TKM-Ebola: Difference between revisions
No edit summary |
mNo edit summary |
||
Line 1: | Line 1: | ||
[[File:Ebola virus virion.jpg|thumb|Ebola virus]] |
[[File:Ebola virus virion.jpg|thumb|Ebola virus]] |
||
'''TKM-Ebola''' is an experimental [[antiviral drug]] for [[Ebola disease]] being developed by [ |
'''TKM-Ebola''' is an experimental [[antiviral drug]] for [[Ebola disease]] being developed by [[Arbutus Biopharma]] (Former name: Tekmira Pharmaceuticals Corp.) in Vancouver, Canada.<ref name=Kroll/><ref>[http://www.tekmira.com/ Tekmira Official Website]</ref> It was formerly known as Ebola-SNALP.<ref name=BCMIQ>{{cite web|title=TKM-Ebola|url=http://www.biocentury.com/products/tkm-ebola|website=BioCentury|publisher=BioCentury Publications Inc.|accessdate=1 August 2015}}</ref> |
||
[[File:Ebola Pathenogensis path.svg|thumb|Ebola Pathenogensis path]] |
[[File:Ebola Pathenogensis path.svg|thumb|Ebola Pathenogensis path]] |
||
TKM-Ebola is a RNAi based therapy for Ebola infection, a highly infectious and fatal disease. It is a combination of [[small interfering RNA]]s targeting three of the seven proteins in [[Ebola virus]]: Zaire Ebola L polymerase, Zaire Ebola membrane-associated protein (VP24), and Zaire Ebola polymerase complex protein (VP35).<ref name="Kroll">David Kroll for Forbes. August 7, 2014 [http://www.forbes.com/sites/davidkroll/2014/08/07/fda-moves-on-tekmiras-ebola-drug-while-sareptas-sits-unused/ FDA Moves On Tekmira's Ebola Drug While Sarepta's Sits Unused]</ref><ref name="BCMIQ" /> By down-regulate these three protein, TKM-Ebola inhibit virus replication that eliminate the infection. The drug was effective in rhesus monkeys infected with Ebola.<ref>{{cite journal|last1=Thi|first1=Emily P.|last2=Mire|first2=Chad E.|last3=Lee|first3=Amy C. H.|last4=Geisbert|first4=Joan B.|last5=Zhou|first5=Joy Z.|last6=Agans|first6=Krystle N.|last7=Snead|first7=Nicholas M.|last8=Deer|first8=Daniel J.|last9=Barnard|first9=Trisha R.|last10=Fenton|first10=Karla A.|last11=MacLachlan|first11=Ian|last12=Geisbert|first12=Thomas W.|title=Lipid nanoparticle siRNA treatment of Ebola-virus-Makona-infected nonhuman primates|journal=Nature|date=22 April 2015|volume=521|issue=7552|pages=362–365|doi=10.1038/nature14442}}</ref> After the Ebola outbreak in West Africa in 2014, the new variant responsible for was isolated from several Ebola virus family and the specific genomic sequence was determined. The company re-designed TKM-Ebola and termed as "TKM-Ebola-Guinea".<ref>{{Cite web|title = Tekmira Provides Periodic Update on TKM-Ebola Program (NASDAQ:ABUS)|url = http://investor.arbutusbio.com/releasedetail.cfm?ReleaseID=877397|website = investor.arbutusbio.com|accessdate = 2015-11-30}}</ref> |
TKM-Ebola is a RNAi based therapy for Ebola infection, a highly infectious and fatal disease. It is a combination of [[small interfering RNA]]s targeting three of the seven proteins in [[Ebola virus]]: Zaire Ebola L polymerase, Zaire Ebola membrane-associated protein (VP24), and Zaire Ebola polymerase complex protein (VP35).<ref name="Kroll">David Kroll for Forbes. August 7, 2014 [http://www.forbes.com/sites/davidkroll/2014/08/07/fda-moves-on-tekmiras-ebola-drug-while-sareptas-sits-unused/ FDA Moves On Tekmira's Ebola Drug While Sarepta's Sits Unused]</ref><ref name="BCMIQ" /> By down-regulate these three protein, TKM-Ebola inhibit virus replication that eliminate the infection. The drug was effective in rhesus monkeys infected with Ebola.<ref>{{cite journal|last1=Thi|first1=Emily P.|last2=Mire|first2=Chad E.|last3=Lee|first3=Amy C. H.|last4=Geisbert|first4=Joan B.|last5=Zhou|first5=Joy Z.|last6=Agans|first6=Krystle N.|last7=Snead|first7=Nicholas M.|last8=Deer|first8=Daniel J.|last9=Barnard|first9=Trisha R.|last10=Fenton|first10=Karla A.|last11=MacLachlan|first11=Ian|last12=Geisbert|first12=Thomas W.