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FDC-SP

January 01, 1970

FDC-SP or follicular dendritic cell-secreted protein, is a small, secreted protein, located on chromosome 4 in humans. It is thought to play an immune role in the junctional epithelium at the gingival crevice in the human mouth. It is very similar in structure to statherin, a protein contained in saliva.[1] [2]

Structure and genetics edit

FDC-SP is a 68-amino acid protein containing a signal peptide at its N terminus, which is used for directing the transport of the protein. Adjacent to the signal peptide, the protein contains a highly charged N-terminal sequence.[2] The C-terminal half of FDC-SP is proline-rich and not highly conserved between species, but the alignment of proline residues within this region is highly conserved. FDC-SP homologues are only easily located within the human, rat, mouse and chimpanzee genome. There is a 70% sequence homology between mouse and rat[3] and a 45% homology between human and mouse. The N-terminal, however, is highly conserved between all three species and is thought to contain potential casein kinase 2 (CK2) phosphorylation sites. CK2 is a constitutively and widely expressed serine/threonine kinase that has many substrates related to signal transduction and cell growth regulation. Several casein genes have also been found nearby to the FDC-SP gene. Numerous genes that are expressed in oral tissues, including statherin, mucin, ameloblastin, histatin, enamelin and proline-rich protein are also located in close proximity to the FDC-SP gene. This indicates that the aforementioned genes may be expressed through the same mechanism. The recent evolutionary development of FDC-SP correlates with the development of certain aspects of the mammalian immune system and with the emergence of the follicular germinal centre (GC) reaction in secondary lymphoid tissues.[4]

 
Chromosome 4

Expression edit

In humans, FDC-SP was first found within follicular dendritic cell isolates from the tonsil, and later was found to be specifically expressed within the periodontal ligament. FDC-SP expression can be induced in human FDC-like cell lines by exposure to tumour necrosis factor (TNF). Exposure of human peripheral blood cells to LPS can also result in FDC-SP expression, but TNF exposure does not cause FDC-SP expression and similarly LPS exposure does not cause expression within FDC-like cell lines. Expression in mouse splenocytes can be induced by LPS in a similar manner to that of human peripheral blood cells.[4]

In mice, as in humans, FDC-SP is not expressed in B cells, but FDC-SP expression in FDCs can be dependent on B cells after their stimulation by CD40. After stimulation with CD40, B cells have been shown to be able to induce phenotypic changes in FDCs through the B cell's surface TNF expression. It has therefore been suggested that the expression of TNF cytokines by B cells causes FDC-SP expression within FDCs upon contact. This reaction is said to be typical during GC formation.[4]

FDC-SP is highly expressed in the junctional epithelium and well as in the tonsils, prostate, lymph nodes and trachea. The proline rich region in the C-terminal half bears some resemblance to the antimicrobial peptide Bac5. FDC-SP may therefore have a role in microbial defense in the oral cavity.[2]

Function edit

In transgenic mice engineered to constitutively express FDC-SP, the number and size of GCs formed after immunization with a T-dependent antigen significantly decreased. The position of these GCs is normal, but they do not form centres of highly-proliferating B cells, which us thought be due to FDC-SP affecting the development of GCs. The mechanism by which FDC-SP exerts its effects upon GC development is not currently known. The formation of FDC networks appears to be normal in transgenic mice, as does T cell response.[4]

FDC-SP is an amphipathic molecule, similar to surfactant proteins A and D, which are thought to be involved in the innate immune system of the lung. These proteins allow for the phagocytosis of bacteria by binding to them. Stathrin has been proposed to have similar properties, which itself possesses similar properties to FDC-SP. Stathrin can bind oral bacteria, so it has been proposed that FDC-SP acts as part of a host defence mechanism against oral pathogens.[3]

FDC-SP is thought to bind target cells through a specific receptor in a similar manner to cytokines and chemokines. Although it shares no sequence homology with chemokines or cytokines, FDC-SP has several properties in common with several inflammatory mediators, including molecular mass and amino acid composition. The FDC-SP gene is also located next to a group of proline-rich salivary peptide genes, which themselves are next several to CXC chemokine genes. FDC-SP has an effect on B cell migration when used in conjunction with L cells, and migration is significantly increased when the B cells are stimulated with anti-CD40 plus IL-4. The addition of anti-CD40 causes the B cells to resemble those found in the GC. Pertussis toxin inhibits the action of G proteins and B cells treated with the toxin were observed to migrate poorly in response to FDC-SP.[4]

