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This Sandbox is Reserved from January through July 31, 2018 for use in the course HLSC322: Principles of Genetics and Genomics taught by Genevieve Houston-Ludlam at the University of Maryland, College Park, USA. This reservation includes Sandbox Reserved 1311 through Sandbox Reserved 1430.

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Coagulation Factor VIII (FVIII)

Structure

The Factor VIII polypeptide chain consists of 3 A domains, a B domains, and 2 C domains (A1-A2-B-A3-C1-C2). The A domains are homologous to ceruloplasmin, a copper binding protein; the C domains are homologous to phospholipid binding lectin, which has an effect on binding to other proteins. The polypeptide is cleaved between the B-A3 domains to make the (A1-A2-B) and light (A3-C1-C2) chains as a heterodimeric protein before secretion. Thrombin then activates the heterodimer to cleave into the Factor VIIIa. The C2 domain contains the major binding motif that has high affinity and selectivity for membrane binding sites such as phosphatidylserine and is stereo selective to phosphatidyl-l-serine. This is where it interacts with the cofactor Factor IXa to form a tenase complex for the continuation of the coagulation cascade. Further research has shown that there is interaction between the first epidermal growth factor domain of factor IXa and the A3 domain of factor VIIIa as well as the serine protease domain of factor IXa and the A2 domain of factor VIIIa.

Function

Normally, Factor VIII forms a non-covalent complex with another clotting glycoprotein, the von Willebrand factor, after being released from endothelium cells or sinusoidal cells in the liver. When it is not interacting with other proteins such as the von Willebrand factor, it is proteolytically inactivated. After inactivation, it is taken out of the blood stream. Factor VIII mainly acts during the Tissue Factor Pathway of the coagulation cascade. In the presence of Thrombin, Factor VIII cleaves into a heterotrimeric protein with an exposed C2 part of the domain that includes the . This area interacts on its phosphatidyl-l-serine containing phospholipid membranes with its cofactor Factor IXa to form a tenase complex in the presence of Ca2+. The tenase complex speeds up the activation pathway for Factor X and blocks inhibitors, continuing the coagulation cascade. Factor X with its cofactor Factor Va activates more thrombin, which in turn cleaves fibrinogen into fibrin. Fibrin will polymerize and cross links to clot blood.

Genetics

Coagulation Factor VIII, otherwise known as Anti-Hemophilic Factor (AHF) is a glycoprotein procofactor. It is a single polypeptide chain coded by the F8 gene located on the X chromosome (Xq28). It is released by the vascular, glomerular, and tubular endothelium, and by sinusoidal cells in the liver. There are 1,300 known mutations in this gene, which could result in Factor VIII deficiency. Since it is part of the coagulation cascade, mutations creating deficiencies in Factor VIII result in the X-linked genetic disease Hemophilia A. Because of its importance to the coagulation cascade, concentrated Factor VIII from blood plasma is a key ingredient treatment for Hemophiliacs.

References

Blostein‡§, M. D., Furie¶, B. C., & And, I. R. (2003, August 15). Mark D. Blostein. Retrieved February 27, 2018, from http://www.jbc.org/content/278/33/31297.full
BW, S., PC, S., CH, C., JW, H., JS, L., J, K., . . . BL, S. (1970, January 01). BW. Retrieved February 27, 2018, from https://www.ebi.ac.uk/pdbe/entry/pdb/2r7e
F8 gene - Genetics Home Reference. (n.d.). Retrieved February 27, 2018, from https://ghr.nlm.nih.gov/gene/F8#
Factor VIII. (2018, February 27). Retrieved February 27, 2018, from https://en.wikipedia.org/wiki/Factor_VIII
Konkle, B. A. (2017, June 22). Hemophilia A. Retrieved February 27, 2018, from https://www.ncbi.nlm.nih.gov/books/NBK1404/
Saenko, E. L., Shima, M., Rajalakshmi, K. J., & Scandella, D. (1994, April 15). A role for the C2 domain of factor VIII in binding to von Willebrand factor. Retrieved February 27, 2018, from https://www.ncbi.nlm.nih.gov/pubmed/7512568

Retrieved from "http://52.214.119.220/wiki/index.php/Sandbox_Reserved_1349"

