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Cytochrome P450 testing covered by Health policies

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10% of Caucasians are “non metabolizers”.  This means that they cannot metabolize more than 50% of today’s drugs such as adderall, and other SSRIS.  It is suspected that the heinous trend of school shootings and suicides are caused by non metabolizers who are given psychiatric drugs without first being tested for their ability to metabolize them.  Because this test is not standard of care hospitals and doctors who destroy lives by giving counter indicated medication can not be successfully sued.  There is a movement to make this test standard of care but it is being thwarted by the invested pharmacuetical companies who would stand to lose billions of dollars if the public knew.

Description: 

The cytochrome p450 (CYP450) family is involved in the metabolism of a significant proportion of currently administered drugs, and genetic variants in cytochrome p450 are associated with altered metabolism of many drugs. It is proposed that genetic testing for cytochrome p450 variants may assist in selecting and dosing drugs that are impacted by these genetic variants.

Drug efficacy and toxicity vary substantially between individuals.  Because drugs and doses are typically adjusted to meet individual requirements as needed by using trial and error, clinical consequences may include a prolonged time to optimal therapy and serious adverse events.

Various factors may influence the variability of drug effects, including age, liver function, concomitant diseases, nutrition, smoking, and drug-drug interactions. Inherited (germline) DNA sequence variation (polymorphisms) in genes coding for drug metabolizing enzymes, drug receptors, drug transporters, and molecules involved signal transduction pathways also may have major effects on the activity of those molecules and also on the efficacy and toxicity of the drug.

Pharmacogenomics is the study of how an individual’s genetic inheritance affects the body’s response to drugs. It may be possible to predict therapeutic failures or severe adverse drug reactions in individual patients by testing for important DNA polymorphisms (genotyping) in genes related to the metabolic pathway (pharmacokinetics) or single transduction pathway (pharmacodynamics) of the drug. Potentially, test results could be used to optimize drug choice and/or dose for more effective therapy, avoid serious adverse effects and decrease medical costs.

Some CYP450 enzyme genes are highly polymorphic, resulting in some enzyme variants that have variable metabolic capacities among individuals, and some with little to no impact on activity.

Individuals with a lack of function activity in these enzymes (CYP2C19, CYP2D6, CYP2C9, etc.) can be classified according to how fast they metabolize medications:

  • Poor metabolizers (PMs): lack active enzyme gene alleles, they will process a certain drug more slowly than normal because of the missing enzyme(s), the medication can build up in their system which can increase the likelihood that it will cause side effects. The individual might still be able to benefit from the medication, but at lower dosages.
  • Intermediate metabolizers (IMs): have one active and one inactive enzyme gene allele, these individuals have a reduced enzyme function in processing drugs, they may not process some medications as well as a normal metabolizer would. This can increase risk of side effects and drug interactions.
  • Normal metabolizers (extensive metabolizers Ems): these individuals have 2 copies (alleles) of the most common (wild type) DNA sequence of a particular CYP450 enzyme gene resulting in an active molecule and are termed extensive metabolizers. Medications are processed normally, these individuals are more likely to benefit from treatment and have fewer side effects than people who don’t process the same medication(s) as well.
  • Ultra-rapid metabolizers (UMs): individuals with more than 2 alleles of an active enzyme gene, which cause the medications to leave the body too quickly and often before they have had a chance to work properly. These individuals will likely need a higher than usual dose of medications.

US patents on Cannibas

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Patents Related To The Dietary And Medicinal Study And Use Of Cannabis

US Patent 6,630,507 (pdf-120KB)
“Cannabinoids as Antioxidants and Neuroprotectants” Assigned to the United States of America, it provides guidelines for relevant medical conditions and dosage schedules for CBD. Review LOG notes on the use of vaporization to separate CBD from THC
Medicinal Acidic Cannabinoids / US 7,807,711 B2 (pdf-120KB)
Invention relates to an acidic cannabinoid, the method for extracting and preparing.
Pharmaceutical Compositions For The Treatment Of Chronic Obstructive Pulmonary Disease US 2009 / 0197941 A1 Aug. 6, 2009 (pdf-132KB)
Discusses the preferred ratio of CBD to THC being 1:1
Anti-nausea And Anti-vomiting Activity Of Cannabidiol Compounds / US 2003 0225156 A1 Dec. 4, 2003 (pdf-64KB)
Inventor: Raphael Mechoulam. The applied dose can be adjusted based on the relative bioavailability and potency of the administered compound. Adjusting the dose to achieve maximal efficacy…
Combination Of Cannabinoids For The Treatment Of Peripheral Neuropathic Pain US 2010/0035978 A1 Feb 11, 2010 (pdf-1.5MB)
This patent identifies “the ratio of CBD:THC by weight is between 10:1 to 1:10.”
US Patent 6,410,588 B1 (pdf-1.5MB)
Feldmann, et al. “Use of Cannabinoids as Anti-inflammatory Agents”
US 2007/0099987 A1 (pdf-1.4MB)
Weiss, et al. “Treating or Preventing Diabetes with Cannabidiol”
US Patent 6,946,150 B27 (pdf-2.7MB)
Brian Whittle. “Pharmaceutical Formulation.” Using a pump action spray to administer cannabinoids via the mucosal surfaces

HPV vaccine (Gardasil/Cervarix) Orthomolecular Treatment Protocol

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Severity of side effects

When other health experts re-evaluated those cases, they determined 1,112 (44%) to be serious. The initial onset of symptoms occurred several weeks to a year after the HPV vaccine was given. They included: headache, dizziness, muscle weakness and pain, nausea, hypersomnia, learning difficulty, impaired writing, photophobia, tremors of arms, feet and fingers, joint pain, irregular menstruation, gait disturbance, memory loss, skin eczema and acne.

