Fibroblast growth factor 4 is a protein that in humans is encoded by the FGF4gene.[1][2]
The protein encoded by this gene is a member of the fibroblast growth factor (FGF) family. FGF family members possess broad mitogenic and cell survival activities and are involved in a variety of biological processes including embryonic development, cell growth, morphogenesis, tissue repair, tumor growth and invasion. This gene was identified by its oncogenic transforming activity. This gene and FGF3, another oncogenic growth factor, are located closely on chromosome 11. Co-amplification of both genes was found in various kinds of human tumors. Studies on the mouse homolog suggested a function in bone morphogenesis and limb development through the sonic hedgehog (SHH) signaling pathway.[2]
Function
During embryonic development, the 21-kD protein FGF4 functions as a signaling molecule that is involved in many important processes.[3][4] Studies using Fgf4 gene knockout mice showed developmental defects in embryos both in vivo and in vitro, revealing that FGF4 facilitates the survival and growth of the inner cell mass during the postimplantation phase of development by acting as an autocrine or paracrine ligand.[3] FGFs produced in the apical ectodermal ridge (AER) are critical for the proper forelimb and hindlimb outgrowth.[5] FGF signaling in the AER is involved in regulating limb digit number and cell death in the interdigital mesenchyme.[6] When FGF signaling dynamics and regulatory processes are altered, postaxial polydactyly and cutaneous syndactyly, two phenotypic abnormalities collectively known as polysyndactyly, can occur in the limbs. Polysyndactyly is observed when an excess of Fgf4 is expressed in limb buds of wild-type mice. In mutant limb buds that do not express Fgf8, the expression of Fgf4 still results in polysyndactyly, but Fgf4 is also able to rescue all skeletal defects that arise from the lack of Fgf8. Therefore, the Fgf4 gene compensates for the loss of the Fgf8 gene, revealing that FGF4 and FGF8 perform similar functions in limb skeleton patterning and limb development.[6] Studies of zebrafish Fgf4 knockdown embryos demonstrated that when Fgf4 signaling is inhibited, randomized left-right patterning of the liver, pancreas, and heart takes place, showing that Fgf4 is a crucial gene involved in developing left-right patterning of visceral organs. Furthermore, unlike the role of FGF4 in limb development, FGF4 and FGF8 have distinct roles and function independently in the process of visceral organ left-right patterning.[7]
Fgf signaling pathway has also been demonstrated to drive hindgut identity during gastrointestinal development, and the up regulation of the Fgf4 in pluripotent stem cell has been used to direct their differentiation for the generation of intestinal Organoids and tissues in vitro.[8]
References
↑Galland F, Stefanova M, Lafage M, Birnbaum D (Jul 1992). "Localization of the 5' end of the MCF2 oncogene to human chromosome 15q15----q23". Cytogenetics and Cell Genetics. 60 (2): 114–6. doi:10.1159/000133316. PMID1611909.
↑ 3.03.1Feldman B, Poueymirou W, Papaioannou VE, DeChiara TM, Goldfarb M (Jan 1995). "Requirement of FGF-4 for postimplantation mouse development". Science. 267 (5195): 246–9. doi:10.1126/science.7809630. PMID7809630.
↑Yuan H, Corbi N, Basilico C, Dailey L (Nov 1995). "Developmental-specific activity of the FGF-4 enhancer requires the synergistic action of Sox2 and Oct-3". Genes & Development. 9 (21): 2635–45. doi:10.1101/gad.9.21.2635. PMID7590241.
↑Boulet AM, Moon AM, Arenkiel BR, Capecchi MR (Sep 2004). "The roles of Fgf4 and Fgf8 in limb bud initiation and outgrowth". Developmental Biology. 273 (2): 361–72. doi:10.1016/j.ydbio.2004.06.012. PMID15328019.
↑ 6.06.1Lu P, Minowada G, Martin GR (Jan 2006). "Increasing Fgf4 expression in the mouse limb bud causes polysyndactyly and rescues the skeletal defects that result from loss of Fgf8 function". Development. 133 (1): 33–42. doi:10.1242/dev.02172. PMID16308330.
↑Yamauchi H, Miyakawa N, Miyake A, Itoh N (Aug 2009). "Fgf4 is required for left-right patterning of visceral organs in zebrafish". Developmental Biology. 332 (1): 177–85. doi:10.1016/j.ydbio.2009.05.568. PMID19481538.
