# Somatostatin Effect on Growth Factors in Hepatocellular Carcinoma

**Authors:** Angeliki Tsakou, George Notas, Costantinos Xidakis, Ioannis Tsomidis, Elias Kouroumalis, Argyro Voumvouraki

PMC · DOI: 10.3390/cimb48020134 · 2026-01-26

## TL;DR

This study shows that somatostatin and its analog octreotide affect growth factors linked to liver diseases and hepatocellular carcinoma.

## Contribution

The study demonstrates the impact of somatostatin and octreotide on multiple growth factors in patients with liver diseases.

## Key findings

- Octreotide and somatostatin significantly reduced Gastrin levels in HCC and cirrhosis.
- IGF1 levels were reduced in HCC and cirrhosis but not in chronic hepatitis C.
- HGF levels increased in HCC and cirrhosis and were further elevated after treatment.

## Abstract

Growth factors play a significant role in the immunopathogenesis of liver diseases, especially liver cirrhosis and hepatocellular carcinoma (HCC). The somatostatin analog octreotide has been used as treatment in advanced HCC, based on its anti-neoplastic effects in vitro. Therefore, the effect of somatostatin and octreotide was studied on several growth factors in patients with HCC. Nineteen patients with advanced HCC were treated with octreotide and compared with thirty-seven patients with viral cirrhosis (19 decompensated) treated with intravenous somatostatin for severe bleeding from portal gastropathy. Five growth factors, namely Gastrin, Insulin-like growth factor 1 (IGF 1), Hepatocyte growth factor (HGF), Stem cell factor (SCF) and Vascular endothelial growth factor (VEGF) were measured in serum before and after treatment with specific commercially available ELISAs. Seventeen healthy individuals and nineteen patients with chronic viral hepatitis C (CAH) were used as pre-treatment controls. Eighteen patients with advanced Primary Biliary Cholangitis (stage III and IV) before and after Ursodeoxycholic acid (UDCA) treatment were also studied. Pre-treatment levels of Gastrin were significantly increased in HCC, cirrhosis and PBC but not in CAH. Levels were significantly reduced by octreotide or somatostatin but also by UDCA in PBC. By contrast, IGF1 showed a mirror image being significantly reduced in HCC, cirrhosis and PBC, but not in CAH. Post-treatment levels were reduced in all groups, but not in PBC. Levels of HGF were significantly increased in HCC and cirrhosis but not in CAH and PBC. They were further increased in HCC after treatment. SCF increased only in HCC and was reduced after octreotide but not after somatostatin treatment. VEGF was reduced in cirrhosis and CAH but not in PBC. It was not significantly increased in HCC, but it was reduced by octreotide and was increased after UDCA. In this retrospective observational study, somatostatin and its analog octreotide have a significant effect on several growth factors involved in HCC pathogenesis.

## Linked entities

- **Proteins:** gastrin (gastrin/cholecystokinin-like peptide)
- **Chemicals:** octreotide (PubChem CID 448601), somatostatin (PubChem CID 16129706), Ursodeoxycholic acid (PubChem CID 31401)
- **Diseases:** Hepatocellular Carcinoma (MONDO:0007256), Primary Biliary Cholangitis (MONDO:0005388)

