Ebola primary prevention: Difference between revisions

Vaccines have been produced for both Ebola <ref name="Jones2005">{{cite journal |last=Jones |first=Steven |authorlink= |coauthors=''et al.'' |year=2005 |month= |title=Live attenuated recombinant vaccine protects nonhuman primates against Ebola and Marburg viruses |journal=[[Nature Medicine]] |volume=11 |issue=7 |pages=786-790 |doi=10.1038/nm1258 |url= |accessdate= |quote= }}</ref> and Marburg<ref name="Hevey1998">{{cite journal |last=Hevey |first=M |authorlink= |coauthors=''et al.'' |year=1998 |month= |title=Marburg Virus Vaccines Based upon Alphavirus Replicons Protect Guinea Pigs and Nonhuman Primates |journal=Virology |volume=251 |issue=1 |pages=28-37 |doi=10.1006/viro.1998.9367 |url= |accessdate= |quote= }}</ref> that were 99% effective in protecting a group of monkeys from the disease. These vaccines are based on either a [[recombinant]] [[Vesicular stomatitis virus]] or a recombinant [[Adenoviridae|Adenovirus]]<ref name="Sullivan2003">{{cite journal |last=Sullivan |first=Nancy |authorlink= |coauthors=''et al.'' |year=2003 |month= |title=Accelerated vaccination for Ebola virus haemorrhagic fever in non-human primates |journal=[[Nature (journal)|Nature]] |volume=424 |issue=6949 |pages=681-684 |doi=10.1038/nature01876 |url= |accessdate= |quote= }}</ref> carrying the Ebola spikeprotein on its surface. Early human vaccine efforts, like the one at [[NIAID]] in 2003, have so far not reported any successes. The biggest problem with the vaccine is that unless the patient is given it near the onset of the virus (1-4 days after the symptoms begin) then there will be too much damage to the human body to repair, ie: ruptured [[arteries]] and [[capillaries]], [[vomiting]], and other symptoms which may still cause enough harm to kill or seriously traumatize the patient.