Vaccines or candidate vaccines used to prevent EBOLA HEMORRHAGIC FEVER.
A highly fatal, acute hemorrhagic fever, clinically very similar to MARBURG VIRUS DISEASE, caused by EBOLAVIRUS, first occurring in the Sudan and adjacent northwestern (what was then) Zaire.
A genus in the family FILOVIRIDAE consisting of several distinct species of Ebolavirus, each containing separate strains. These viruses cause outbreaks of a contagious, hemorrhagic disease (HEMORRHAGIC FEVER, EBOLA) in humans, usually with high mortality.
Suspensions of killed or attenuated microorganisms (bacteria, viruses, fungi, protozoa), antigenic proteins, synthetic constructs, or other bio-molecular derivatives, administered for the prevention, amelioration, or treatment of infectious and other diseases.
Vaccines in which the infectious microbial nucleic acid components have been destroyed by chemical or physical treatment (e.g., formalin, beta-propiolactone, gamma radiation) without affecting the antigenicity or immunogenicity of the viral coat or bacterial outer membrane proteins.
Suspensions of attenuated or killed viruses administered for the prevention or treatment of infectious viral disease.
Recombinant DNA vectors encoding antigens administered for the prevention or treatment of disease. The host cells take up the DNA, express the antigen, and present it to the immune system in a manner similar to that which would occur during natural infection. This induces humoral and cellular immune responses against the encoded antigens. The vector is called naked DNA because there is no need for complex formulations or delivery agents; the plasmid is injected in saline or other buffers.
Small synthetic peptides that mimic surface antigens of pathogens and are immunogenic, or vaccines manufactured with the aid of recombinant DNA techniques. The latter vaccines may also be whole viruses whose nucleic acids have been modified.
Two or more vaccines in a single dosage form.
Suspensions of attenuated or killed bacteria administered for the prevention or treatment of infectious bacterial disease.
Vaccines or candidate vaccines containing inactivated HIV or some of its component antigens and designed to prevent or treat AIDS. Some vaccines containing antigens are recombinantly produced.

Chimpanzee adenovirus vaccine protects against Zaire Ebola virus. (1/60)

This study evaluated the use of a chimpanzee-based adenovirus vaccine in mouse and Guinea pigs models of Zaire Ebola virus (ZEBOV) infection. Vaccine vector expressing the envelope glycoprotein of ZEBOV was created from the molecular clone of chimpanzee adenovirus pan7 (AdC7). AdC7 vaccine stimulated robust T and B cell responses to ZEBOV in naive mice inducing complete protection to an otherwise lethal challenge of ZEBOV. Complete protection to Zaire Ebola virus was also observed in Guinea pigs vaccinated with a relatively low dose of AdC7 (5 x 10(9)/kg). Pre-existing immunity to AdHu5 was generated in mice following pre-exposure to AdHu5 or administration of pooled human immune globulin. Pre-existing immunity to human adenoviruses severely compromised the efficacy of the human AdHu5 vaccine but not the chimpanzee AdC7 vaccine. These results validate further development of Chimpanzee-based vaccine and highlight the impact of pre-existing immunity to the vaccine carrier.  (+info)

A single intranasal inoculation with a paramyxovirus-vectored vaccine protects guinea pigs against a lethal-dose Ebola virus challenge. (2/60)

To determine whether intranasal inoculation with a paramyxovirus-vectored vaccine can induce protective immunity against Ebola virus (EV), recombinant human parainfluenza virus type 3 (HPIV3) was modified to express either the EV structural glycoprotein (GP) by itself (HPIV3/EboGP) or together with the EV nucleoprotein (NP) (HPIV3/EboGP-NP). Expression of EV GP by these recombinant viruses resulted in its efficient incorporation into virus particles and increased cytopathic effect in Vero cells. HPIV3/EboGP was 100-fold more efficiently neutralized by antibodies to EV than by antibodies to HPIV3. Guinea pigs infected with a single intranasal inoculation of 10(5.3) PFU of HPIV3/EboGP or HPIV3/EboGP-NP showed no apparent signs of disease yet developed a strong humoral response specific to the EV proteins. When these animals were challenged with an intraperitoneal injection of 10(3) PFU of EV, there were no outward signs of disease, no viremia or detectable EV antigen in the blood, and no evidence of infection in the spleen, liver, and lungs. In contrast, all of the control animals died or developed severe EV disease following challenge. The highly effective immunity achieved with a single vaccine dose suggests that intranasal immunization with live vectored vaccines based on recombinant respiratory viruses may be an advantageous approach to inducing protective responses against severe systemic infections, such as those caused by hemorrhagic fever agents.  (+info)

Development of a cAdVax-based bivalent ebola virus vaccine that induces immune responses against both the Sudan and Zaire species of Ebola virus. (3/60)

Ebola virus (EBOV) causes a severe hemorrhagic fever for which there are currently no vaccines or effective treatments. While lethal human outbreaks have so far been restricted to sub-Saharan Africa, the potential exploitation of EBOV as a biological weapon cannot be ignored. Two species of EBOV, Sudan ebolavirus (SEBOV) and Zaire ebolavirus (ZEBOV), have been responsible for all of the deadly human outbreaks resulting from this virus. Therefore, it is important to develop a vaccine that can prevent infection by both lethal species. Here, we describe the bivalent cAdVaxE(GPs/z) vaccine, which includes the SEBOV glycoprotein (GP) and ZEBOV GP genes together in a single complex adenovirus-based vaccine (cAdVax) vector. Vaccination of mice with the bivalent cAdVaxE(GPs/z) vaccine led to efficient induction of EBOV-specific antibody and cell-mediated immune responses to both species of EBOV. In addition, the cAdVax technology demonstrated induction of a 100% protective immune response in mice, as all vaccinated C57BL/6 and BALB/c mice survived challenge with a lethal dose of ZEBOV (30,000 times the 50% lethal dose). This study demonstrates the potential efficacy of a bivalent EBOV vaccine based on a cAdVax vaccine vector design.  (+info)