## Full-text entities

- **Genes:** MET (MET proto-oncogene, receptor tyrosine kinase) [NCBI Gene 4233] {aka AUTS9, DA11, DFNB97, HGFR, RCCP2, c-Met}, PDCD1 (programmed cell death 1) [NCBI Gene 5133] {aka ADMIO4, AIMTBS, CD279, PD-1, PD1, SLEB2}, INS (insulin) [NCBI Gene 3630] {aka IDDM, IDDM1, IDDM2, ILPR, IRDN, MODY10}, IGF1 (insulin like growth factor 1) [NCBI Gene 3479] {aka IGF, IGF-I, IGFI, MGF}, GCG (glucagon) [NCBI Gene 2641] {aka GLP-1, GLP1, GLP2, GRPP}, AKT1 (AKT serine/threonine kinase 1) [NCBI Gene 207] {aka AKT, PKB, PKB-ALPHA, PRKBA, RAC, RAC-ALPHA}, STAT3 (signal transducer and activator of transcription 3) [NCBI Gene 6774] {aka ADMIO, ADMIO1, APRF, HIES}, NUP210 (nucleoporin 210) [NCBI Gene 23225] {aka GP210, POM210}, GGH (gamma-glutamyl hydrolase) [NCBI Gene 8836] {aka GATD10, GH}, CD34 (CD34 molecule) [NCBI Gene 947], EGF (epidermal growth factor) [NCBI Gene 1950] {aka HOMG4, URG}, HGF (hepatocyte growth factor) [NCBI Gene 3082] {aka DFNB39, F-TCF, HGFB, HPTA, SF}, VEGFA (vascular endothelial growth factor A) [NCBI Gene 7422] {aka L-VEGF, MVCD1, VEGF, VPF}, KITLG (KIT ligand) [NCBI Gene 4254] {aka DCUA, DFNA69, FPH2, FPHH, KL-1, Kitl}, GAST (gastrin) [NCBI Gene 2520] {aka GAS}, IGF2 (insulin like growth factor 2) [NCBI Gene 3481] {aka C11orf43, GRDF, IGF-II, PP9974, SRS3}, TGFB1 (transforming growth factor beta 1) [NCBI Gene 7040] {aka CAEND1, CED, DPD1, IBDIMDE, LAP, TGF-beta1}, KIT (KIT proto-oncogene, receptor tyrosine kinase) [NCBI Gene 3815] {aka C-Kit, CD117, MASTC, PBT, SCFR}, CD8A (CD8 subunit alpha) [NCBI Gene 925] {aka CD8, CD8alpha, IMD116, Leu2, p32}, SST (somatostatin) [NCBI Gene 6750] {aka SMST, SST1}, CSF2 (colony stimulating factor 2) [NCBI Gene 1437] {aka CSF, GMCSF}, CTSB (cathepsin B) [NCBI Gene 1508] {aka APPS, CPSB, KWE, RECEUP}, IGF1R (insulin like growth factor 1 receptor) [NCBI Gene 3480] {aka CD221, IGFIR, IGFR, JTK13}, DLAT (dihydrolipoamide S-acetyltransferase) [NCBI Gene 1737] {aka DLTA, E2, PBC, PDC-E2, PDCE2}, CCKBR (cholecystokinin B receptor) [NCBI Gene 887] {aka CCK-2R, CCK-B, CCK2R, GASR}, HIF1A (hypoxia inducible factor 1 subunit alpha) [NCBI Gene 3091] {aka HIF-1-alpha, HIF-1A, HIF-1alpha, HIF1, HIF1-ALPHA, MOP1}, IGFBP3 (insulin like growth factor binding protein 3) [NCBI Gene 3486] {aka BP-53, IBP-3, IBP3, IGFBP-3}, SP100 (SP100 nuclear body protein) [NCBI Gene 6672] {aka lysp100b}, PIK3CB (phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit beta) [NCBI Gene 5291] {aka P110BETA, PI3K, PI3KBETA, PIK3C1}, EGFR (epidermal growth factor receptor) [NCBI Gene 1956] {aka ERBB, ERBB1, ERRP, HER1, NISBD2, NNCIS}, IL2 (interleukin 2) [NCBI Gene 3558] {aka IL-2, TCGF, lymphokine}
- **Diseases:** antral tumors (MESH:D009369), CAH (MESH:D019698), liver cirrhosis (MESH:D008103), variceal bleeding (MESH:D014648), cirrhosis (MESH:D005355), cholestatic liver disease (MESH:D008107), sarcopenia (MESH:D055948), Chronic hepatitis (MESH:D006521), inflammation (MESH:D007249), disease (MESH:D004194), injury to (MESH:D014947), cirrhotic (MESH:D000094724), Compensated cirrhosis (MESH:D005902), hypoxia (MESH:D000860), Bleeding (MESH:D006470), autoimmune conditions (MESH:D001327), esophageal varices (MESH:D004932), gastric cancer (MESH:D013274), and stomach tumorigenesis (MESH:D063646), chronic liver injury (MESH:D056487), jaundice (MESH:D007565), chronic viral hepatitis (MESH:D006525), cholestatic disease (MESH:D002779), infections (MESH:D007239), acute liver injury (MESH:D017114), portal vein thrombosis (MESH:D012170), metastases (MESH:D009362), portal gastropathy (MESH:D006975), ascites (MESH:D001201), viral cirrhosis (MESH:D014777), stage III (MESH:D062706), HCC (MESH:D006528), Biliary Cholangitis (MESH:D008105), liver tumor (MESH:D008113), vein invasion (MESH:D009361), chronic (MESH:D002908), Decompensated cirrhosis (MESH:D006333), IV (MESH:D006011), liver injuries (MESH:D017093), hepatic encephalopathy (MESH:D006501), liver toxicity (MESH:D056486)
- **Chemicals:** acetaminophen (MESH:D000082), hydrochloric acid (MESH:D006851), sorafenib (MESH:D000077157), Octreotide (MESH:D015282), bevacizumab (MESH:D000068258), TACE (MESH:D002741), Proglumide (MESH:D011377), UDCA (MESH:D014580)
- **Species:** Mus musculus (house mouse, species) [taxon 10090], Homo sapiens (human, species) [taxon 9606]
- **Cell lines:** HepG2 — Homo sapiens (Human), Hepatoblastoma, Cancer cell line (CVCL_0027)

## Figures

10 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12939631/full.md

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Source: https://tomesphere.com/paper/PMC12939631