Clinical Enteric Neuroscience Translational and Epidemiology Research (C.E.N.T.E.R.), Rochester, Minnesota.
Department of Quantitative Health Sciences, Mayo Clinic, Rochester, Minnesota.
Am J Physiol Gastrointest Liver Physiol. 2022 Aug 1;323(2):G88-G101. doi: 10.1152/ajpgi.00063.2022. Epub 2022 May 3.
Altered mucosal functions are documented in jejunal or colorectal mucosa from patients with irritable bowel syndrome (IBS). Our aim was to quantify ileal, ascending, and rectosigmoid colon mucosal expression of genes in IBS-diarrhea (D) and IBS-constipation (C). Forty-four patients with IBS-D, 30 with IBS-C, and 30 healthy volunteers underwent colonoscopic ileal, ascending, and rectosigmoid colon biopsies. Biopsies were stored in RNA at -80 °C, purified with on-column DNase, cDNA libraries prepared from 100-200 ng of total RNA, sequenced on Illumina NovaSeq 6000, and analyzed on Illumina's RTA version 3.4.4. Normalized mRNA expression was obtained using MAP-RSeq bioinformatics pipeline. Differential expressions in the groups (Log2-fold change) were measured using the bioinformatics package edgeR 2.6.2, corrected for false discovery rate ( <0.05). There were 30 females with IBS-C and 31 females and 13 males with IBS-D. In IBS-D and IBS-C groups, there were differential expressions of 181 genes in ascending colon and 199 genes in rectosigmoid colon. The majority were gene upregulations in IBS-D with functions reflecting activation of inflammation genes, TRPV1 (visceral hypersensitivity) and neurotransmitters/receptors (specifically purinergic, GABA, and cannabinoid). Although gene differential expressions in the ascending and rectosigmoid colon mucosa of the two groups were different, the diverse upregulated genes involved immune functions, receptors, transmitters, ion channels, and transporters. Conversely, there was reduced expression of PI15 and PI16 genes that inhibit proteases. In patients with IBS-D and IBS-C, differential expressions of genes related to immune, transmitter, nociceptive, protease inhibition, channel, and transporter functions suggest opportunities to reverse the pathobiology and treat patients with IBS. This study compares gene expression in mucosa of the terminal ileum, right colon, and left colon in patients with diarrhea- or constipation-predominant irritable bowel syndrome (IBS) and contrasts expression between these two disease entities and also between each entity and mucosa from healthy controls. The study shows there is differential expression of genes related to immune, transmitter, nociceptive, ion channel, and transporter functions, as well as reduced serine protease inhibition, in patients with IBS.
在肠易激综合征(IBS)患者的空肠或结直肠黏膜中,已记录到黏膜功能改变。我们的目的是定量检测 IBS-腹泻(D)和 IBS-便秘(C)患者的回肠、升结肠和直肠乙状结肠黏膜中基因的表达。44 例 IBS-D 患者、30 例 IBS-C 患者和 30 例健康志愿者接受了结肠镜检查的回肠、升结肠和直肠乙状结肠活检。活检组织在-80°C 下以 RNA 形式储存,用柱内 DNase 进行纯化,从 100-200ng 总 RNA 制备 cDNA 文库,在 Illumina NovaSeq 6000 上进行测序,并在 Illumina 的 RTA 版本 3.4.4 上进行分析。使用 MAP-RSeq 生物信息学管道获得标准化 mRNA 表达。使用生物信息学软件包 edgeR 2.6.2 测量组间的差异表达(对数倍变化),并校正假发现率(<0.05)。IBS-C 组中有 30 名女性,IBS-D 组中有 31 名女性和 13 名男性。在 IBS-D 和 IBS-C 组中,升结肠中有 181 个基因和直肠乙状结肠中有 199 个基因表达存在差异。大多数基因在 IBS-D 中上调,其功能反映了炎症基因、TRPV1(内脏敏感性)和神经递质/受体(特别是嘌呤能、GABA 和大麻素)的激活。尽管两组升结肠和直肠乙状结肠黏膜的基因差异表达不同,但涉及免疫功能、受体、递质、离子通道和转运体的多种上调基因。相反,抑制蛋白酶的 PI15 和 PI16 基因表达减少。在 IBS-D 和 IBS-C 患者中,与免疫、递质、伤害感受、蛋白酶抑制、通道和转运体功能相关的基因表达存在差异,这为逆转病理生理学和治疗 IBS 患者提供了机会。本研究比较了腹泻型或便秘型肠易激综合征(IBS)患者末端回肠、右结肠和左结肠黏膜的基因表达,并比较了这两种疾病实体之间以及每个实体与健康对照之间的表达差异。研究表明,IBS 患者存在与免疫、递质、伤害感受、离子通道和转运体功能相关的基因表达差异,以及丝氨酸蛋白酶抑制减少。
