IL-22 可调节肠上皮细胞中 MASTL 的表达。

IF 3.9 3区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY American journal of physiology. Gastrointestinal and liver physiology Pub Date : 2024-08-01 Epub Date: 2024-05-21 DOI:10.1152/ajpgi.00260.2023
Kristina Pravoverov, Iram Fatima, Susmita Barman, Frank Jühling, Mark Primeaux, Thomas F Baumert, Amar B Singh, Punita Dhawan
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引用次数: 0

摘要

微管相关丝氨酸-苏氨酸激酶样(MASTL)最近被确定为一种致癌激酶,因为它在许多癌症中过度表达。我们的研究小组发现,在散发性 CRC 和结肠炎相关癌症(CAC)的小鼠模型中,MASTL 的表达上调。CAC 是慢性 IBD 最严重的并发症之一,但人们对 IBD 从正常愈合到肿瘤发生的机制了解有限,这凸显了加强该领域研究的必要性。然而,MASTL在IBD患者中的表达及其在IBD和CAC中的分子调控尚未得到研究。本研究揭示了 MASTL 受细胞因子白细胞介素(IL)-22 的上调,而白细胞介素(IL)-22 可促进增殖并在结肠炎恢复过程中发挥重要作用;然而,IL-22 长期升高也可促进肿瘤发生。在查阅公开资料后,我们发现与对照组相比,晚期溃疡性结肠炎患者活检组织中的 MASTL 和 IL-22 水平明显升高,而且 MASTL 的上调与 IL-22 的高表达有关。我们随后的体外研究发现,IL-22 会增加肠上皮细胞系中 MASTL 的表达,促进 IL-22 介导的细胞增殖和下游生存信号转导。抑制 AKT 的活化可减轻 IL-22 诱导的 MASTL 上调。我们进一步发现,在IL-22处理的细胞中,碳酸酐酶IX(CAIX)与MASTL的结合增加,从而稳定了MASTL的表达。抑制 CAIX 可阻止 IL-22 诱导的 MASTL 表达和细胞存活。总之,我们的研究表明,IL-22/AKT 信号传导会增加 MASTL 的表达,从而促进细胞存活和增殖。此外,CAIX在IL-22刺激下与MASTL结合,从而稳定MASTL。
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IL-22 regulates MASTL expression in intestinal epithelial cells.

Microtubule-associated serine-threonine kinase-like (MASTL) has recently been identified as an oncogenic kinase given its overexpression in numerous cancers. Our group has shown that MASTL expression is upregulated in mouse models of sporadic colorectal cancer and colitis-associated cancer (CAC). CAC is one of the most severe complications of chronic inflammatory bowel disease (IBD), but a limited understanding of the mechanisms governing the switch from normal healing to neoplasia in IBD underscores the need for increased research in this area. However, MASTL levels in patients with IBD and its molecular regulation in IBD and CAC have not been studied. This study reveals that MASTL is upregulated by the cytokine interleukin (IL)-22, which promotes proliferation and has important functions in colitis recovery; however, IL-22 can also promote tumorigenesis when chronically elevated. Upon reviewing the publicly available data, we found significantly elevated MASTL and IL-22 levels in the biopsies from patients with late-stage ulcerative colitis compared with controls, and that MASTL upregulation was associated with high IL-22 expression. Our subsequent in vitro studies found that IL-22 increases MASTL expression in intestinal epithelial cell lines, which facilitates IL-22-mediated cell proliferation and downstream survival signaling. Inhibition of AKT activation abrogated IL-22-induced MASTL upregulation. We further found an increased association of carbonic anhydrase IX (CAIX) with MASTL in IL-22-treated cells, which stabilized MASTL expression. Inhibition of CAIX prevented IL-22-induced MASTL expression and cell survival. Overall, we show that IL-22/AKT signaling increases MASTL expression to promote cell survival and proliferation. Furthermore, CAIX associates with and stabilizes MASTL in response to IL-22 stimulation.NEW & NOTEWORTHY MASTL is upregulated in colorectal cancer; however, its role in colitis and colitis-associated cancer is poorly understood. This study is the first to draw a link between MASTL and IL-22, a proinflammatory/intestinal epithelial recovery-promoting cytokine that is also implicated in colon tumorigenesis. We propose that IL-22 increases MASTL protein stability by promoting its association with CAIX potentially via AKT signaling to promote cell survival and proliferation.

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来源期刊
CiteScore
9.40
自引率
2.20%
发文量
104
审稿时长
1 months
期刊介绍: The American Journal of Physiology-Gastrointestinal and Liver Physiology publishes original articles pertaining to all aspects of research involving normal or abnormal function of the gastrointestinal tract, hepatobiliary system, and pancreas. Authors are encouraged to submit manuscripts dealing with growth and development, digestion, secretion, absorption, metabolism, and motility relative to these organs, as well as research reports dealing with immune and inflammatory processes and with neural, endocrine, and circulatory control mechanisms that affect these organs.
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