FDC-SP has been found to have an unusually high level of expression in a number of tumours, including breast carcinoma, epithelial ovarian carcinoma and endometrial carcinoma. It is hypothesised that FDC-SP can influence cell motility by specific receptor binding in a similar manner to chemokines. It is also thought that FDC-SP can regulate the assembly of the actin cytoskeleton, which may have an effect on cell motility.[5]

References edit

  1. ^ Tamayuki Shinomura; et al. (November 28, 2008). "Adsorption of Follicular Dendritic Cell-secreted Protein (FDC-SP) onto Mineral Deposits". J. Biol. Chem. 283 (48): 33658–33664. doi:10.1074/jbc.M800719200. PMC 2662279. PMID 18806264.
  2. ^ a b c Aaron J. Marshall; et al. (September 1, 2002). "FDC-SP, a Novel Secreted Protein Expressed by Follicular Dendritic Cells". The Journal of Immunology. 169 (5): 2381–2389. doi:10.4049/jimmunol.169.5.2381. PMID 12193705.
  3. ^ a b Sayaka Nakamura; et al. (2005). "Identification of genes preferentially expressed in periodontal ligament: Specific expression of a novel secreted protein, FDC-SP". Biochemical and Biophysical Research Communications. 338 (2): 1197–1203. doi:10.1016/j.bbrc.2005.10.076. PMID 16259954.
  4. ^ a b c d e Monther Al-Alwan (2007). "Follicular Dendritic Cell Secreted Protein (FDC-SP) Regulates Germinal Center and Antibody Responses". The Journal of Immunology. 178 (12): 7859–7867. doi:10.4049/jimmunol.178.12.7859. PMID 17548624.
  5. ^ Changyu Wang (2010). "C4orf7 contributes to ovarian cancer metastasis by promoting cancer cell migration and invasion". Oncology Reports. 24 (4): 933–936. doi:10.3892/or_00000939. PMID 20811673.

