A pig BodyMap transcriptome reveals diverse tissue physiologies and evolutionary dynamics of transcription

Jin, Long; Tang, Qianzi; Hu, Silu; Chen, Zhongxu; Zhou, Xuming; Zeng, Bo; Wang, Yuhao; He, Mengnan; Li, Yan; Gui, Lixuan; Shen, Linyuan; Long, Keren; Ma, Jideng; Wang, Xun; Chen, Zhengli; Jiang, Yanzhi; Tang, Guoqing; Zhu, Li; Liu, Fei; Zhang, Bo; Huang, Zhiqing; Li, Guisen; Li, Diyan; Gladyshev, Vadim N.; Yin, Jingdong; Gu, Yiren; Li, Xuewei; Li, Mingzhou

doi:10.1038/s41467-021-23560-8

Cited by 68 publications

(70 citation statements)

References 106 publications

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“…More importantly, in line with our findings, Asgr1-deficient mice showed more severe liver injury and elevated hepatocyte death upon Streptococcus pneumoniae infection than did WT controls [ 37 ], supporting genetic susceptibility to liver injury in ASGR1 deficiency. Furthermore, reanalysis of data from our recent work [ 38 ] showed that, from a phylogenetic point of view, the liver exhibited a relatively lower evolutionary divergence in transcriptional output and resilience (with a shorter total branch length of expression-based trees [0.77]) than lung (0.88), adipose tissue (0.86), kidney (0.84) and spleen (0.79), and was comparable to heart (0.77) and higher than skeletal muscle [0.67]) among nine mammalian species ( S10A and S10B Fig ). Of the single-copy orthologous genes shared by nine mammalian species, ASGR1 and genes spatially close to ASGR1 exhibited relatively lower ΔAIC values and thus are relatively lower species-specific expression differences in the liver (variation in expression across species not due to evolutionary history, or expression changes after correcting the evolutionary nucleotide divergence between mammals) ( S11A and S11B Fig ).…”

Section: Discussionmentioning

confidence: 99%

Deficiency of ASGR1 in pigs recapitulates reduced risk factor for cardiovascular disease in humans

Xie

Shi

et al. 2021

PLoS Genet

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Genetic variants in the asialoglycoprotein receptor 1 (ASGR1) are associated with a reduced risk of cardiovascular disease (CVD) in humans. However, the underlying molecular mechanism remains elusive. Given the cardiovascular similarities between pigs and humans, we generated ASGR1-deficient pigs using the CRISPR/Cas9 system. These pigs show age-dependent low levels of non-HDL-C under standard diet. When received an atherogenic diet for 6 months, ASGR1-deficient pigs show lower levels of non-HDL-C and less atherosclerotic lesions than that of controls. Furthermore, by analysis of hepatic transcriptome and in vivo cholesterol metabolism, we show that ASGR1 deficiency reduces hepatic de novo cholesterol synthesis by downregulating 3-hydroxy-3-methylglutaryl-CoA reductase (HMGCR), and increases cholesterol clearance by upregulating the hepatic low-density lipoprotein receptor (LDLR), which together contribute to the low levels of non-HDL-C. Despite the cardioprotective effect, we unexpectedly observed mild to moderate hepatic injury in ASGR1-deficient pigs, which has not been documented in humans with ASGR1 variants. Thus, targeting ASGR1 might be an effective strategy to reduce hypercholesterolemia and atherosclerosis, whereas further clinical evidence is required to assess its hepatic impact.

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Section: Discussionmentioning

confidence: 99%

Deficiency of ASGR1 in pigs recapitulates reduced risk factor for cardiovascular disease in humans

Xie

Shi

et al. 2021

PLoS Genet

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“…S3A), out of which a large fraction was also classified as testis enriched. The highly specific expression of the testis is due to the testis-specific Sertoli and germ cells and has previously been described in human [ 2 ], pig [ 15 , 32 ], macaque [ 33 ], and mouse [ 34 ]. In contrast, a large portion of the genes is classified as low tissue specificity and detected in all tissues ( n = 7699), and this set of genes is also interesting to study further.…”

