What is the clinical evidence from this study?

Study design: Other. Population: Colorectal cancer. Intervention: METTL7A vs. Control. Primary outcome: Tumor progression and cholesterol synthesis.

What question did this study set out to answer?

This research aims to explore the role of METTL7A in colorectal cancer (CRC) progression and its effects on cholesterol metabolism.

April 23, 2026Open Access

METTL7A inhibits progression of colorectal cancer through the SREBP1 / FDFT1 / SQLE / CYP51A1 / cholesterol metabolic pathway

Key Result

METTL7A functions as a tumor suppressor in colorectal cancer by binding to SREBP1 and SCAP, inhibiting SREBP1 nuclear translocation and reducing cholesterol synthesis.

Key Points

This research aims to explore the role of METTL7A in colorectal cancer (CRC) progression and its effects on cholesterol metabolism.
Investigated the function of METTL7A in CRC cells
Analyzed the impact of METTL7A on cholesterol synthesis and metabolic pathways
Identified potential therapeutic implications for targeting METTL7A in treatment
METTL7A was found to inhibit CRC progression through modulation of cholesterol synthesis
Alterations in the SREBP1/FDFT1/SQLE/CYP51A1 pathway were observed
METTL7A emerged as a potential therapeutic target for CRC due to its role in metabolic regulation

Structured PICO

Population

Human CRC cell lines (HCT116, HCT8, HCT15, SW480, SW620, HT29, T84), xenograft tumor in nude mice (n=12), orthotopic tumor in C57BL/6 mice (n=12), and spontaneous tumor in ApcMin/+ C57BL/6 mice (n=12).

Intervention

METTL7A overexpression or knockout/knockdown

Comparator

Wild-type or empty vector controls

Outcome

Tumor progression and cholesterol synthesis (SREBP1/FDFT1/SQLE/CYP51A1 pathway)surrogate

METTL7A inhibits colorectal cancer progression by suppressing the SREBP1-mediated cholesterol synthesis pathway.

Abstract

This study provides valuable insights into the role of METTL7A in CRC and its impact on metabolic reprogramming, particularly cholesterol synthesis, and identifies METTL7A as a potential therapeutic target of CRC.

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