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The CDC indicated nasal spray flu vaccine should not be used during 2016-2017
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The purpose of this study is to evaluate FluMist with and without Ampligen in healthy volunteers.
Influenza epidemics continue to represent a significant medical problem in the developed as well as the developing world. Even with existing vaccines, annual influenza epidemics typically results in 20-50 million cases, resulting in 30,000-40,000 deaths in the U.S. alone. A possible pandemic could have even more devastating consequences. Current vaccines have a number of disadvantages including slow and expensive manufacturing, and a relative lack of efficacy in elderly, children and immune-compromised populations. These disadvantages would be multiplied during a pandemic. Use of Ampligen® as an adjuvant combined with FluMist® has a number of potential advantages as compared to traditional inactivated vaccines: it is simpler to administer (intranasally), generation of a broader immunity at the natural site of entry of the influenza virus as well as systemic immunity (and hence should be more efficacious than traditional vaccines) and may stimulate cross-protection against pre-pandemic H5N1 and/or H7N9 avian influenza strains. As FluMist®, due to its intranasal administration, imitates the natural entry of the influenza virus, it will generate local 'first-line' immunity as well as the traditional systemic immunity; therefore, at least theoretically provide greater protection than injectable vaccines.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| FluMist + Ampligen, Group 1 | Experimental | Nasal administration; dose group 1; FluMist + Poly I:Poly C12U 50 ug; 3 doses separated by 28 days |
|
| FluMist + Ampligen, Group 2 | Experimental | Nasal administration; dose group 2; FluMist + Poly I:Poly C12U 200 ug; 3 doses separated by 28 days |
|
| FluMist + Ampligen, Group 3 | Experimental | Nasal administration; dose group 3; FluMist + Poly I:Poly C12U 500 ug; 3 doses separated by 28 days |
|
| FluMist + Ampligen, Group 4 | Experimental | Nasal administration; dose group 4; FluMist + Poly I:Poly C12U 50 ug; 3 doses separated by 28 days |
|
| FluMist + Ampligen, Group 5 | Experimental | Nasal administration; dose group 5; FluMist + Poly I:Poly C12U 1250 ug; 3 doses separated by 28 days |
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Poly I:Poly C12U 50 ug | Drug | Poly I:Poly C12U 50 ug; 3 doses; nasal administration every 28 days |
|
| Measure | Description | Time Frame |
|---|---|---|
| Evaluate safety and tolerability | Reactogenicity; other adverse events, serious adverse events, new onset of chronic illnesses, and adverse events of special interest | Every 28 days |
| Measure | Description | Time Frame |
|---|---|---|
| Evaluation of immune response | Evaluated by measurements of serum antibody HI titers against the seasonal viral strains contained in vaccine and various H5N1 and/or H7N9 clades. Immunogenicity will be evaluated by comparing the titer levels in each of the treatment groups. | Every 28 days |
| Immunogenicity Assessments |
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Inclusion Criteria:
Males and females in good general health, 19 to 49 years of age.
Subjects must provide written informed consent.
Subjects must be willing to participate through study completion.
Have not been vaccinated for influenza virus in the current season or had a known influenza virus infection in the current season
Subjects must be willing to undergo nasal washes and provide parotid saliva, urine and blood samples per protocol for safety and immunogenicity analyses.
Females of childbearing potential must have a negative urine pregnancy test.
A female volunteer must:
Agree to consistently use effective contraception from at least 21 days prior to enrollment through the Day 84 clinic visit for sexual activity that could lead to pregnancy;
Effective contraception is defined as using any of the following methods:
Or not be of reproductive potential, such as having reached menopause (no menses for 1 year) or having undergone hysterectomy, bilateral oophorectomy, or tubal ligation;
Or be sexually abstinent;
Volunteers who were born female must also agree not to seek pregnancy through alternative methods, such as artificial insemination or in vitro fertilization, until after the Day 84 clinical visit.
Screening Laboratory Inclusion Criteria. Screening values must be within Institutional Normal Range, unless they are not clinically significant (i.e. values do not reach the threshold for mild (Grade 1) or higher toxicity as defined in Appendix D). Repeat laboratory testing may be performed at the discretion of the clinical investigators for spurious results on a case by case basis.
Subjects must weigh at least 120 pounds at screening
Exclusion Criteria:
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| Name | Affiliation | Role |
|---|---|---|
| David R Strayer, MD | AIM ImmunoTech Inc. | Study Director |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| The University of Alabama at Birmingham | Birmingham | Alabama | 35294 | United States |
| PubMed Identifier | Type | Citation | Retractions |
|---|---|---|---|
| 17922395 | Background | Ichinohe T, Tamura S, Kawaguchi A, Ninomiya A, Imai M, Itamura S, Odagiri T, Tashiro M, Takahashi H, Sawa H, Mitchell WM, Strayer DR, Carter WA, Chiba J, Kurata T, Sata T, Hasegawa H. Cross-protection against H5N1 influenza virus infection is afforded by intranasal inoculation with seasonal trivalent inactivated influenza vaccine. J Infect Dis. 2007 Nov 1;196(9):1313-20. doi: 10.1086/521304. Epub 2007 Oct 5. | |
| 20827774 |
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| ID | Term |
|---|---|
| D007251 | Influenza, Human |
| ID | Term |
|---|---|
| D012141 | Respiratory Tract Infections |
| D007239 | Infections |
| D009976 | Orthomyxoviridae Infections |
| D012327 | RNA Virus Infections |
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| ID | Term |
|---|---|
| C047490 | poly(I).poly(c12,U) |
| C000613429 | FluMist |
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| FluMist + Placebo, Group 6 | Experimental | Nasal administration; dose group 6; FluMist + placebo; 3 doses separated by 28 days |
|
|
| Poly I:Poly C12U 200 ug | Drug | Poly I:Poly C12U 200 ug; 3 doses; nasal administration every 28 days |
|
|
| Poly I:Poly C12U 500 ug | Drug | Poly I:Poly C12U 500 ug; 3 doses; nasal administration every 28 days |
|
|
| Poly I:Poly C12U 1250 ug | Drug | Poly I:Poly C12U 1250 ug; 3 doses; nasal administration every 28 days |
|
|
| Placebo | Drug | Placebo; 3 doses; nasal administration every 28 days |
|
| FluMist | Drug | FluMist 0.2 ml; 3 doses; nasal administration every 28 days |
|
Micro-neutralization assay and IgA (nasal wash and parotid saliva) |
| Every 28 days |
| Background |
| Ichinohe T, Ainai A, Ami Y, Nagata N, Iwata N, Kawaguchi A, Suzaki Y, Odagiri T, Tashiro M, Takahashi H, Strayer DR, Carter WA, Chiba J, Tamura S, Sata T, Kurata T, Hasegawa H. Intranasal administration of adjuvant-combined vaccine protects monkeys from challenge with the highly pathogenic influenza A H5N1 virus. J Med Virol. 2010 Oct;82(10):1754-61. doi: 10.1002/jmv.21824. |
| 25128802 | Result | Overton ET, Goepfert PA, Cunningham P, Carter WA, Horvath J, Young D, Strayer DR. Intranasal seasonal influenza vaccine and a TLR-3 agonist, rintatolimod, induced cross-reactive IgA antibody formation against avian H5N1 and H7N9 influenza HA in humans. Vaccine. 2014 Sep 22;32(42):5490-5. doi: 10.1016/j.vaccine.2014.07.078. Epub 2014 Aug 13. |
| D014777 | Virus Diseases |
| D012140 | Respiratory Tract Diseases |