Wednesday, August 6, 2014

The future of Hemophilia

The future of Hemophilia is Gene Therapy. Currently we treat those with Hemophilia by supplying them with the missing protein coagulation factor they lack, but this treatment does not actually cure the patient and has a very high treatment burden. The current goal of the future is to find a way to correct the harmful mutation that leads to the Hemophilia disorders manifestation. Positive results from gene therapy have been achieved in animals such as dogs and mice, but we have yet to break through with a humans.  

"Before the gene treatment, the animals experienced about five serious bleeding events a year. After receiving the novel gene therapy, though, they experienced substantially fewer bleeding events over three years, as reported in the journal Nature Communications."

"“We’ve cured mice 10 different ways,” says Trent Spencer, Ph.D., director of the Gene Therapy Laboratory at the Aflac Cancer Center and Assistant Professor of Pediatrics with Emory University School of Medicine.
“We can cure a mouse of hemophilia with our eyes closed. Getting from a mouse to a human, however, is a massive step and that is what we’re trying to do now.”
  
  
Currently the biggest block in the progression of gene therapy is the potential commercialism of a new treatment. Companies are less willing to invest in creating a product that would be very expensive initially to offset the development cost, as well as possibly unpopular due to moral concerns. Why risk bringing gene therapy treatments to the market when you already have a working, profitable traditional hemophilia treatments in place? Those with the most to gain from a gene therapy treatment for hemophilia would be individuals living in developmental countries. One hight-tech intervention is much more feasible than creating an infrastructure that would allow for an individual to receive daily treatments.   It will be interesting to see where Hemophilia is ten years from now, when the cost of gene therapy may be cheaper and the general public more accepting of gene manipulation. 

References:

Du, Lily M., et al. "Platelet-targeted gene therapy with human factor VIII establishes haemostasis in dogs with haemophilia A." Nature communications4 (2013).

"Gene Therapy and Hemophilia A - Children's Healthcare of Atlanta."Children's Healthcare of Atlanta. N.p., n.d. Web. 02 Aug. 2014.


Saturday, August 2, 2014

Coagulation Factor VIII



The Coagulation Factor VIII Gene, known as F8, is located on the X chromosome. Most cases of Hemophilia are caused by a mutation on the F8 gene that produces the Factor VIII. The mutation is often caused by point mutations or inversions that lead to a disruption of the factor creation. Lakich et al (1993) found in approximately 45% of families with severe disease “recombination between the homologous F8A sequences within intron 22 and upstream of the F8 gene. Such a recombination would lead to an inversion of all intervening DNA and a disruption of the gene.” Furthermore, in a study of 147 cases of severe hemophilia A, done by Becker et al. (1996) found a “causative defect in the F8 gene in 126 patients (85.7%). An inversion of the gene was found in 55 patients (37.4%), a point mutation in 47 (32%), a small deletion in 14 (9.5%), a large deletion in 8 (5.4%), and a small insertion in 2 (1.4%). “





More Gene information can be found hereRefSeq Gene Information, and
FASTA Gene Sequence.


Coagulation factor protein VIII is produced from this gene:


The Coagulation factor VIII protein is very important in the blood coagulation cascade that results in blood clots forming.  

A video explaining the coagulation cascade:  






An even simpler explanation:

Those with the Hemophilia disorder A have a mutation that leads to the production of faulty Coagulation factor VIII protein; this mutation is often caused by a point mutations: inversions, deletions, or missense mutations
To give a very simple example of what a point mutation is, using words in place of codons, instead of the DNA's message being, "the cat sleeps", it could be either, "the cat 'sleeps'" (silent mutation),  "the cat ... " (nonsense), or "the cat runs" (missense). 

Additionally, the Coagulation factor VIII protein is highly conserved amongst organisms. The Coagulation factor VIII protein is a very efficient way to coagulate blood and thus has been maintained from a common ancestor through several species. Making a phylogeny tree of the Coagulation factor VIII you would see that humans and chimpanzees both have a highly related Coagulation factor VIII - but you would also see that humans and Danio Rerio (zebrafish) are also very closely related. For this reason animals research is very important to helping learn more about and treat Hemophilia.  


 
References: 

Becker, J., Schwaab, R., Moller-Taube, A., Schwaab, U., Schmidt, W., Brackmann, H. H., Grimm, T., Olek, K., Oldenburg, J. Characterization of the factor VIII defect in 147 patients with sporadic hemophilia A: family studies indicate a mutation type-dependent sex ratio of mutation frequencies. Am. J. Hum. Genet. 58: 657-670 (1996)

Bowen, D. J. "Haemophilia A and haemophilia B: molecular insights." Molecular Pathology 55.1 (2002): 1

ChristensenUniversity of Wisconsin-Madison, Allison. "Phylogeny."Coagulation Factor VIII and Hemophilia A. University of Wisconsin-Madison, 19 May 2013. Web. 19 July 2014.

"Coagulation Cascade." YouTube. Ferrosan Medical Devices10, 10 Sept. 2010. Web. 07 Aug. 2014.
Naoum, Paulo C., and Alia F. Naoum. "Hemostasis, Coagulation and Fibrinolisis." YouTube. YouTube, 12 Mar. 2010. Web. 07 Aug. 2014


Lakich, D., Kazazian, H. H., Jr., Antonarakis, S. E., Gitschier, J. Inversions disrupting the factor VIII gene are a common cause of severe haemophilia A. Nature Genet. 5: 236-241, (1993)

"Point Mutation." Wikipedia. Wikimedia Foundation, 08 Feb. 2014. Web. 02 Aug. 2014.

"The Genomic Era !" The Genomic Era ! N.p., n.d. Web. 02 Aug. 2014.