↑Lancaster MA, Knoblich JA (2014). "Organogenesis in a dish: modeling development and disease using organoid technologies". Science. 345 (6194): 1247125. doi:10.1126/science.1247125. PMID25035496.
Further reading
Powers CJ, McLeskey SW, Wellstein A (Sep 2000). "Fibroblast growth factors, their receptors and signaling". Endocrine-Related Cancer. 7 (3): 165–97. doi:10.1677/erc.0.0070165. PMID11021964.
Delli Bovi P, Curatola AM, Kern FG, Greco A, Ittmann M, Basilico C (Aug 1987). "An oncogene isolated by transfection of Kaposi's sarcoma DNA encodes a growth factor that is a member of the FGF family". Cell. 50 (5): 729–37. doi:10.1016/0092-8674(87)90331-X. PMID2957062.
Wada A, Sakamoto H, Katoh O, Yoshida T, Yokota J, Little PF, Sugimura T, Terada M (Dec 1988). "Two homologous oncogenes, HST1 and INT2, are closely located in human genome". Biochemical and Biophysical Research Communications. 157 (2): 828–35. doi:10.1016/S0006-291X(88)80324-3. PMID2974287.
Huebner K, Ferrari AC, Delli Bovi P, Croce CM, Basilico C (1989). "The FGF-related oncogene, K-FGF, maps to human chromosome region 11q13, possibly near int-2". Oncogene Research. 3 (3): 263–70. PMID3060803.
Adelaide J, Mattei MG, Marics I, Raybaud F, Planche J, De Lapeyriere O, Birnbaum D (Apr 1988). "Chromosomal localization of the hst oncogene and its co-amplification with the int.2 oncogene in a human melanoma". Oncogene. 2 (4): 413–6. PMID3283658.
Ornitz DM, Xu J, Colvin JS, McEwen DG, MacArthur CA, Coulier F, Gao G, Goldfarb M (Jun 1996). "Receptor specificity of the fibroblast growth factor family". The Journal of Biological Chemistry. 271 (25): 15292–7. doi:10.1074/jbc.271.25.15292. PMID8663044.
Tanaka S; et al. (1998). "Promotion of trophoblast stem cell proliferation by FGF-4". Science. 282: 2072–2075. doi:10.1126/science.282.5396.2072.
Helland R, Berglund GI, Otlewski J, Apostoluk W, Andersen OA, Willassen NP, Smalås AO (Jan 1999). "High-resolution structures of three new trypsin-squash-inhibitor complexes: a detailed comparison with other trypsins and their complexes". Acta Crystallographica Section D. 55 (Pt 1): 139–48. doi:10.1107/S090744499801052X. PMID10089404.
Britto JA, Evans RD, Hayward RD, Jones BM (Dec 2001). "From genotype to phenotype: the differential expression of FGF, FGFR, and TGFbeta genes characterizes human cranioskeletal development and reflects clinical presentation in FGFR syndromes". Plastic and Reconstructive Surgery. 108 (7): 2026–39, discussion 2040–6. doi:10.1097/00006534-200112000-00030. PMID11743396.
Sieuwerts AM, Martens JW, Dorssers LC, Klijn JG, Foekens JA (Apr 2002). "Differential effects of fibroblast growth factors on expression of genes of the plasminogen activator and insulin-like growth factor systems by human breast fibroblasts". Thrombosis and Haemostasis. 87 (4): 674–83. PMID12008951.
Koh KR, Ohta K, Nakamae H, Hino M, Yamane T, Takubo T, Tatsumi N (Oct 2002). "Differential effects of fibroblast growth factor-4, epidermal growth factor and transforming growth factor-beta1 on functional development of stromal layers in acute myeloid leukemia". Leukemia Research. 26 (10): 933–8. doi:10.1016/S0145-2126(02)00033-4. PMID12163055.
Lopez-Sanchez C, Climent V, Schoenwolf GC, Alvarez IS, Garcia-Martinez V (Aug 2002). "Induction of cardiogenesis by Hensen's node and fibroblast growth factors". Cell and Tissue Research. 309 (2): 237–49. doi:10.1007/s00441-002-0567-2. PMID12172783.