# The Two-Way Role of Jagged1 in Cancer: A Focus on CRC

**Authors:** Sabrina Zema, Francesca Di Fazio, Rocco Palermo, Claudio Talora, Diana Bellavia

PMC · DOI: 10.3390/cells14221815 · 2025-11-19

## TL;DR

Jagged1 plays a dual role in colorectal cancer by promoting tumor growth and drug resistance through both normal and reverse signaling.

## Contribution

The paper highlights Jagged1 as a novel oncogenic driver in CRC through its non-canonical reverse signaling.

## Key findings

- Jagged1 is cleaved to release Jag1-ICD, which exhibits oncogenic properties in CRC.
- Jagged1 contributes to the adenoma-to-carcinoma progression in CRC.
- Understanding Jagged1's dual role may lead to new strategies for overcoming drug resistance in CRC.

## Abstract

What are the main findings?
Jagged1 is cleaved, releasing an intracellular domain (Jag1-ICD).Jag1-ICD acquires oncogenic properties in CRC.

Jagged1 is cleaved, releasing an intracellular domain (Jag1-ICD).

Jag1-ICD acquires oncogenic properties in CRC.

What are the implications of the main findings?
Jagged1 is a novel oncogenic driver that contributes to the multistep genetic model underlying the adenoma-to-carcinoma sequence in CRC.Understanding the two-way role of Jagged1 could lead to new strategies for addressing drug resistance in CRC.

Jagged1 is a novel oncogenic driver that contributes to the multistep genetic model underlying the adenoma-to-carcinoma sequence in CRC.

Understanding the two-way role of Jagged1 could lead to new strategies for addressing drug resistance in CRC.

Colorectal cancer (CRC) remains one of the most prevalent and lethal malignancies. Accumulating genetic evidence supports a multistep model of tumor progression, in which early APC loss leads to chromosomal instability and adenoma formation, followed by activating mutations in KRAS that synergize with β-catenin signaling to promote tumor growth and invasion. Among the downstream effectors of these pathways, the Notch ligand Jagged1 has emerged as a critical mediator of CRC progression and chemoresistance. Jagged1 is not only a transcriptional target of the Wnt/β-catenin axis but also undergoes proteolytic cleavage via the KRAS/ERK/ADAM17 signaling cascade, generating a nuclear Jagged1 intracellular domain (Jag1-ICD) that drives reverse signaling. This dual functionality, activating canonical Notch signaling and initiating reverse nuclear signaling, positions Jagged1 as a key oncogenic driver in CRC. In this review, we first summarize the role of Jagged1 as an integral part of canonical Notch signaling. We then focus on the non-canonical Jagged1 reverse signaling function in cancer, with a particular emphasis on CRC. We underscore the dual role of Jagged1 in tumor biology and propose that it functions as a novel oncogene within the adenoma-to-carcinoma sequence, supporting CRC development and drug resistance via non-canonical mechanisms.

## Linked entities

- **Genes:** jag1.L (jagged 1 L homeolog) [NCBI Gene 399110], APC (APC regulator of Wnt signaling pathway) [NCBI Gene 324], KRAS (KRAS proto-oncogene, GTPase) [NCBI Gene 3845], ctnnb1.S (catenin beta 1 S homeolog) [NCBI Gene 380441]
- **Proteins:** Notch (neurogenic locus notch homolog), ADAM17 (ADAM metallopeptidase domain 17)
- **Diseases:** CRC (MONDO:0005575), colorectal cancer (MONDO:0005575)

## Full-text entities

- **Genes:** KRAS (KRAS proto-oncogene, GTPase) [NCBI Gene 3845] {aka 'C-K-RAS, C-K-RAS, CFC2, K-RAS2A, K-RAS2B, K-RAS4A}, CTNNB1 (catenin beta 1) [NCBI Gene 1499] {aka CTNNB, EVR7, MRD19, NEDSDV, armadillo}, ADAM17 (ADAM metallopeptidase domain 17) [NCBI Gene 6868] {aka ADAM18, CD156B, CSVP, HYPT16, NISBD, NISBD1}, APC (APC regulator of Wnt signaling pathway) [NCBI Gene 324] {aka BTPS2, DESMD, DP2, DP2.5, DP3, GS}, JAG1 (jagged canonical Notch ligand 1) [NCBI Gene 182] {aka AGS, AGS1, AHD, AWS, CD339, CMT2HH}, MAPK1 (mitogen-activated protein kinase 1) [NCBI Gene 5594] {aka ERK, ERK-2, ERK2, ERT1, MAPK2, NS13}
- **Diseases:** CRC (MESH:D015179), Cancer (MESH:D009369), adenoma (MESH:D000236)

## Figures

3 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12650915/full.md

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Source: https://tomesphere.com/paper/PMC12650915