Immune protection of nonhuman primates against Ebola virus with single low-dose adenovirus vectors encoding modified GPs. (4/60)

BACKGROUND: Ebola virus causes a hemorrhagic fever syndrome that is associated with high mortality in humans. In the absence of effective therapies for Ebola virus infection, the development of a vaccine becomes an important strategy to contain outbreaks. Immunization with DNA and/or replication-defective adenoviral vectors (rAd) encoding the Ebola glycoprotein (GP) and nucleoprotein (NP) has been previously shown to confer specific protective immunity in nonhuman primates. GP can exert cytopathic effects on transfected cells in vitro, and multiple GP forms have been identified in nature, raising the question of which would be optimal for a human vaccine. METHODS AND FINDINGS: To address this question, we have explored the efficacy of mutant GPs from multiple Ebola virus strains with reduced in vitro cytopathicity and analyzed their protective effects in the primate challenge model, with or without NP. Deletion of the GP transmembrane domain eliminated in vitro cytopathicity but reduced its protective efficacy by at least one order of magnitude. In contrast, a point mutation was identified that abolished this cytopathicity but retained immunogenicity and conferred immune protection in the absence of NP. The minimal effective rAd dose was established at 10(10) particles, two logs lower than that used previously. CONCLUSIONS: Expression of specific GPs alone vectored by rAd are sufficient to confer protection against lethal challenge in a relevant nonhuman primate model. Elimination of NP from the vaccine and dose reductions to 10(10) rAd particles do not diminish protection and simplify the vaccine, providing the basis for selection of a human vaccine candidate.  (+info)

Reverse genetic generation of recombinant Zaire Ebola viruses containing disrupted IRF-3 inhibitory domains results in attenuated virus growth in vitro and higher levels of IRF-3 activation without inhibiting viral transcription or replication. (5/60)

The VP35 protein of Zaire Ebola virus is an essential component of the viral RNA polymerase complex and also functions to antagonize the cellular type I interferon (IFN) response by blocking activation of the transcription factor IRF-3. We previously mapped the IRF-3 inhibitory domain within the C terminus of VP35. In the present study, we show that mutations that disrupt the IRF-3 inhibitory function of VP35 do not disrupt viral transcription/replication, suggesting that the two functions of VP35 are separable. Second, using reverse genetics, we successfully recovered recombinant Ebola viruses containing mutations within the IRF-3 inhibitory domain. Importantly, we show that the recombinant viruses were attenuated for growth in cell culture and that they activated IRF-3 and IRF-3-inducible gene expression at levels higher than that for Ebola virus containing wild-type VP35. In the context of Ebola virus pathogenesis, VP35 may function to limit early IFN-beta production and other antiviral signals generated from cells at the primary site of infection, thereby slowing down the host's ability to curb virus replication and induce adaptive immunity.  (+info)

Complex adenovirus-vectored vaccine protects guinea pigs from three strains of Marburg virus challenges. (6/60)

The Marburg virus (MARV), an African filovirus closely related to the Ebola virus, causes a deadly hemorrhagic fever in humans, with up to 90% mortality. Currently, treatment of disease is only supportive, and no vaccines are available to prevent spread of MARV infections. In order to address this need, we have developed and characterized a novel recombinant vaccine that utilizes a single complex adenovirus-vectored vaccine (cAdVax) to overexpress a MARV glycoprotein (GP) fusion protein derived from the Musoke and Ci67 strains of MARV. Vaccination with the cAdVaxM(fus) vaccine led to efficient production of MARV-specific antibodies in both mice and guinea pigs. Significantly, guinea pigs vaccinated with at least 5 x 10(7) pfu of cAdVaxM(fus) vaccine were 100% protected against lethal challenges by the Musoke, Ci67 and Ravn strains of MARV, making it a vaccine with trivalent protective efficacy. Therefore, the cAdVaxM(fus) vaccine serves as a promising vaccine candidate to prevent and contain multi-strain infections by MARV.  (+info)

Generation of an adenoviral vaccine vector based on simian adenovirus 21. (7/60)

Adenoviral vectors can be used to generate potent humoral and cellular immune responses to transgene products. Use of adenoviral vectors based on non-human isolates may allow for their utilization in populations harbouring neutralizing antibodies to common human serotypes. A vector chimera was constructed using simian adenovirus 22 (a serotype belonging to the species Human adenovirus E) and simian adenovirus 21 (a serotype belonging to the species Human adenovirus B) expressing the Ebola (Zaire) virus glycoprotein (Ad C5/C1-ZGP). This chimeric adenovirus vector was used as a model to test its efficacy as a genetic vaccine and comparisons were made to a vector based on the commonly used human adenovirus C serotype 5 (Adhu5-ZGP). Ebola glycoprotein-specific T- and B-cell responses were measured in B10BR mice vaccinated with either Adhu5-ZGP or Ad C5/C1-ZGP vectors. Both vectors resulted in Ebola glycoprotein-specific gamma interferon-expressing T cells, although the Ad C5/C1-ZGP vector appeared to induce lower frequencies with kinetics slower than those elicited by the Adhu5-ZGP vector. The total immunoglobulin G response to Ebola glycoprotein was similar in sera from mice vaccinated with either vector. Two rhesus macaques vaccinated with the Ad C5/C1-ZGP vector were found to mount T-cell and antibody responses to the Ebola glycoprotein. It was found that a single administration of the chimeric Ad C5/C1-ZGP vector protected mice against a lethal challenge with a mouse-adapted strain of the Ebola (Zaire) virus.  (+info)

A DNA vaccine for Ebola virus is safe and immunogenic in a phase I clinical trial. (8/60)

