR showed that FTO expression was highest in yak heart tissue and subcutaneous adipose tissue, and lowest in spleen. The expression of FTO was significantly higher at 30 months than that at 18 months age (P<0.05). The FTO expression was found to be significantly decreased at 4, 8 and 12 d (P<0.05) during yak preadipocyte differentiation, and the FTO protein expression detected by Western blot had the same changing trend. This study can provide basic material for further research on the biological function of FTO gene in yak fat development.
[1] 付言峰, 李兰, 王学敏, 等. 2013. 苏钟猪FTO基因的mRNA表达、克隆测序及其生物信息学分析[J]. 华北农学报, 28(01): 128-134. (Fu Y F, Li L, Wang X M, et al.2013. The mRNA expression,cloning and sequencing of FTO gene and bioinformatics analysis in Suzhong pig[J]. Acta Agriculturae Boreali-Sinica. 28(01): 128-134.) [2] 林森, 林亚秋, 朱江江, 等. 2017. 藏鸡FTO基因表达的时空特性及与肌内脂肪含量的相关分析[J]. 畜牧兽医学报, 48(07): 1191-1201. (Lin S, Lin Y Q, Zhu J J, et al.2017. Temporal-spatial characteristics of FTO gene expression in Tibetan chicken and its correlation with intramuscular fat content[J]. Acta Veterinaria et Zootechnica Sinica, 48(07): 1191-1201.) [3] 林亚秋, 廖红海, 贺庆华, 等. 2016. 山羊FTO基因克隆及其表达谱[J]. 畜牧兽医学报, 47(05): 888-898. (Lin Y Q, Liao H H, He Q H, et al.2016. Cloning and expression profiling of FTO gene of goat[J]. Acta Veterinaria et Zootechnica Sinica, 47(05): 888-898.) [4] 任倩. 2019. FTO通过抑制线粒体UPR缓解小鼠脂肪细胞凋亡的作用机制[D]. 硕士学位论文, 西北农林科技大学, 导师: 孙超, pp. 17-24. (Ren Q.2019. The mechanism of FTO on suppressing mice adipocytes apoptosis by reducing mitochondrial UPR[D]. Thesis for M.S., Northwest A&F University, Suppervisor: Sun C, pp. 17-24. [5] 夏琴, 吴永文, 瞿秋红, 等. 2018. 陆川猪FTO基因的克隆及生物信息学分析[J]. 黑龙江畜牧兽医,(19): 1-5, 239. (Xia Q, Wu Y W, Qu Q H, et al.2018. The cloning and bioinformatics analysis of FTO gene in Luchuan pig[J]. Heilongjiang Animal Science Veterinary Medicine,(19): 1-5, 239.) [6] 张莹, 吴铁梅, 王雪, 等. 2016. 脂肪与肥胖相关基因对动物脂肪代谢的调节[J]. 动物营养学报, 28(04): 999-1003. (Zhang Y, Wu T M, Wang X, et al.2016. Regulation of fat mass and obesity associated gene in animal fat metabolism: A review[J]. Chinese Journal of Animal Nutrition, 28(04): 999-1003.) [7] Chen A, Chen X D, Cheng S Q, et al.2018. FTO promotes SREBP1c maturation and enhances CIDEC transcription during lipid accumulation in HepG2 cells[J]. Biochimica et Biophysica Acta-Molecular and Cell Biology of Lipids, 1863(5): 538-548. [8] Church C, Moir L, McMurray F, et al.2010. Overexpression of FTO leads to increased food intake and results in obesity[J]. Nature Genetics. 42(12): 1086-1092. [9] Ding X Z, Guo X, Yan P, et al.2012. Seasonal and nutrients intake regulation of lipoprotein lipase (LPL) activity in grazing yak (Bos grunniens) in the Alpine Regions around Qinghai Lake[J]. Livestock Science, 143(1): 29-34. [10] Ferenc K, Pilžys T, Garbicz D, et al.2020. Intracellular and tissue specific expression of FTO protein in pig: Changes with age, energy intake and metabolic status[J]. Scientific Reports, 10(1): 13029. [11] Frayling T M, Timpson N J, Weedon M N, et al.2007. A common variant in the FTO gene is associated with body mass index and predisposes to childhood and adult obesity[J]. Science, 316(5826): 889-894. [12] Fuller-Jackson J P, Henry B A.2018. Adipose and skeletal muscle thermogenesis: Studies from large animals[J]. Journal of Endocrinology, 237(3): R99-R115. [13] Gan X T, Zhao G, Huang C X, et al.2013. Identification of fat mass and obesity associated (FTO) protein expression in cardiomyocytes:Regulation by leptin and its contribution to leptin-induced hypertrophy[J]. PLOS ONE, 8(9): e74235. [14] Gerken T, Girard C A, Tung Y C, et al.2007. The obesity-associated FTO gene encodes a 2-oxoglutarate-dependent nucleic acid demethylase[J]. Science, 318(5855): 1469-1472. [15] Gulati P, Avezov E, Ma M, et al.2014. Fat mass and obesity-related (FTO) shuttles between the nucleus and cytoplasm[J]. Bioscience Reports, 34(5): e00144. [16] Huang J, Liu X, Feng X, et al.2020. Characterization of different adipose depots in fattened buffalo: Histological features and expression profiling of adipocyte markers[J]. Archives Animal Breeding, 63(1): 61-67. [17] Longo M, Zatterale F, Naderi J, et al.2019. Adipose tissue dysfunction as determinant of obesity-associated metabolic complications[J]. Internationl Journal of Molecular Sciences, 20(9): 2358. [18] Merkestein M, Laber S, McMurray F, et al.2015. FTO influences adipogenesis by regulating mitotic clonal expansion[J]. Nature Communications, 6: 6792. [19] Valverde A M, Mur C, Brownlee M, Benito M.et al.2004. Susceptibility to apoptosis in insulin-like growth factor-Ⅰreceptor-deficient brown adipocytes[J]. Molecular Biology of the Cell, 15(11): 5101-5117. [20] Vanderhoeven F, Schimmang T, Volkmanna A, et al.1994. Programmed cell death is affected in the novel mouse mutant fused toes (Ft)[J]. Development, 120(9): 2601-2607. [21] Wang J Y, Wang J Q, Gu Q, et al.2020. The biological function of m6A demethylase ALKBH5 and its role in human disease[J]. Cancer Cell International, 20(1): 347. [22] Yang J, Zhang J Y, Lu L J, et al.2016. The Fto gene regulates the proliferation and differentiation of pre-adipocytes in vitro[J]. Nutrients, 8(2): 102. [23] Zhang M, Zhang Y, Ma J, et al.2015. The demethylase activity of FTO (fat mass and obesity associated protein) is required for preadipocyte differentiation[J]. PLOS ONE, 10(7): e0133788. [24] Zhang Y F, Wu X Y, Liang C N, et al.2018. MicroRNA-200a regulates adipocyte differentiation in the domestic yak Bos grunniens[J]. Gene, 650: 41-48. [25] Zhao X, Yang Y, Sun B F, et al.2014. FTO-dependent demethylation of N6-methyladenosine regulates mRNA splicing and is required for adipogenesis[J]. Cell Research, 24(12): 1403-1419.
