miR-330-5p Suppress Cell Growth and Invasion via Disrupting HSF4-mediated MACC1/STAT3 Pathway in Colorectal Cancer

² Department of Gastroenterology, The First People’s Hospital of Yunnan Province, Affiliated Hospital of Kunming University of Science and Technology, 650000 Kunming, Yunnan, China

³ Yunnan Digestive Endoscopy Clinical Medical Center, 650000 Kunming, Yunnan, China

⁴ Faculty of Medicine, Kunming University of Science and Technology, 650000 Kunming, Yunnan, China

⁵ Department of Medical Oncology, The First People's Hospital of Yunnan Province, Affiliated Hospital of Kunming University of Science and Technology, 650000 Kunming, Yunnan, China

^*Correspondence: yuzhang320@sina.com (Yu Zhang); wenjing_zhang1@163.com (Wenjing Zhang)
^†These authors contributed equally.

Front. Biosci. (Landmark Ed) 2024, 29(2), 53; https://doi.org/10.31083/j.fbl2902053

Submitted: 16 July 2023 | Revised: 17 November 2023 | Accepted: 27 November 2023 | Published: 4 February 2024

(This article belongs to the Special Issue Gastrointestinal Cancer: Pathogenesis, Carcinogenesis and Targeted Therapies)

This is an open access article under the CC BY 4.0 license.

Abstract

Background: Recently, miRNAs are demonstrated to restrain mRNA translation through novel pattern with bind complementary sites in the coding sequence (CDS). Heat Shock Transcription Factor 4 (HSF4) has been newly described as a tumor-associated transcription factor. Therefore, the present study intends to explore miRNAs that bind CDS region of HSF4, and identify the function of their interactions in the malignant biological behavior of colorectal cancer (CRC). Methods: Prognostic value of HSF4 and correlation between HSF4 and MACC1 expression were estimated via bioinformatics with the Cancer Genome Atlas (TCGA) data. HSF4 and downstream MACC1/STAT3 signaling cascade was characterized by immunoblotting. To characterize the effects of miR-330-5p and HSF4 on the malignant phenotype of CRC cells by functional experiments. The binding activity of miR-330-5p to coding sequence (CDS) of HSF4 was identified using DIANA-microT-CDS algorithm and dual-luciferase reporter assay. Results: HSF4 was aberrantly overexpressed and associated with poor outcomes of CRC patients. Overexpression of HSF4 was correlated with Tumor Node Metastasis stage, and positively regulated malignant behaviors such as growth, migration, invasion of CRC cells. Moreover, miR-330-5p suppressed CRC cell growth, colony formation, migration and invasive. Interestingly, miR-330-5p recognized complementary sites within the HSF4 CDS region to reduce HSF4 expression. In rescue experiments, restoration of HSF4 expression functionally alleviated miR-330-5p-induced inhibition of cell growth, colon formation, invasion, and wound healing of CRC cells. HSF4 was associated positively with the well-known oncogenic factor MACC1 in TCGA cohort CRC samples, and knockdown of HSF4 resulted in downregulation of MACC1. In mechanism, MACC1 was suppressed upon miR-330-5p-induced downregulation of HSF4, leading to inactivation of phosphorylation of downstream STAT3. Conclusion: miR-330-5p suppresses tumors by directly inhibiting HSF4 to negatively modify activity of MACC1/STAT3 pathway.

Keywords

colorectal cancer

prognosis

bioinformatics

miR-330-5p

Heat Shock Transcription Factor 4

Funding

202201AY070001-272/Joint Foundation of Kunming Medical University and Yunnan Provincial Science and Technology Department

202201AY070001-256/Joint Foundation of Kunming Medical University and Yunnan Provincial Science and Technology Department

2021LCZXXF-XH03/Clinical Medical Center of Yunnan Provincial Health Commission

202205AC160070/Yunnan Medical Training Program

Figures

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