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功能和基因网络分析鉴定了初生牛乳腺实质或脂肪垫的转录特征,揭示了发育过程中组织间的新信号网络。

Functional and gene network analyses of transcriptional signatures characterizing pre-weaned bovine mammary parenchyma or fat pad uncovered novel inter-tissue signaling networks during development.

机构信息

Department of Animal Sciences, University of Illinois, Urbana, IL 61801, USA.

出版信息

BMC Genomics. 2010 May 26;11:331. doi: 10.1186/1471-2164-11-331.

Abstract

BACKGROUND

The neonatal bovine mammary fat pad (MFP) surrounding the mammary parenchyma (PAR) is thought to exert proliferative effects on the PAR through secretion of local modulators of growth induced by systemic hormones. We used bioinformatics to characterize transcriptomics differences between PAR and MFP from approximately 65 d old Holstein heifers. Data were mined to uncover potential crosstalk through the analyses of signaling molecules preferentially expressed in one tissue relative to the other.

RESULTS

Over 9,000 differentially expressed genes (DEG; False discovery rate <or= 0.05) were found of which 1,478 had a >or=1.5-fold difference between PAR and MFP. Within the DEG highly-expressed in PAR vs. MFP (n = 736) we noted significant enrichment of functions related to cell cycle, structural organization, signaling, and DNA/RNA metabolism. Only actin cytoskeletal signaling was significant among canonical pathways. DEG more highly-expressed in MFP vs. PAR (n = 742) belong to lipid metabolism, signaling, cell movement, and immune-related functions. Canonical pathways associated with metabolism and signaling, particularly immune- and metabolism-related were significantly-enriched. Network analysis uncovered a central role of MYC, TP53, and CTNNB1 in controlling expression of DEG highly-expressed in PAR vs. MFP. Similar analysis suggested a central role for PPARG, KLF2, EGR2, and EPAS1 in regulating expression of more highly-expressed DEG in MFP vs. PAR. Gene network analyses revealed putative inter-tissue crosstalk between cytokines and growth factors preferentially expressed in one tissue (e.g., ANGPTL1, SPP1, IL1B in PAR vs. MFP; ADIPOQ, IL13, FGF2, LEP in MFP vs. PAR) with DEG preferentially expressed in the other tissue, particularly transcription factors or pathways (e.g., MYC, TP53, and actin cytoskeletal signaling in PAR vs. MFP; PPARG and LXR/RXR Signaling in MFP vs. PAR).

CONCLUSIONS

Functional analyses underscored a reciprocal influence in determining the biological features of MFP and PAR during neonatal development. This was exemplified by the potential effect that the signaling molecules (cytokines, growth factors) released preferentially (i.e., more highly-expressed) by PAR or MFP could have on molecular functions or signaling pathways enriched in the MFP or PAR. These bidirectional interactions might be required to coordinate mammary tissue development under normal circumstances or in response to nutrition.

摘要

背景

人们认为,牛的新生乳腺脂肪垫(MFP)环绕在乳腺实质(PAR)周围,通过分泌受全身激素诱导的局部生长调节剂,对 PAR 发挥增殖作用。我们使用生物信息学方法来描述大约 65 天大的荷斯坦奶牛的 PAR 和 MFP 之间的转录组学差异。通过分析在一种组织中优先表达而在另一种组织中相对较少表达的信号分子,我们对数据进行挖掘,以揭示潜在的串扰。

结果

发现超过 9000 个差异表达基因(False discovery rate <or= 0.05),其中 1478 个基因在 PAR 和 MFP 之间的差异大于或等于 1.5 倍。在 PAR 中高表达的差异表达基因(n = 736)中,我们注意到与细胞周期、结构组织、信号转导和 DNA/RNA 代谢相关的功能显著富集。在经典途径中,只有肌动蛋白细胞骨架信号是显著的。在 MFP 中高表达的差异表达基因(n = 742)属于脂质代谢、信号转导、细胞运动和免疫相关功能。与代谢和信号转导相关的经典途径,特别是与免疫和代谢相关的途径,显著富集。网络分析发现 MYC、TP53 和 CTNNB1 在控制 PAR 中高表达的差异表达基因的表达中起着核心作用。类似的分析表明,PPARG、KLF2、EGR2 和 EPAS1 在调节 MFP 中高表达的差异表达基因的表达中起着核心作用。基因网络分析显示,在一种组织中优先表达的细胞因子和生长因子(例如 PAR 中的 ANGPTL1、SPP1 和 IL1B;MFP 中的 ADIPOQ、IL13、FGF2 和 LEP)与在另一种组织中优先表达的差异表达基因之间存在潜在的组织间串扰,特别是转录因子或途径(例如 PAR 中的 MYC、TP53 和肌动蛋白细胞骨架信号;MFP 中的 PPARG 和 LXR/RXR 信号)。

结论

功能分析强调了在新生牛乳腺发育过程中,MFP 和 PAR 之间的相互影响。这可以通过 PAR 或 MFP 优先释放的信号分子(细胞因子、生长因子)对 MFP 或 PAR 中富集的分子功能或信号通路产生的潜在影响来例证。这些双向相互作用可能是在正常情况下或在营养响应下协调乳腺组织发育所必需的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ca2f/2890563/af82c076173c/1471-2164-11-331-1.jpg

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