|title=Lipid nanoparticle siRNA treatment of Ebola-virus-Makona-infected nonhuman primates|journal=Nature|date=22 April 2015|volume=521|issue=7552|pages=362–365|doi=10.1038/nature14442}}</ref> After the Ebola outbreak in West Africa in 2014, the new variant responsible for was isolated from several Ebola virus family and the specific genomic sequence was determined. The company re-designed TKM-Ebola and termed as "TKM-Ebola-Guinea".<ref>{{Cite web|title = Tekmira Provides Periodic Update on TKM-Ebola Program (NASDAQ:ABUS)|url = http://investor.arbutusbio.com/releasedetail.cfm?ReleaseID=877397|website = investor.arbutusbio.com|accessdate = 2015-11-30}}</ref> |
Revision as of 17:27, 25 December 2015
TKM-Ebola is an experimental antiviral drug for Ebola disease being developed by Arbutus Biopharma (Former name: Tekmira Pharmaceuticals Corp.) in Vancouver, Canada.[1][2] It was formerly known as Ebola-SNALP.[3]
TKM-Ebola is a RNAi based therapy for Ebola infection, a highly infectious and fatal disease. It is a combination of small interfering RNAs targeting three of the seven proteins in Ebola virus: Zaire Ebola L polymerase, Zaire Ebola membrane-associated protein (VP24), and Zaire Ebola polymerase complex protein (VP35).[1][3] By down-regulate these three protein, TKM-Ebola inhibit virus replication that eliminate the infection. The drug was effective in rhesus monkeys infected with Ebola.[4] After the Ebola outbreak in West Africa in 2014, the new variant responsible for was isolated from several Ebola virus family and the specific genomic sequence was determined. The company re-designed TKM-Ebola and termed as "TKM-Ebola-Guinea".[5]
In January 2014, Tekmira started a Phase I clinical trial of TKM-Ebola to assess its safety in healthy people with a dose of 0.24 mg/kg/day for seven day treatment. The FDA put the trial on clinical hold in July 2014 to assess results, after some subjects had flu-like responses.[6] In August, the FDA changed the status to "partial hold", allowing the drug to be used under Expanded access in people infected with Ebola but with the Phase I trial still suspended.[1] In April 2015 the FDA allowed the study to resume at a lower dose.[7]
A Phase II trial started on 11 March 2015 in Sierra Leone, West Africa and stopped enrolling new subjects on 19 June 2015 after it appeared not to work; statistical analysis was ongoing at the time.[8][9]
TKM-Ebola is under a $140 million contract with the U.S. Department of Defense. Phase II trial is funded by Welcome Trust's £3.2 million Ebola therapeutics platform.
See also
References
- ^ a b c David Kroll for Forbes. August 7, 2014 FDA Moves On Tekmira's Ebola Drug While Sarepta's Sits Unused
- ^ Tekmira Official Website
- ^ a b "TKM-Ebola". BioCentury. BioCentury Publications Inc. Retrieved 1 August 2015.
- ^ Thi, Emily P.; Mire, Chad E.; Lee, Amy C. H.; Geisbert, Joan B.; Zhou, Joy Z.; Agans, Krystle N.; Snead, Nicholas M.; Deer, Daniel J.; Barnard, Trisha R.; Fenton, Karla A.; MacLachlan, Ian; Geisbert, Thomas W. (22 April 2015). "Lipid nanoparticle siRNA treatment of Ebola-virus-Makona-infected nonhuman primates". Nature. 521 (7552): 362–365. doi:10.1038/nature14442.
- ^ "Tekmira Provides Periodic Update on TKM-Ebola Program (NASDAQ:ABUS)". investor.arbutusbio.com. Retrieved 2015-11-30.
- ^ Cynthia Koons, Caroline Chen and Robert Langreth for Bloomberg News. Aug 8, 2014 Ebola Drug by Tekmira May Be Used on Infected Patients
- ^ "FDA modifies partial clinical hold on Tekmira Ebola study". Reuters. Retrieved 1 August 2015.
- ^ Kupferschmidt, Kai (11 March 2015). "New Ebola drug trial starts in Sierra Leone". Science Magazine. AAAS. Retrieved 1 August 2015.
- ^ Vogel, Gretchen; Kupferschmidt, Kai (19 June 2015). "In setback for potential Ebola drug, company halts trial". news.sciencemag.org. Retrieved 24 June 2015.