Ebola viruses represent a class of filoviruses that causes severe hemorrhagic fever with high mortality. Recognized first in 1976 in the Democratic Republic of Congo, outbreaks continue to occur in equatorial Africa. A safe and effective Ebola virus vaccine is needed because of its continued emergence and its potential for use for biodefense. We report the safety and immunogenicity of an Ebola virus vaccine in its first phase I human study. A three-plasmid DNA vaccine encoding the envelope glycoproteins (GP) from the Zaire and Sudan/Gulu species as well as the nucleoprotein was evaluated in a randomized, placebo-controlled, double-blinded, dose escalation study. Healthy adults, ages 18 to 44 years, were randomized to receive three injections of vaccine at 2 mg (n = 5), 4 mg (n = 8), or 8 mg (n = 8) or placebo (n = 6). Immunogenicity was assessed by enzyme-linked immunosorbent assay (ELISA), immunoprecipitation-Western blotting, intracellular cytokine staining (ICS), and enzyme-linked immunospot assay. The vaccine was well-tolerated, with no significant adverse events or coagulation abnormalities. Specific antibody responses to at least one of the three antigens encoded by the vaccine as assessed by ELISA and CD4(+) T-cell GP-specific responses as assessed by ICS were detected in 20/20 vaccinees. CD8(+) T-cell GP-specific responses were detected by ICS assay in 6/20 vaccinees. This Ebola virus DNA vaccine was safe and immunogenic in humans. Further assessment of the DNA platform alone and in combination with replication-defective adenoviral vector vaccines, in concert with challenge and immune data from nonhuman primates, will facilitate evaluation and potential licensure of an Ebola virus vaccine under the Animal Rule.  (+info)

Ebola vaccines are medical products designed to confer immunity against the Ebola virus, a deadly pathogen that causes hemorrhagic fever. Several Ebola vaccine candidates have been developed and tested in clinical trials, with some showing promising results. The most advanced Ebola vaccine is rVSV-ZEBOV, which has been shown to be highly effective in preventing the disease in clinical trials. It uses a weakened version of the vesicular stomatitis virus (VSV) to deliver a protein from the Ebola virus surface, triggering an immune response that protects against infection. Other Ebola vaccine candidates use different approaches, such as delivering Ebola virus genes using a harmless adenovirus vector or using inactivated whole Ebola viruses. These vaccines are still in development and have not yet been approved for widespread use.

Ebola Hemorrhagic Fever (EHF) is a severe, often fatal illness in humans. It is one of the five identified subtypes of the Ebolavirus. The virus is transmitted to people from wild animals and spreads in the human population through human-to-human transmission.

The early symptoms include sudden onset of fever, fatigue, muscle pain, headache and sore throat. This is followed by vomiting, diarrhea, rash, symptoms of impaired kidney and liver function, and in some cases, both internal and external bleeding.

Laboratory findings include low white blood cell and platelet counts and elevated liver enzymes.

The virus is introduced into the human population through close contact with the blood, secretions, organs or other bodily fluids of infected animals such as fruit bats, porcupines and non-human primates. Then it spreads in communities through human-to-human transmission via direct contact (through broken skin or mucous membranes) with the blood, secretions, organs or other bodily fluids of infected people, and with surfaces and materials contaminated with these fluids.

Healthcare workers have frequently been infected while treating patients with suspected or confirmed EVD due to a lack of adequate infection prevention and control measures.

There are currently no approved specific antiviral drugs or vaccines for Ebola. Several promising treatments and vaccine candidates are being evaluated.

Ebolavirus is a genus of viruses in the family Filoviridae, order Mononegavirales. It is named after the Ebola River in the Democratic Republic of Congo (formerly Zaire), where the virus was first identified in 1976. There are six species of Ebolavirus, four of which are known to cause disease in humans: Zaire ebolavirus, Sudan ebolavirus, Bundibugyo ebolavirus, and Tai Forest ebolavirus (formerly Cote d'Ivoire ebolavirus). The fifth species, Reston ebolavirus, is known to cause disease in non-human primates and pigs, but not in humans. The sixth and most recently identified species, Bombali ebolavirus, has not been associated with any human or animal diseases.

Ebolaviruses are enveloped, negative-sense, single-stranded RNA viruses that cause a severe and often fatal hemorrhagic fever in humans and non-human primates. The virus is transmitted to people from wild animals and spreads in the human population through human-to-human transmission. Fruit bats of the Pteropodidae family are considered to be the natural host of Ebolavirus.

The symptoms of Ebolavirus disease (EVD) typically include fever, severe headache, muscle pain, weakness, fatigue, and sore throat, followed by vomiting, diarrhea, rash, impaired kidney and liver function, and in some cases, both internal and external bleeding. The case fatality rate of EVD is variable but has been historically high, ranging from 25% to 90% in past outbreaks depending on the species and the quality of medical care. There are no licensed specific treatments or vaccines available for EVD, although several promising candidates are currently under development.

A vaccine is a biological preparation that provides active acquired immunity to a particular infectious disease. It typically contains an agent that resembles the disease-causing microorganism and is often made from weakened or killed forms of the microbe, its toxins, or one of its surface proteins. The agent stimulates the body's immune system to recognize the agent as a threat, destroy it, and "remember" it, so that the immune system can more easily recognize and destroy any of these microorganisms that it encounters in the future.

Vaccines can be prophylactic (to prevent or ameliorate the effects of a future infection by a natural or "wild" pathogen), or therapeutic (to fight disease that is already present). The administration of vaccines is called vaccination. Vaccinations are generally administered through needle injections, but can also be administered by mouth or sprayed into the nose.

The term "vaccine" comes from Edward Jenner's 1796 use of cowpox to create immunity to smallpox. The first successful vaccine was developed in 1796 by Edward Jenner, who showed that milkmaids who had contracted cowpox did not get smallpox. He reasoned that exposure to cowpox protected against smallpox and tested his theory by injecting a boy with pus from a cowpox sore and then exposing him to smallpox, which the boy did not contract. The word "vaccine" is derived from Variolae vaccinae (smallpox of the cow), the term devised by Jenner to denote cowpox. He used it in 1798 during a conversation with a fellow physician and later in the title of his 1801 Inquiry.