@@ Line 3: / Line 3: @@
 <StructureSection load='2r7e' size='340' side='right' caption='Coagulation Factor VIII structure.' scene=''>
 ===Structure===
+The Factor VIII polypeptide chain consists of 3 A domains, a B domains, and 2 C domains (A1-A2-B-A3-C1-C2). The A domains are homologous to ceruloplasmin, a copper binding protein; the C domains are homologous to phospholipid binding lectin, which has an effect on binding to other proteins.
+	The polypeptide is cleaved between the B-A3 domains to make the <scene name='77/777669/Fviii_heavy_chain/2'>heavy</scene> (A1-A2-B) and light (A3-C1-C2) chains as a heterodimeric protein before secretion. Thrombin then activates the heterodimer to cleave into the <scene name='77/777669/Domains/3'>heterotrimeric protein (A1, A2, A3-C1-C2)</scene> Factor VIIIa. The C2 domain contains the major binding motif that has high affinity and selectivity for membrane binding sites such as phosphatidylserine and is stereo selective to phosphatidyl-l-serine. This is where it interacts with the cofactor Factor IXa to form a tenase complex for the continuation of the coagulation cascade.
+	Further research has shown that there is interaction between the first epidermal growth factor domain of factor IXa and the A3 domain of factor VIIIa as well as the serine protease domain of factor IXa and the A2 domain of factor VIIIa.
-===Genetics===
-:FVIII is encoded by the ''F8'' gene, located on Xq28 (28th position on the q arm of the X chromosome).  Mutations in this gene are associated with hemophilia A, a X-linked recessive disorder.  There are 1,300 mutations associated with Hemophilia A in the F8 gene, ranging from single base substitutions to multi base indels.  These mutations typically lower the concentration of or inactivate the FVIII protein.  As it can no longer participate in the coagulation processes, blood clotting does not occur properly, leading to the excessive bleeding commonly seen in hemophilia.  The severity of hemophilia depends largely on the mutation, with loss-of-function mutations resulting in more severe hemophilia than those lowing FVIII'c concentration.
 ===Function===
+	Normally, Factor VIII forms a non-covalent complex with another clotting glycoprotein, the von Willebrand factor, after being released from endothelium cells or sinusoidal cells in the liver. When it is not interacting with other proteins such as the von Willebrand factor, it is proteolytically inactivated. After inactivation, it is taken out of the blood stream.
+Factor VIII mainly acts during the Tissue Factor Pathway of the coagulation cascade. In the presence of Thrombin, Factor VIII cleaves into a heterotrimeric protein with an exposed C2 part of the domain that includes the <scene name='77/777669/C2_binding_site/2'>highly selective membrane binding motif</scene>. This area interacts on its phosphatidyl-l-serine containing phospholipid membranes with its cofactor Factor IXa to form a tenase complex in the presence of Ca2+. The tenase complex speeds up the activation pathway for Factor X and blocks inhibitors, continuing the coagulation cascade. Factor X with its cofactor Factor Va activates more thrombin, which in turn cleaves fibrinogen into fibrin. Fibrin will polymerize and cross links to clot blood.
+===Genetics===
+Coagulation Factor VIII, otherwise known as Anti-Hemophilic Factor (AHF) is a glycoprotein procofactor. It is a single polypeptide chain coded by the F8 gene located on the X chromosome (Xq28). It is released by the vascular, glomerular, and tubular endothelium, and by sinusoidal cells in the liver.
+There are 1,300 known mutations in this gene, which could result in Factor VIII deficiency. Since it is part of the coagulation cascade, mutations creating deficiencies in Factor VIII result in the X-linked genetic disease Hemophilia A. Because of its importance to the coagulation cascade, concentrated Factor VIII from blood plasma is a key ingredient treatment for Hemophiliacs.
 </StructureSection>
 == References ==
-*https://ghr.nlm.nih.gov/gene/F8#
+*Blostein‡§, M. D., Furie¶, B. C., & And, I. R. (2003, August 15). Mark D. Blostein. Retrieved February 27, 2018, from http://www.jbc.org/content/278/33/31297.full
-*https://www.ebi.ac.uk/pdbe/entry/pdb/2r7e
+*BW, S., PC, S., CH, C., JW, H., JS, L., J, K., . . . BL, S. (1970, January 01). BW. Retrieved February 27, 2018, from https://www.ebi.ac.uk/pdbe/entry/pdb/2r7e
-*https://en.wikipedia.org/wiki/Factor_VIII
+*F8 gene - Genetics Home Reference. (n.d.). Retrieved February 27, 2018, from https://ghr.nlm.nih.gov/gene/F8#
+*Factor VIII. (2018, February 27). Retrieved February 27, 2018, from https://en.wikipedia.org/wiki/Factor_VIII
+*Konkle, B. A. (2017, June 22). Hemophilia A. Retrieved February 27, 2018, from https://www.ncbi.nlm.nih.gov/books/NBK1404/
+*Saenko, E. L., Shima, M., Rajalakshmi, K. J., & Scandella, D. (1994, April 15). A role for the C2 domain of factor VIII in binding to von Willebrand factor. Retrieved February 27, 2018, from https://www.ncbi.nlm.nih.gov/pubmed/7512568
 <references/>

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Coagulation Factor VIII (FVIII)

Structure

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