# INHBA Promotes the Progression of Gastric Cancer by Activating MAPK Signaling Pathway via Targeting ITGA6

**Authors:** Guojian Zhou, Rui Zhang, Lei Nie, Yi Si, Ting Liu, Jing Wang, Shuangshuang Han, Mingda Xuan, Jia Wang, Weifang Yu

PMC · DOI: 10.32604/or.2025.070333 · Oncology Research · 2026-02-24

## TL;DR

This study shows that INHBA promotes gastric cancer by activating the MAPK pathway through ITGA6, offering a potential new treatment target.

## Contribution

The study identifies a novel mechanism involving INHBA, ITGA6, and the MAPK pathway in gastric cancer progression.

## Key findings

- INHBA expression is higher in gastric cancer tissues and correlates with worse outcomes.
- INHBA promotes cancer cell growth, migration, and tumor formation in animal models.
- INHBA activates the MAPK pathway via ITGA6, suggesting a new therapeutic target.

## Abstract

Gastric cancer (GC) is among the most prevalent malignancies worldwide, ranking as the fifth most common cancer and the fifth leading cause of cancer-related mortality. This study intends to investigate how Inhibin subunit beta A (INHBA) promotes the progression of GC by activating the mitogen-activated protein kinase (MAPK) signaling pathway via targeting Integrin alpha-6 (ITGA6).

Quantitative reverse transcription-Polymerase Chain Reaction (qRT-PCR) and Immunohistochemistry (IHC) were utilised to validate the expression levels of INHBA in GC, which were subsequently correlated with the clinicopathological factors and outcomes. Cellular and animal studies were conducted to ascertain the role of INHBA in GC. RNA-sequencing (RNA-seq) and bioinformatics analysis were used to screen for the downstream target and pathway of INHBA, with Co-immunoprecipitation (Co-IP), Co-Immunofluorescent (Co-IF), Western blot (WB) and Rescue experiments validating their mechanisms of action in GC.

IHC and qRT–PCR analysis confirmed that GC tissues exhibited higher INHBA expression than adjacent noncancerous tissues. This elevated INHBA expression was found to be significantly associated with the incidence of tumor lesions, lymph node metastasis, and progression to higher TNM stages. Functional experiments showed that INHBA promoted GC cell proliferation and enhanced their migration and invasion in vitro while inhibiting apoptosis. Animal studies results indicated that INHBA overexpression promoted tumor growth and increased tumor weight and volume. Through a series of experiments, including RNA-seq, Co-IP, Co-IF, WB, and rescue assays, this study demonstrated that INHBA promotes GC progression by targeting ITGA6 to regulate the MAPK signaling pathway.

INHBA/ITGA6/MAPK axis can provide new insights into GC therapy. Targeted INHBA inhibition holds promise as a therapeutic approach for GC treatment.

## Linked entities

- **Genes:** INHBA (inhibin subunit beta A) [NCBI Gene 3624], ITGA6 (integrin subunit alpha 6) [NCBI Gene 3655]
- **Diseases:** gastric cancer (MONDO:0001056)

## Full-text entities

- **Genes:** GAPDH (glyceraldehyde-3-phosphate dehydrogenase) [NCBI Gene 2597] {aka G3PD, GAPD, HEL-S-162eP}, Inhba (inhibin beta-A) [NCBI Gene 16323], Mki67 (antigen identified by monoclonal antibody Ki 67) [NCBI Gene 17345] {aka D630048A14Rik, Ki-67, Ki67}, MAPK1 (mitogen-activated protein kinase 1) [NCBI Gene 5594] {aka ERK, ERK-2, ERK2, ERT1, MAPK2, NS13}, TGFB1 (transforming growth factor beta 1) [NCBI Gene 7040] {aka CAEND1, CED, DPD1, IBDIMDE, LAP, TGF-beta1}, MAP2K7 (mitogen-activated protein kinase kinase 7) [NCBI Gene 5609] {aka JNKK2, MAPKK7, MEK, MEK 7, MKK7, PRKMK7}, POTEF (POTE ankyrin domain family member F) [NCBI Gene 728378] {aka A26C1B, POTE2alpha, POTEACTIN}, ANXA5 (annexin A5) [NCBI Gene 308] {aka ANX5, CPB-I, ENX2, HEL-S-7, PP4, RPRGL3}, INHBA (inhibin subunit beta A) [NCBI Gene 3624] {aka EDF, FRP}, Itga6 (integrin alpha 6) [NCBI Gene 16403] {aka 5033401O05Rik, Cd49f, VLA-6}, ITGA6 (integrin subunit alpha 6) [NCBI Gene 3655] {aka CD49f, ITGA6A, ITGA6B, JEB6, VLA-6}, MAP2K1 (mitogen-activated protein kinase kinase 1) [NCBI Gene 5604] {aka CFC3, MAPKK1, MEK1, MEL, MKK1, PRKMK1}
- **Diseases:** ovarian cancer (MESH:D010051), colorectal and breast cancers (MESH:D001943), lymph node metastasis (MESH:D008207), necrotic (MESH:D009336), esophageal carcinoma (MESH:D004938), hepatocellular carcinoma (MESH:D006528), esophageal squamous cancer (MESH:D018307), signet-ring cell carcinoma (MESH:D018279), colorectal cancer (MESH:D015179), immunodeficient (MESH:D007153), tumorigenic (MESH:D002471), metastasis (MESH:D009362), gastric carcinogenesis (MESH:D063646), Gastric Cancer (MESH:D013274), neuroblastoma (MESH:D009447), genetic disease (MESH:D030342), pancreatic cancer (MESH:D010190), cervical cancer (MESH:D002583), cancers (MESH:D009369)
- **Chemicals:** PFA (MESH:C003043), CO2 (MESH:D002245), neomycin (MESH:D009355), polyvinylidene fluoride (MESH:C024865), PBS (MESH:D007854), penicillin (MESH:D010406), G418 (MESH:C010680), HE (MESH:D006371), crystal violet (MESH:D005840), Annexin-FITC (-), phosphatidylserine (MESH:D010718), CCK-8 (MESH:D012844), SDS (MESH:D012967), PI (MESH:D010716), paraffin (MESH:D010232), polyacrylamide (MESH:C016679), streptomycin (MESH:D013307), nitrogen (MESH:D009584), FITC (MESH:D016650)
- **Species:** Homo sapiens (human, species) [taxon 9606], Mycoplasma (genus) [taxon 2093], Mus musculus (house mouse, species) [taxon 10090]
- **Cell lines:** HGC-27 — Homo sapiens (Human), Gastric carcinoma, Cancer cell line (CVCL_1279), NUGC-3 — Homo sapiens (Human), Gastric adenocarcinoma, Cancer cell line (CVCL_1612), GES-1 — Homo sapiens (Human), Transformed cell line (CVCL_EQ22), Hs746T — Homo sapiens (Human), Gastric adenocarcinoma, Cancer cell line (CVCL_0333), AGS — Homo sapiens (Human), Gastric adenocarcinoma, Cancer cell line (CVCL_0139)

## Full text

_Full body text omitted from this summary view._ Fetch the complete paper as Markdown: https://tomesphere.com/paper/PMC12963699/full.md

## Figures

7 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12963699/full.md

## References

32 references — full list in the complete paper: https://tomesphere.com/paper/PMC12963699/full.md

---
Source: https://tomesphere.com/paper/PMC12963699