Inactivated vaccines, also known as killed or non-live vaccines, are created by using a version of the virus or bacteria that has been grown in a laboratory and then killed or inactivated with chemicals, heat, or radiation. This process renders the organism unable to cause disease, but still capable of stimulating an immune response when introduced into the body.

Inactivated vaccines are generally considered safer than live attenuated vaccines since they cannot revert back to a virulent form and cause illness. However, they may require multiple doses or booster shots to maintain immunity because the immune response generated by inactivated vaccines is not as robust as that produced by live vaccines. Examples of inactivated vaccines include those for hepatitis A, rabies, and influenza (inactivated flu vaccine).

A viral vaccine is a biological preparation that introduces your body to a specific virus in a way that helps your immune system build up protection against the virus without causing the illness. Viral vaccines can be made from weakened or inactivated forms of the virus, or parts of the virus such as proteins or sugars. Once introduced to the body, the immune system recognizes the virus as foreign and produces an immune response, including the production of antibodies. These antibodies remain in the body and provide immunity against future infection with that specific virus.

Viral vaccines are important tools for preventing infectious diseases caused by viruses, such as influenza, measles, mumps, rubella, polio, hepatitis A and B, rabies, rotavirus, chickenpox, shingles, and some types of cancer. Vaccination programs have led to the control or elimination of many infectious diseases that were once common.

It's important to note that viral vaccines are not effective against bacterial infections, and separate vaccines must be developed for each type of virus. Additionally, because viruses can mutate over time, it is necessary to update some viral vaccines periodically to ensure continued protection.

I could not find a specific medical definition for "Vaccines, DNA." However, I can provide you with some information about DNA vaccines.

DNA vaccines are a type of vaccine that uses genetically engineered DNA to stimulate an immune response in the body. They work by introducing a small piece of DNA into the body that contains the genetic code for a specific antigen (a substance that triggers an immune response). The cells of the body then use this DNA to produce the antigen, which prompts the immune system to recognize and attack it.

DNA vaccines have several advantages over traditional vaccines. They are relatively easy to produce, can be stored at room temperature, and can be designed to protect against a wide range of diseases. Additionally, because they use DNA to stimulate an immune response, DNA vaccines do not require the growth and culture of viruses or bacteria, which can make them safer than traditional vaccines.

DNA vaccines are still in the experimental stages, and more research is needed to determine their safety and effectiveness. However, they have shown promise in animal studies and are being investigated as a potential tool for preventing a variety of infectious diseases, including influenza, HIV, and cancer.

Synthetic vaccines are artificially produced, designed to stimulate an immune response and provide protection against specific diseases. Unlike traditional vaccines that are derived from weakened or killed pathogens, synthetic vaccines are created using synthetic components, such as synthesized viral proteins, DNA, or RNA. These components mimic the disease-causing agent and trigger an immune response without causing the actual disease. The use of synthetic vaccines offers advantages in terms of safety, consistency, and scalability in production, making them valuable tools for preventing infectious diseases.

Combined vaccines are defined in medical terms as vaccines that contain two or more antigens from different diseases, which are given to provide protection against multiple diseases at the same time. This approach reduces the number of injections required and simplifies the immunization schedule, especially during early childhood. Examples of combined vaccines include:

1. DTaP-Hib-IPV (e.g., Pentacel): A vaccine that combines diphtheria, tetanus, pertussis (whooping cough), Haemophilus influenzae type b (Hib) disease, and poliovirus components in one injection to protect against these five diseases.
2. MMRV (e.g., ProQuad): A vaccine that combines measles, mumps, rubella, and varicella (chickenpox) antigens in a single injection to provide immunity against all four diseases.
3. HepA-HepB (e.g., Twinrix): A vaccine that combines hepatitis A and hepatitis B antigens in one injection, providing protection against both types of hepatitis.
4. MenACWY-TT (e.g., MenQuadfi): A vaccine that combines four serogroups of meningococcal bacteria (A, C, W, Y) with tetanus toxoid as a carrier protein in one injection for the prevention of invasive meningococcal disease caused by these serogroups.
5. PCV13-PPSV23 (e.g., Vaxneuvance): A vaccine that combines 13 pneumococcal serotypes with PPSV23, providing protection against a broader range of pneumococcal diseases in adults aged 18 years and older.

Combined vaccines have been thoroughly tested for safety and efficacy to ensure they provide a strong immune response and an acceptable safety profile. They are essential tools in preventing various infectious diseases and improving overall public health.

Bacterial vaccines are types of vaccines that are created using bacteria or parts of bacteria as the immunogen, which is the substance that triggers an immune response in the body. The purpose of a bacterial vaccine is to stimulate the immune system to develop protection against specific bacterial infections.

There are several types of bacterial vaccines, including:

1. Inactivated or killed whole-cell vaccines: These vaccines contain entire bacteria that have been killed or inactivated through various methods, such as heat or chemicals. The bacteria can no longer cause disease, but they still retain the ability to stimulate an immune response.
2. Subunit, protein, or polysaccharide vaccines: These vaccines use specific components of the bacterium, such as proteins or polysaccharides, that are known to trigger an immune response. By using only these components, the vaccine can avoid using the entire bacterium, which may reduce the risk of adverse reactions.
3. Live attenuated vaccines: These vaccines contain live bacteria that have been weakened or attenuated so that they cannot cause disease but still retain the ability to stimulate an immune response. This type of vaccine can provide long-lasting immunity, but it may not be suitable for people with weakened immune systems.

Bacterial vaccines are essential tools in preventing and controlling bacterial infections, reducing the burden of diseases such as tuberculosis, pneumococcal disease, meningococcal disease, and Haemophilus influenzae type b (Hib) disease. They work by exposing the immune system to a harmless form of the bacteria or its components, which triggers the production of antibodies and memory cells that can recognize and fight off future infections with that same bacterium.

It's important to note that while vaccines are generally safe and effective, they may cause mild side effects such as pain, redness, or swelling at the injection site, fever, or fatigue. Serious side effects are rare but can occur, so it's essential to consult with a healthcare provider before receiving any vaccine.

