Copyright
©The Author(s) 2022.
World J Gastroenterol. Sep 7, 2022; 28(33): 4744-4761
Published online Sep 7, 2022. doi: 10.3748/wjg.v28.i33.4744
Published online Sep 7, 2022. doi: 10.3748/wjg.v28.i33.4744
Table 1 Characteristics of individual colorectal cancer subtypes
| CMS1 | CMS2 | CMS3 | CMS4 |
| (MSI immune) | (Canonical) | (Metabolic) | (Mesenchymal) |
| CIMP high | CIN | CIN, CIMP low | CIN |
| Hypermethylation | |||
| SCNA-low | SCNA-high | SCNA-intermediate | SCNA-high |
| BRAF mutant | KRAS mutant | ||
| Activation of immune cells | WNT, MYC activation | Metabolic deregulation | TGF- activation |
| Worse survival after relapse | Superior survival after relapse | Worse relapse-free and overall survival |
Table 2 Roles of individual small mothers against decapentaplegic homolog proteins in the onset and progression of colorectal cancer
| Type of SMAD | Role in colorectal cancer | References |
| SMAD1 | Participates in the modification of cell growth, differentiation, apoptosis and other processes that are essential in the regulation of the body’s immune system | [39-42] |
| Promotes epithelial-mesenchymal transition process | ||
| By increasing the expression of ATG5 induces autophagy | ||
| SMAD2 | Inhibits the expression of related functional genes, cell proliferation and regulates the transcriptional response that promotes cell apoptosis | [43,44] |
| Expression of SMAD2 is correlated with patient survival | ||
| SMAD3 | In the formation of a tumor, depending on the stage of the cancer, it plays the double role of an oncogene or a tumor suppressor gene | [45-48] |
| Reduces its expression through mir-4429, and inhibits the appearance, development and metastasis of cancer cells | ||
| SMAD4 | Plays a very important role in the transduction of the TGF-β signaling pathway | [32,49] |
| Maintains the cell cycle in the G1 phase, which leads to abnormal tumor proliferation | ||
| Is a tumor suppressor gene | ||
| High mutation rate of SMAD4 in CRC patients was associated with poor prognosis, but not with clinical stage | ||
| SMAD5 | Mediates TGF-β superfamily ligand signaling pathway and thus influences cancer progression | [50] |
| No relevant studies on the role of SMAD5 in CRC patients have been found in the last 5 years | ||
| SMAD6 | Regulates TGF-β signaling pathway, promotes angiogenesis, stimulates extracellular matrix, and inhibits immunity, thus contributing to tumor growth, diffusion, and metastasis | [51] |
| No relevant studies on the role of SMAD6 in CRC patients have been found in the last 5 years | ||
| SMAD7 | Plays a dual role in different tumor stages, acting as a tumor suppressor gene by inhibiting proliferation and promoting apoptosis in the early stage, and increasing invasion in the late stage, promoting epithelial-mesenchymal transition, which correlates with the degree of malignancy | [52,53] |
Table 3 Clinical trials of drugs for the treatment of colorectal cancer (United States National Library of Medicine; ClinicalTrials.gov)
| Clinical trials (phase) | Drug | Target | Mechanism of action |
| Antisense oligonucleotides | |||
| NCT00844064 (I) | AP12009 (trabedersen) | TGF-β2 | By binding to TGF-βII mrna, its expression is reduced |
| Antibodies | |||
| NCT04952753 (II) | NIS793 | TGF-β | Reduction of active cytokine, reduction of SMAD2/3 phosphorylation, and reduction of TGF-β target gene expression |
| NCT02947165 (I) | NIS793 | TGF-β | Reduction of active cytokine, reduction of SMAD2/3 phosphorylation, and reduction of TGF-β target gene expression |
| NCT01646203(I) | IMC-TR1 | TGF-βRII | Reduction of active cytokine, reduction of SMAD2/3 phosphorylation, and reduction of TGF-β target gene expression |
| Ligand traps | |||
| NCT03436563 (I/II) | M7824 | TGF-βRII | Bifunctional anti-PD-L1/TGF-βRII trap fusion protein |
| NCT02517398(I) | Bintrafusp alfa | TGF-βRII and PD-L1 | First-in-class bifunctional fusion protein composed of a mab against PD-L1 fused to the extracellular domain of the TGF-β receptor II |
| NCT04856787 (II/III) | SHR-1701 | TGF-βRII | Bifunctional anti-PD-L1/TGF-βRII agent |
| Small molecule receptor kinase inhibitors | |||
| NCT04031872 (I/II) | LY3200882; capecitabine | TGF-βRI | By blocking ATP binding to TGF-βR, receptor kinase activity and signal transduction are reduced |
| NCT05400122 (I) | Vactosertib | TGF-βRI | Inhibits the activity of TGF-βR1 |
| NCT03724851 (I/II) | Vactosertib + Pembroli-zumab | TGF-βRI | Inhibits the activity of TGF-βR1 |
| NCT03470350 (I/II) | Galunisertib | TGF-βRI | Inhibits the activity of TGF-βR1 |
| Immune checkpoints | |||
| NCT04540159 | TGF-β1 | Measuring the level Active TGF-β1 by flow-cytometric analysis in the intraabdominal ascites | |
| Adoptive cell therapy | |||
| NCT03431311 (I/II) | ACT | TGF-βII | ACT with Radium-1 TCR + T cells transiently redirected against the TGF-βRII frameshift antigen which is expressed in MSI+ colon cancer. |
| NCT05040568 (I) | CB-NK-TGF-βR2-/NR3C1 | Immunotherapy with ex vivo preactivated and expanded CB-NK cells in combination with cetuximab | |
- Citation: Maslankova J, Vecurkovska I, Rabajdova M, Katuchova J, Kicka M, Gayova M, Katuch V. Regulation of transforming growth factor-β signaling as a therapeutic approach to treating colorectal cancer. World J Gastroenterol 2022; 28(33): 4744-4761
- URL: https://www.wjgnet.com/1007-9327/full/v28/i33/4744.htm
- DOI: https://dx.doi.org/10.3748/wjg.v28.i33.4744