Targeting miR‐31 represses tumourigenesis and dedifferentiation of BRAF<sup>V600E</sup>‐associated thyroid carcinoma-Reference-Cited by-同舟云学术

Targeting miR‐31 represses tumourigenesis and dedifferentiation of BRAF^V600E‐associated thyroid carcinoma

Published:2024-05 Issue:5 Volume:14 Page:
ISSN:2001-1326
Container-title:Clinical and Translational Medicine
language:en
Short-container-title:Clinical & Translational Med

Author:

Zhang Peitao¹,Guan Lizhao²³,Sun Wei⁴,Zhang Yu²³,Du Yaying⁵^ORCID,Yuan Shukai²³,Cao Xiaolong⁶,Yu Zhengquan⁷,Jia Qiang¹,Zheng Xiangqian⁸,Meng Zhaowei¹,Li Xingrui⁵,Zhao Li²³^ORCID

Affiliation:

1. Department of Nuclear Medicine, Tianjin Medical University General Hospital Tianjin Medical University Tianjin China

2. Department of Thyroid and Neck Tumor, Key Laboratory of Cancer Prevention and Therapy, Tianjin's Clinical Research Center for Cancer, National Clinical Research Center for Cancer, Tianjin Medical University Cancer Institute and Hospital Tianjin Medical University Tianjin China

3. Department of Biochemistry and Molecular Biology, The Province and Ministry Co‐sponsored Collaborative Innovation Center for Medical Epigenetics, Key Laboratory of Immune Microenvironment and Disease (Ministry of Education), School of Basic Medical Sciences Tianjin Medical University Tianjin China

4. Laboratory of molecular genetics, School of Medicine Nankai University Tianjin China

5. Department of Thyroid and Breast Surgery, Tongji Hospital, Tongji Medical College Huazhong University of Science and Technology (HUST) Wuhan China

6. Department of Pulmonary and Critical Care Medicine, Zhujiang Hospital Southern Medical University Guangzhou China

7. State Key Laboratories for Agrobiotechnology, College of Biological Sciences China Agricultural University Beijing China

8. Department of Thyroid and Neck Tumor, Tianjin Medical University Cancer Institute and Hospital, National Clinical Research Center for Cancer, Key Laboratory of Cancer Prevention and Therapy Tianjin's Clinical Research Center for Cancer Tianjin China

Abstract

AbstractBackgroundBRAFV600E is the most common genetic mutation in differentiated thyroid cancer (DTC) occurring in 60% of patients and drives malignant tumour cell phenotypes including proliferation, metastasis and immune‐escape. BRAFV600E‐mutated papillary thyroid cancer (PTC) also displays greatly reduced expression of thyroid differentiation markers, thus tendency to radioactive iodine (RAI) refractory and poor prognosis. Therefore, understanding the molecular mechanisms and main oncogenic events underlying BRAFV600E will guide future therapy development.MethodsBioinformatics and clinical specimen analyses, genetic manipulation of BRAFV600E‐induced PTC model, functional and mechanism exploration guided with transcriptomic screening, as well as systematic rescue experiments were applied to investigate miR‐31 function within BRAFV600E‐induced thyroid cancer development. Besides, nanoparticles carrying miR‐31 antagomirs were testified to alleviate 131I iodide therapy on PTC models.ResultsWe identify miR‐31 as a significantly increased onco‐miR in BRAFV600E‐associated PTC that promotes tumour progression, metastasis and RAI refractoriness via sustained Wnt/β‐catenin signalling. Mechanistically, highly activated BRAF/MAPK pathway induces miR‐31 expression via c‐Jun‐mediated transcriptional regulation across in vitro and transgenic mouse models. MiR‐31 in turn facilitates β‐catenin stabilisation via directly repressing tumour suppressors CEBPA and DACH1, which direct the expression of multiple essential Wnt/β‐catenin pathway inhibitors. Genetic functional assays showed that thyroid‐specific knockout of miR‐31 inhibited BRAFV600E‐induced PTC progression, and strikingly, enhanced expression of sodium‐iodide symporter and other thyroid differentiation markers, thus promoted 131I uptake. Nanoparticle‐mediated application of anti‐miR‐31 antagomirs markedly elevated radio‐sensitivity of BRAFV600E‐induced PTC tumours to 131I therapy, and efficiently suppressed tumour progression in the pre‐clinical mouse model.ConclusionsOur findings elucidate a novel BRAF/MAPK‐miR‐31‐Wnt/β‐catenin regulatory mechanism underlying clinically BRAFV600E‐associated DTC tumourigenesis and dedifferentiation, also highlight a potential adjuvant therapeutic strategy for advanced DTC.

Funder

National Natural Science Foundation of China

China Postdoctoral Science Foundation

Fundamental Research Funds for the Central Universities

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/ctm2.1694

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