An AIDS vaccine is a type of preventive vaccine that aims to stimulate the immune system to produce an effective response against the human immunodeficiency virus (HIV), which causes acquired immunodeficiency syndrome (AIDS). The goal of an AIDS vaccine is to induce the production of immune cells and proteins that can recognize and eliminate HIV-infected cells, thereby preventing the establishment of a persistent infection.

Despite decades of research, there is still no licensed AIDS vaccine available. This is due in part to the unique challenges posed by HIV, which has a high mutation rate and can rapidly evolve to evade the immune system's defenses. However, several promising vaccine candidates are currently being tested in clinical trials around the world, and researchers continue to explore new approaches and strategies for developing an effective AIDS vaccine.

Ebola vaccines are vaccines either approved or in development to prevent Ebola. As of 2022, there are only vaccines against the ... "Ebola Vaccine Information Statement". U.S. Centers for Disease Control and Prevention (CDC). June 2022. Ebola Vaccines at the U ... Scholia has a topic profile for Ebola vaccine. "Ebola Vaccines". Drug Information Portal. U.S. National Library of Medicine. " ... The Wellcome Trust-CIDRAP Ebola Vaccine Team B (January 2017). Completing the development of Ebola vaccines: current status, ...
An Ebola vaccine was approved by the US FDA in December 2019. While there is no approved treatment for Ebola as of 2019[update ... "Ebola virus disease: Vaccines". www.who.int. Retrieved 29 March 2023. "Ebola Hemorrhagic Fever Prevention". Centers for Disease ... Ebola, also known as Ebola virus disease (EVD) and Ebola hemorrhagic fever (EHF), is a viral hemorrhagic fever in humans and ... "Ebola virus disease Information for Clinicians in U.S. Healthcare Settings , For Clinicians , Ebola (Ebola Virus Disease) , ...
... expressing Ebola envelope glycoprotein. The vaccine is targeted against the Makona variant of Ebola that was circulating in ... and Ad5-vectored Ebola vaccine. There is also a version called GamEvac which is a homologous Ad5-vectored vaccine. GamEvac- ... "Update with the development of Ebola vaccines and implications of emerging evidence to inform future policy recommendations" ( ... and Ad5-vectored Ebola vaccine: An open phase I/II trial in healthy adults in Russia". Hum Vaccin Immunother. 13 (3): 613-620. ...
The FDA subsequently approved the device for testing in up to 20 infected Ebola cases in the United States. Ebola vaccine Ebola ... Roberts D. "Ebola CDC director warns Ebola like 'forest fire' as Congress readies for hearing - Ebola crisis live updates". The ... Briggs H (7 August 2014). "Ebola: Experimental drugs and vaccines". BBC News Online. Retrieved 1 August 2014. Park A (19 ... 2018). "Advances in Designing and Developing Vaccines, Drugs, and Therapies to Counter Ebola Virus". Frontiers in Immunology. 9 ...
... also known as Ebola Zaire vaccine live and sold under the brand name Ervebo, is an Ebola vaccine for adults that prevents Ebola ... Study confirms efficacy of NewLink Genetics ebola vaccine "Scientists hail '100% effective' Ebola vaccine". National Health ... August 2015). "EBOLA VACCINE. VSV-EBOV rapidly protects macaques against infection with the 2014/15 Ebola virus outbreak strain ... Scholia has a topic profile for RVSV-ZEBOV vaccine. Ebola Vaccines at the U.S. National Library of Medicine Medical Subject ...
... typhoid vaccines and, more recently, new vaccines against Ebola. OVG is a research group within the Department of Paediatrics ... Vaccine Knowledge homepage. Retrieved 25 June 2015 NHS Choices page on the MenC vaccine with external link to Vaccine Knowledge ... 2014-15: a phase 1 study into a new vaccine against Ebola. In January 2015 this trial was commended in the House of Commons by ... "Oxford University doctors and scientists start trials for new Ebola vaccine". ITV News. 6 January 2015. Retrieved 25 June 2015 ...
In December 2019, the first Ebola vaccine was approved. rVSV-ZEBOV, otherwise known as Ervebo, is a vaccine for adults that ... Ebola virus epidemic in Guinea Ebola virus epidemic in Liberia Ebola virus epidemic in Nigeria Ebola virus epidemic in Sierra ... "Americans 'can't give in to hysteria or fear' over Ebola: Obama". Reuters. October 18, 2014. "WHO: Millions of Ebola Vaccine ... Ebola: How it spreads What gear to wear for protection from Ebola infection Ebola Hemorrhagic Fever - CDC.gov Portals: United ...
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As of April 2021[update], six viral vector vaccines, four COVID-19 vaccines and two Ebola vaccines, have been authorized for ... The rVSV-ZEBOV vaccine, known as Ervebo, was approved as a prophylactic Ebola vaccine for medical use by the FDA in 2019. The ... Two Ebola vaccines that used viral vector technology were used to combat Ebola outbreaks in West Africa (2013-2016), and in the ... The Janssen vaccine uses serotype 26. Convidecia uses serotype 5. Zabdeno, the first dose of the Zabdeno/Mvabea Ebola vaccine, ...
Other current Ebola research is focused on developing treatments or vaccines against the virus. Early investigations into ... Wilson JA, Bray M, Bakken R, Hart MK (August 2001). "Vaccine potential of Ebola virus VP24, VP30, VP35, and VP40 proteins". ... Sullivan N, Yang ZY, Nabel GJ (September 2003). "Ebola virus pathogenesis: implications for vaccines and therapies". Journal of ... there has been a considerable increase in research focused on developing a vaccine for Ebola. Shabman RS, Gulcicek EE, Stone KL ...
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Sullivan, Nancy; Yang, Zhi-Yong; Nabel, Gary (2003). "Ebola Virus Pathogenesis: Implications for Vaccines and Therapies". ... This research may lead to new ways to combat deadly viruses such as the Ebola virus and HIV. Research using wild-type mutations ... Research is also being done dealing with the manipulation of certain wild-type traits in viruses to develop new vaccines. ... Davidson, Nagar, Ribshtein, Shkoda, Perk, Garcia (2009). "Detection of Wild- and Vaccine-Type Avian Infectious ...