Section: Resultsmentioning

confidence: 99%

Genome-wide annotation of protein-coding genes in pig

et al. 2022

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Background There is a need for functional genome-wide annotation of the protein-coding genes to get a deeper understanding of mammalian biology. Here, a new annotation strategy is introduced based on dimensionality reduction and density-based clustering of whole-body co-expression patterns. This strategy has been used to explore the gene expression landscape in pig, and we present a whole-body map of all protein-coding genes in all major pig tissues and organs. Results An open-access pig expression map (www.rnaatlas.org) is presented based on the expression of 350 samples across 98 well-defined pig tissues divided into 44 tissue groups. A new UMAP-based classification scheme is introduced, in which all protein-coding genes are stratified into tissue expression clusters based on body-wide expression profiles. The distribution and tissue specificity of all 22,342 protein-coding pig genes are presented. Conclusions Here, we present a new genome-wide annotation strategy based on dimensionality reduction and density-based clustering. A genome-wide resource of the transcriptome map across all major tissues and organs in pig is presented, and the data is available as an open-access resource (www.rnaatlas.org), including a comparison to the expression of human orthologs.

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“…Several previous studies [ 10 – 13 , 17 ] have characterized the architecture of chromatin in porcine tissues and cell types. These studies mainly compared chromatin organization between species or during early development, and limited data on the differences in chromatin organization between pig breeds were presented.…”

Section: Discussionmentioning

confidence: 99%

“…We separately constructed four Hi-C libraries for wild boar ATs (two libraries for ULB and GOM, separately) and three libraries for Bama pig ATs (one library for ULB and two libraries for GOM) according to a previously described in situ Hi-C method with some modifications [ 2 ]. We also downloaded one corresponding Hi-C library for ULB in Bama pig, which was generated using the same experimental protocol, from our previous study [ 17 ]. Briefly, 1 g of adipose tissue was cross-linked in 4% freshly prepared formaldehyde (Sigma Aldrich, Louis, MO, USA) for 30 min at room temperature, followed by quenching with glycine (Amresco, Solon, OH, USA) at a final concentration of 0.25 mol/L.…”

Section: Methodsmentioning

confidence: 99%

“…To explore the relationship between gene expression and 3D genome conformation, we constructed four RNA-seq libraries for ATs in wild boars (two libraries for ULB and GOM, separately) and three libraries for ATs in Bama pigs (one library for ULB and two libraries for GOM). One corresponding library for ULB in Bama pigs was collected from our previous study [ 17 ]. Total RNA was extracted from each sample using an RNeasy Mini Kit (Qiagen, Valencia, CA, USA).…”

Section: Methodsmentioning

confidence: 99%

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Reorganization of 3D genome architecture across wild boar and Bama pig adipose tissues

Zhang

Liu

et al. 2022

J Animal Sci Biotechnol

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Background A growing body of evidence has revealed that the mammalian genome is organized into hierarchical layers that are closely correlated with and may even be causally linked with variations in gene expression. Recent studies have characterized chromatin organization in various porcine tissues and cell types and compared them among species and during the early development of pigs. However, how chromatin organization differs among pig breeds is poorly understood. Results In this study, we investigated the 3D genome organization and performed transcriptome characterization of two adipose depots (upper layer of backfat [ULB] and greater omentum [GOM]) in wild boars and Bama pigs; the latter is a typical indigenous pig in China. We found that over 95% of the A/B compartments and topologically associating domains (TADs) are stable between wild boars and Bama pigs. In contrast, more than 70% of promoter-enhancer interactions (PEIs) are dynamic and widespread, involving over a thousand genes. Alterations in chromatin structure are associated with changes in the expression of genes that are involved in widespread biological functions such as basic cellular functions, endocrine function, energy metabolism and the immune response. Approximately 95% and 97% of the genes associated with reorganized A/B compartments and PEIs in the two pig breeds differed between GOM and ULB, respectively. Conclusions We reported 3D genome organization in adipose depots from different pig breeds. In a comparison of Bama pigs and wild boar, large-scale compartments and TADs were mostly conserved, while fine-scale PEIs were extensively reorganized. The chromatin architecture in these two pig breeds was reorganized in an adipose depot-specific manner. These results contribute to determining the regulatory mechanism of phenotypic differences between Bama pigs and wild boar.

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A pig BodyMap transcriptome reveals diverse tissue physiologies and evolutionary dynamics of transcription

Cited by 68 publications

References 106 publications

Deficiency of ASGR1 in pigs recapitulates reduced risk factor for cardiovascular disease in humans

Deficiency of ASGR1 in pigs recapitulates reduced risk factor for cardiovascular disease in humans

Genome-wide annotation of protein-coding genes in pig

Reorganization of 3D genome architecture across wild boar and Bama pig adipose tissues

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