January 01, 1970
follicular, dendritic, cell, secreted, protein, small, secreted, protein, located, chromosome, humans, thought, play, immune, role, junctional, epithelium, gingival, crevice, human, mouth, very, similar, structure, statherin, protein, contained, saliva, conten. FDC SP or follicular dendritic cell secreted protein is a small secreted protein located on chromosome 4 in humans It is thought to play an immune role in the junctional epithelium at the gingival crevice in the human mouth It is very similar in structure to statherin a protein contained in saliva 1 2 Contents 1 Structure and genetics 2 Expression 3 Function 4 ReferencesStructure and genetics editFDC SP is a 68 amino acid protein containing a signal peptide at its N terminus which is used for directing the transport of the protein Adjacent to the signal peptide the protein contains a highly charged N terminal sequence 2 The C terminal half of FDC SP is proline rich and not highly conserved between species but the alignment of proline residues within this region is highly conserved FDC SP homologues are only easily located within the human rat mouse and chimpanzee genome There is a 70 sequence homology between mouse and rat 3 and a 45 homology between human and mouse The N terminal however is highly conserved between all three species and is thought to contain potential casein kinase 2 CK2 phosphorylation sites CK2 is a constitutively and widely expressed serine threonine kinase that has many substrates related to signal transduction and cell growth regulation Several casein genes have also been found nearby to the FDC SP gene Numerous genes that are expressed in oral tissues including statherin mucin ameloblastin histatin enamelin and proline rich protein are also located in close proximity to the FDC SP gene This indicates that the aforementioned genes may be expressed through the same mechanism The recent evolutionary development of FDC SP correlates with the development of certain aspects of the mammalian immune system and with the emergence of the follicular germinal centre GC reaction in secondary lymphoid tissues 4 nbsp Chromosome 4Expression editIn humans FDC SP was first found within follicular dendritic cell isolates from the tonsil and later was found to be specifically expressed within the periodontal ligament FDC SP expression can be induced in human FDC like cell lines by exposure to tumour necrosis factor TNF Exposure of human peripheral blood cells to LPS can also result in FDC SP expression but TNF exposure does not cause FDC SP expression and similarly LPS exposure does not cause expression within FDC like cell lines Expression in mouse splenocytes can be induced by LPS in a similar manner to that of human peripheral blood cells 4 In mice as in humans FDC SP is not expressed in B cells but FDC SP expression in FDCs can be dependent on B cells after their stimulation by CD40 After stimulation with CD40 B cells have been shown to be able to induce phenotypic changes in FDCs through the B cell s surface TNF expression It has therefore been suggested that the expression of TNF cytokines by B cells causes FDC SP expression within FDCs upon contact This reaction is said to be typical during GC formation 4 FDC SP is highly expressed in the junctional epithelium and well as in the tonsils prostate lymph nodes and trachea The proline rich region in the C terminal half bears some resemblance to the antimicrobial peptide Bac5 FDC SP may therefore have a role in microbial defense in the oral cavity 2 Function editIn transgenic mice engineered to constitutively express FDC SP the number and size of GCs formed after immunization with a T dependent antigen significantly decreased The position of these GCs is normal but they do not form centres of highly proliferating B cells which us thought be due to FDC SP affecting the development of GCs The mechanism by which FDC SP exerts its effects upon GC development is not currently known The formation of FDC networks appears to be normal in transgenic mice as does T cell response 4 FDC SP is an amphipathic molecule similar to surfactant proteins A and D which are thought to be involved in the innate immune system of the lung These proteins allow for the phagocytosis of bacteria by binding to them Stathrin has been proposed to have similar properties which itself possesses similar properties to FDC SP Stathrin can bind oral bacteria so it has been proposed that FDC SP acts as part of a host defence mechanism against oral pathogens 3 FDC SP is thought to bind target cells through a specific receptor in a similar manner to cytokines and chemokines Although it shares no sequence homology with chemokines or cytokines FDC SP has several properties in common with several inflammatory mediators including molecular mass and amino acid composition The FDC SP gene is also located next to a group of proline rich salivary peptide genes which themselves are next several to CXC chemokine genes FDC SP has an effect on B cell migration when used in conjunction with L cells and migration is significantly increased when the B cells are stimulated with anti CD40 plus IL 4 The addition of anti CD40 causes the B cells to resemble those found in the GC Pertussis toxin inhibits the action of G proteins and B cells treated with the toxin were observed to migrate poorly in response to FDC SP 4 FDC SP has been found to have an unusually high level of expression in a number of tumours including breast carcinoma epithelial ovarian carcinoma and endometrial carcinoma It is hypothesised that FDC SP can influence cell motility by specific receptor binding in a similar manner to chemokines It is also thought that FDC SP can regulate the assembly of the actin cytoskeleton which may have an effect on cell motility 5 References edit Tamayuki Shinomura et al November 28 2008 Adsorption of Follicular Dendritic Cell secreted Protein FDC SP onto Mineral Deposits J Biol Chem 283 48 33658 33664 doi 10 1074 jbc M800719200 PMC 2662279 PMID 18806264 a b c Aaron J Marshall et al September 1 2002 FDC SP a Novel Secreted Protein Expressed by Follicular Dendritic Cells The Journal of Immunology 169 5 2381 2389 doi 10 4049 jimmunol 169 5 2381 PMID 12193705 a b Sayaka Nakamura et al 2005 Identification of genes preferentially expressed in periodontal ligament Specific expression of a novel secreted protein FDC SP Biochemical and Biophysical Research Communications 338 2 1197 1203 doi 10 1016 j bbrc 2005 10 076 PMID 16259954 a b c d e Monther Al Alwan 2007 Follicular Dendritic Cell Secreted Protein FDC SP Regulates Germinal Center and Antibody Responses The Journal of Immunology 178 12 7859 7867 doi 10 4049 jimmunol 178 12 7859 PMID 17548624 Changyu Wang 2010 C4orf7 contributes to ovarian cancer metastasis by promoting cancer cell migration and invasion Oncology Reports 24 4 933 936 doi 10 3892 or 00000939 PMID 20811673 Retrieved from https en wikipedia org w index php title FDC SP amp oldid 1193957446, wikipedia, wiki, book, books, library,

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