Symptoms are similar to Ebola virus disease. There are no vaccines or antiviral treatments for Marburg. An outbreak of an ... "Equatorial Guinea declares outbreak of Ebola-like Marburg virus". BNO News. Archived from the original on 20 February 2023. ...
"Nearly 700 get Ebola vaccine in Congo; more cases possible". Fox News. 1 June 2018. Retrieved 1 June 2018. "Ebola virus disease ... and was the first time that vaccination with the rVSV-ZEBOV Ebola vaccine had been attempted in the early stages of an Ebola ... vaccine - a recently developed experimental Ebola vaccine, produced by Merck - to try to suppress the outbreak. This live- ... Declaration of End of Ebola Virus Disease Outbreak". ReliefWeb. Retrieved 26 July 2018. "We finally have an Ebola vaccine. And ...
... establishing a successful pipeline of candidate vaccines against HCV, malaria, RSV and Ebola. These vaccines were tested in ... Riccardo Cortese, former head of the Genome Biology Unit, talks about the Ebola vaccine candidate developed by his start-up, ... 2016). "A Monovalent Chimpanzee Adenovirus Ebola Vaccine Boosted with MVA". The New England Journal of Medicine. 374 (17): 1635 ... 2017). "Chimpanzee Adenovirus Vector Ebola Vaccine". The New England Journal of Medicine. 376 (10): 928-938. doi:10.1056/ ...
Field trials for a Russian Ebola vaccine were carried out at the centre, and the vaccine was officially launched in August 2017 ... "Russia to fund Ebola vaccine trials , IOL News". Retrieved 8 September 2017. "Santé : l'hôpital RUSAL lance la vaccination ... During the 2014 Ebola outbreak in West Africa, UC Rusal provided logistical support to the international relief efforts. In ... "UC RUSAL builds US$10m centre in Guinea to combat Ebola , Trade and Forfaiting Review". www.tfreview.com. Archived from the ...
"Ebola/Marburg Vaccine Development" (Press release). National Institute of Allergy and Infectious Diseases. 2008-09-15. Archived ... There are currently no Food and Drug Administration-approved vaccines for the prevention of MVD. Many candidate vaccines have ... Ebola virus, Marburg virus and Venezuelan equine encephalitis virus". Vaccine. 21 (25-26): 4071-4080. doi:10.1016/S0264-410X(03 ... "Live attenuated recombinant vaccine protects nonhuman primates against Ebola and Marburg viruses". Nature Medicine. 11 (7): 786 ...
"Ebola treatment pioneered at ASU". Retrieved 28 August 2019. "Nyet News Report (12.06.11): "Ebola vaccine developed"". Ynetnews ... In 2011, he and his team at the Biodesign Institute were developing a vaccine for the Ebola virus using mice. An outcome of ... Arntzen, C (2015). "Plant-made pharmaceuticals: from 'Edible Vaccines' to Ebola therapeutics". Plant Biotechnol J. 13 (8): 1013 ... "A nonreplicating subunit vaccine protects mice against lethal Ebola virus challenge". Proceedings of the National Academy of ...
Viral vectors had previously been approved as ebola vaccines. Eckhart Buddecke: Molekulare Medizin. ecomed-Storck GmbH, 2002, ... Genetic vaccines thus include DNA vaccines, RNA vaccines and viral vector vaccines. Most vaccines other than live attenuated ... A genetic vaccine (also gene-based vaccine) is a vaccine that contains nucleic acids such as DNA or RNA that lead to protein ... Examples of genetic vaccines approved for use in humans include the RNA vaccines tozinameran and mRNA-1273, the DNA vaccine ...
"Ebola vaccine found safe in humans trials". Outlook India. Press Trust of India. 9 October 2017. Retrieved 3 November 2021. ... He also contributed to the development of vaccines for Ebola which were shown to be safe and effective in clinical trials by ... April 2016). "Phase 1 Trials of rVSV Ebola Vaccine in Africa and Europe". New England Journal of Medicine. 374 (17): 1647-1660 ... Withers, Iain (1 February 2018). "How prepared are we for the next Ebola-scale epidemic?". The Telegraph. ISSN 0307-1235. ...
22 December Ebola virus disease found to be 70-100% prevented by rVSV-ZEBOV vaccine, making it the first proven vaccine against ... 22 December 2016). "Efficacy and effectiveness of an rVSV-vectored vaccine in preventing Ebola virus disease: final results ... Berlinger, Joshua (22 December 2016). "Ebola vaccine gives 100% protection, study finds". CNN. Retrieved 27 December 2016. " ... "First new HIV vaccine efficacy study in seven years has begun". NIH. 28 November 2016. Retrieved 1 December 2016. "Testing ...
"Residents and traders to get Ebola vaccine". Rwanda Today. Retrieved 2020-06-07. "Board of Directors". rbc.gov.rw. 2019-12-18. ... The past few years, Karita has been working on the Umurinzi Ebola Vaccination Program to prevent the spread of Ebola, but the ...
Freudenthal, Emmanuel (10 June 2019). "A short history of an Ebola vaccine". ConverseAfrica.com. v t e (Articles with short ... The variant of the Ebola virus that infected N'Seka was originally named "Zaïre virus strain Mayinga" (now Ebola virus variant ... She died from Ebola virus disease during the 1976 epidemic in Zaïre. She has been incorrectly identified as the index case by ... "Ebola hemorrhagic fever in Zaire, 1976" (PDF). Bulletin of the World Health Organization. 56 (6): 271. 1978. Archived from the ...
December 22 - A study finds the VSV-EBOV vaccine against the Ebola virus between 70 and 100% effective, thus making it the ... Berlinger, Joshua (December 23, 2016). "Ebola vaccine gives 100% protection, study finds". CNN. Archived from the original on ... first proven vaccine against the disease. December 23 - The United Nations Security Council adopts Resolution 2334 condemning " ...
2. Ebola vaccine. Ebola vaccine can prevent Ebola virus disease (Zaire Ebola vaccine is a live virus vaccine that is ... the Ebola vaccine only contains a gene from the Ebola virus goril as, and chimpanzees). Outbreaks of Ebola virus disease ... Ebola vaccine contains a live virus. It is possible that been seriously injured by certain medicines or vaccines. the vaccine ... Ebola vaccine is recommended by CDC for adults 18 years are infected with the virus or who have died of Ebola and older at high ...
Ebola vaccines are vaccines either approved or in development to prevent Ebola. As of 2022, there are only vaccines against the ... "Ebola Vaccine Information Statement". U.S. Centers for Disease Control and Prevention (CDC). June 2022. Ebola Vaccines at the U ... Scholia has a topic profile for Ebola vaccine. "Ebola Vaccines". Drug Information Portal. U.S. National Library of Medicine. " ... The Wellcome Trust-CIDRAP Ebola Vaccine Team B (January 2017). Completing the development of Ebola vaccines: current status, ...
Evaluation in Nonhuman Primates of Vaccines against Ebola Virus Thomas W. Geisbert*, Peter Pushko*, Kevin Anderson*, Jonathan ... Evaluation in Nonhuman Primates of Vaccines against Ebola Virus. ... Sections of spleen from Ebola virus (EBOV)-infected animals. ...
Information you need to know about the Ebola vaccine. Vaccine Information Statements (VISs). ... Ebola vaccine. Ebola vaccine is a live virus vaccine that is administered as a single dose by injection into a muscle. The ... Because the Ebola vaccine only contains a gene from the Ebola virus instead of the whole Ebola virus, it cannot cause Ebola ... Ebola vaccine can prevent Ebola virus disease (Zaire ebolavirus).. Ebola virus disease is a rare disease that most commonly ...
... highlights the need for an Ebola vaccine stockpile, Berkley says. "It basically says we need to have a supply of vaccine ... With the Ebola outbreak in West Africa stubbornly hanging on, officials have brokered an agreement to ensure that a vaccine is ... "We are in the most tenuous situation with regard to Ebola vaccines that weve seen since we started all of this," says Michael ... Much of the devastation wrought by Ebola in West Africa might have been prevented with a vaccine. Credit: Misha Hussain/Reuters ...
Human trials of the Ebola vaccine have been temporarily shut down due to adverse side effects. What will it take to get it up ... Thomas Geisbert of the University of Texas, an Ebola vaccine researcher who has worked with most of the vaccines coming to ... Though the replication-competent VSV-based vaccine trial is having difficulty, the other leading Ebola vaccine candidate is not ... Matthias Schnell, the researcher behind the Ebola-rabies combination vaccine at the Jefferson Vaccine Center in Philadelphia. " ...
... which is about the first known Ebola outbreak, the one that gave it its name, in southern Sudan. Thats about 150 miles, as the ... well within the migratory range of an Ebola carrying fruit bat. ... Ebola: Have more knowledge, need vaccine more * facebook * ... That would be a good argument to get a damn vaccine.. But, one could argue that even though Ebola is known to have been around ... there was not much movement to get a vaccine. Then, one day, a fruit bat, carrying ebola, dropped some bat spit covered fruit ...
Canadian team prepares to study its own vaccine soon ... Clinical trialDrug research and developmentEbola vaccineEbola ... A clinical trial to evaluate an experimental Ebola vaccine has been launched in Mali by the Center for Vaccine Development (CVD ... A recent increase in funding for Ebola vaccine research is also enabling GSK to begin manufacturing at least 10,000 additional ... The trial is one of two possible clinical studies of an Ebola vaccine candidate that could begin this month. ...
Ebola Deaths May Reach Over 1,000 By Next Week (Exclusive Interview). By Sandy Dechert ... West Africa may even reach 1,000 deaths from Ebola this weekend. Thats just a guess, but not a bad guess, considering the ...
... has granted marketing approval to its two-dose Ebola vaccine regimen for the prevention of Ebola Virus caused by Zaire strain. ... The approval of the vaccine is a landmark moment for the company as it brings forth a vaccine to treat the deadly Ebola virus. ... has granted marketing approval to its two-dose Ebola vaccine regimen for the prevention of Ebola Virus caused by Zaire strain. ... We note that another company, Merck MRK, received FDA approval in December 2019 for its vaccine Ervebo (V920) to treat Ebola. ...
First products for Ebola Virus Disease prequalified WHO Prequalification Unit (PQT) added the below new products to its ...
As the race for an Ebola vaccine continues, experts gathered in Ghana from 8-10 April 2015 to review the clinical trial ... application for the Janssen Ebola Zaire Vaccine that will take place in Sierra Leone. ... the water we drink and the medicines and vaccines that treat and protect us. The Organization aims to provide every child, ... efforts continue to find an effective vaccine that can fight the virus both now and for future generations. ...
The World Health Organization and Merck approved using the vaccine in Congo. ... Why this vaccine?. This vaccine was developed to help protect people who have not yet been infected with Ebola. It has been ... What are the current treatments for Ebola?. There is no cure for Ebola, so the mainstay of treatment for Ebola virus involves ... Ebola vaccine deployed in Congo: What to know about the experimental approach. The World Health Organization and Merck approved ...
... but researchers are busy working on vaccines as the virus continues to spread in West Africa. In a few areas in Liberia, cases ... No cases of Ebola remain in the United States at the moment, ... Ebola Ebola Update: Vaccines in Tests, Spike in Mali, Dips in ... No cases of Ebola remain in the United States at the moment, but researchers are busy working on vaccines as the virus ... The vaccine contains a cold virus that infects chimpanzees, along with a single gene from the Ebola virus, which the ...
Our commitment goes beyond developing a vaccine for future use. Johnson & Johnson disaster response efforts continue through ... Janssens Ebola vaccine regimen was shipped and given to patients in late 2019 as part of a vaccination campaign in Rwanda and ... A study volunteer receives the vaccine in the Democratic Republic of the Congo (DRC) during the 2018-2020 outbreak ... A patient receives the vaccine in Rwanda as part of the UMURINZI vaccination campaign ...
Economist report on new Ebola vaccines underlines dangers - EbolaGate. *Economist report on new Ebola vaccines underlines ... Part II: Rockefeller Vaccine Secret Revealed - EbolaGate. *FINAL NAILS IN THE EBOLA SCAM COFFIN: The 2014 Ebola Outbreak is a ... VRM: Special Report « Vaccine Resistance Movement. *Bill Gates - Ebola, Death and Vaccines: Add In WHO, PATH, GAVI, UNICEF, ... Hoping Ebola Vaccines Are As Effective As Smallpox and Polio Vaccines? You Might Seriously Want to Rethink That - EbolaGate. ...
A new experimental Ebola vaccine displayed 100 percent efficacy in a clinical trial involving thousands in Guinea, Africa, ... A new experimental Ebola vaccine displayed 100 percent efficacy in a clinical trial involving thousands in Guinea, Africa, ... The vaccine, however, is not perfect. It appears to work only against one of the two most common strains of Ebola and it is not ... Experimental Ebola vaccine offers complete protection in clinical trial. Brian Zimmerman - Friday, December 23rd, 2016. ...
New studies show one shot of this experimental vaccine can trigger fast protection. Read more... ... New studies show one shot of this experimental vaccine can trigger fast protection.. Read more... ...
The head of the World Health Organization said Wednesday that he expects the first doses of Ebola vaccine targeting the strain ... WHO: 1st Ebola vaccines to arrive in Uganda next week Facebook , path id="pathAttribute" d="M 8.917969 7.773438 L 367.417969 ... vaccines alliance Gavi signed an agreement with Merck to secure 300,000 doses of its candidate Ebola vaccine for use in ... WHO: 1st Ebola vaccines to arrive in Uganda next week. Nov 16, 2022, 8:01 AM , Updated: Nov 18, 2022, 1:21 am ...
In addition, the vaccine targets dendritic cells, which are the same cells that Ebola and Marburg attack, says Geisbert. These ... According to Geisbert, this is the first vaccine system, or platform, that has protected nonhuman primates from both Ebola and ... New Ebola, Marburg Vaccines Effective in Animal Models. June 6, 2005. Article ... have developed vaccines against the Ebola and Marburg viruses that have been shown to be effective in non-human primates. ...
Antibodies from an Ebola survivor protected animals from deadly ebolaviruses and could help inform the development of potential ... Antibodies from Ebola survivor could lead to treatments and vaccines. At a Glance. *Antibodies from an Ebola survivor protected ... The 2014-16 Ebola outbreak in West Africa highlighted the need for an effective treatment or vaccine. Researchers have been ... The findings will help inform the development of potential treatments and vaccines for Ebola and related viruses. ...
Infectious Disease > Ebola Zaire Ebola Vaccines Produce Antibody Responses as Early as 14 Days. - Responses in adults and kids ... since vaccines are often distributed only when Ebola outbreaks occur. "Given that vaccines against EVD have typically been ... Three vaccine regimens for Zaire Ebola virus disease (EVD) produced antibody responses in adults and children, according to the ... Source Reference: PREVAC Study Team "Randomized trial of vaccines for Zaire Ebola virus disease" N Engl J Med 2022; DOI: ...
An Ebola vaccine will take the next critical steps in development under a $24.75 million contract through May 2020 between the ... "We can prevent future epidemics by acting quickly and decisively to complete development of Ebola vaccines and treatments for ... There currently are no vaccines or treatments approved for use against Ebola. The Centers for Disease Control and Prevention ( ... Todays agreement builds on previous Ebola vaccine development efforts undertaken by BPS with support from ASPRs Biomedical ...
In the first test of an Ebola virus vaccine in the US, the University of Maryland announced it will soon start human trial. ... head of Ebola vaccine research at Glaxo, said "We are accelerating development of this Ebola candidate vaccine at an ... The vaccine will be delivered in an adenovirus, that does not contain the full virus, just a single Ebola protein. ... In the first test of an Ebola virus vaccine in the US, the University of Maryland announced it will soon start human trial. ...
Collins argument and appropriates millions of dollars for Ebola research or an Ebola vaccine, and the magic bullet doesnt ... its still false to argue that with more money wed have an Ebola vaccine. Vaccine and drug development just simply doesnt ... No, Budget Cuts Didnt Prevent an Ebola Vaccine Scientists push back on NIH chiefs claims. ... Collins should be out there pointing out that the reason were even in a position to develop an Ebola vaccine is because of our ...
Canada has approved a vaccine to prevent Ebola in non-pregnant and otherwise healthy adults aged 18 and older. ... Canada approves Ebola virus vaccine for adults exposed to the deadly disease. A health-care professional adjusts her mask ... Canada has approved a vaccine to prevent Ebola in non-pregnant and otherwise healthy adults aged 18 and over following exposure ... Canada has approved a vaccine to prevent Ebola in non-pregnant and otherwise healthy adults aged 18 and older. ...
It is "vital that we ensure global preparedness for Ebola given that the worlds largest Ebola outbreaks have taken place in ... to define the required data set for filing of the Janssen Ebola vaccine regimen under the FDAs Animal Rule licensure pathway. ... for its investigational Ebola vaccine regimen.. The companys Janssen division is seeking license for the drug for the ... The company confirmed that two MAAs have been submitted in parallel supporting each vaccine in the two-dose regimen (Ad26.ZEBOV ...
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The Guardian article titled Ebola vaccine offered in exchange for sex, Congo taskforce meeting told, was published on Tuesday ... "However, the IRC clarified that the analysis of their raw data revealed that no specific Ebola-related services was mentioned ... These women and girls expressed their fears and concerns about the Ebola response considering the social and security context ... "In focus group discussions, some participants expressed concerns about women and girls being offered Ebola-related services in ...

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