Girls who had adverse effects from the HPV vaccine were variously diagnosed with:

  1. Higher brain dysfunction
  2. Guillain-Barré syndrome
  3. Multiple sclerosis
  4. ADEM: acute disseminated encephalomyelitis
  5. SSPE: subacute sclerosing panencephalitis
  6. CRPS: Complex regional pain syndrome
  7. POTS: Postural orthostatic tachycardia syndrome
  8. Anti-phospholipid antibody syndrome
  9. SLE: systemic lupus erythematosus
  10. Rheumatoid arthritis
  11. Chronic fatigue syndrome
  12. Fibromyalgia
  13. Cushing’s syndrome (exposure to high level of cortisol)
  14. Hashimoto’s disease (immune system attacks the thyroid)
  15. Hyperprolactinemia (high prolactin, induces breast development and lactation)

Laboratory findings included:

  1. Normal blood chemistry
  2. No inflammatory finding in the blood
  3. Increased pro-inflammatory cytokines in the spinal fluid (IL-2, IL-10, TNF-à)
  4. Reduced brain blood flow by perfusion scintigraphy
  5. High leukocyte sensitivity against aluminum.

 

HPV vaccine contains toxic aluminum

Vaccines often contain an adjuvant, which is an additional chemical added to provoke the body’s immune response to the vaccine. The HPV vaccines contained an adjuvant that consisted of an aluminum compound, amorphous aluminum hydroxyphosphate sulfate (AAHS).

Current research strongly implicates aluminum adjuvants in various inflammatory neurological and autoimmune disorders in both humans and animals. For example, a recent research paper explained that nanomaterials such as this aluminum adjuvant can be transported by immune system cells first into the blood, lymph nodes, and spleen, and in some cases may penetrate into the brain. [1] This type of access throughout the body is potentially life-threatening. The brain symptoms are often the most delayed because of the time the aluminum takes to travel from the blood through the blood-brain-barrier into the brain.

Aluminum accumulates in neurons in the brain, and it is toxic to neurons, causing a variety of pathological conditions. It inhibits uptake of dopamine and serotonin, which are important neurotransmitters in the brain. Aluminum toxicity is a known factor in Alzheimer’s disease, and may contribute symptoms of Parkinson’s disease. Dementia resulting from kidney dialysis is related to aluminum and results in memory loss, loss of coordination, confusion and disorientation. In animal experiments, rabbits given aluminum showed difficulty in memory retention and difficulty in learning.

ORTHOMOLECULAR PROTOCOL

First baby born from IVF technique which eliminates inherited disease

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Lucas Meagu was at high risk of inheriting a rare form of muscular dystrophy.  Lucas’ mother Carmen, 26, who works in recruitment, inherited Charcot-Marie-Tooth disease from her father who suffered with the illness all his life.

The genes responsible for Charcot-Marie-Tooth disease were isolated.  Doctors took DNA swabs from Mrs Meagu, her mother and Lucas’s father Gabriel, 30, who works for Vodafone.They then compared the gene sequences at 300,000 different points of the chromosomes to work out which section of genetic code was defective and responsible for the abnormality.The couple then underwent a normal IVF cycle but, crucially, the embryos created from the procedure were biopsied to find out which ones were free of the genetic disease.  Read more…

Microbiologists confirm Ancient Script formula kills MRSA

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Anglo-Saxon cow bile and garlic potion kills MRSA

Microbiologists were astonished to find that not only did the salve clear up styes, but it also tackled the deadly superbug MRSA, which is resistant to many antibiotics. Read more…

Studies show: Natural Mumps, Measles, Chicken Pox & Influenza viruses protect against cancer

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7081680-digital-illustration-of-influenza-virus-in--colour-background Influenza virus

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GENETICALLY ENGINEERED virus, administered at high dose, the virus set about destroying the cancer cells, leading to complete remission and no tumors for 9 months. Currently, 11 months after treatment, the patient is still cancer free.The larger effects of this step will be discovered soon, a trial for 20 patients has been approved for September, 2014. In addition, the measles virus, as well as other viruses, will be studied for their potential to cure other types of cancer.

Abstract

VLA Comment:  VACCINE POLICY IS HARMFUL TO THE POPULATION:

Getting this infectious disease “naturally” (as listed in the studies below) apparently prevents the disease.   Clearly the above protocol  (creating a genetically engineered virus strain) was advanced by researchers because they realized that “naturally gained” wild viruses protect against cancer.  Hence, they thought, lets genetically engineer the virus in our labs to cure cancer that people are getting because vaccination does not impart the same complex protective quality as in nature. And besides we can patent it and make money on the vaccines, then make money on the disease it provokes and then make money on an artificial cure to an artificial vaccine.

Editor:  So why don’t we get the natural diseases, like before we had the cancer epidemic that is the leading cause of death for children,  and prevent cancer in the first place?  The money make’s purpose is to design expensive pharmacuetical lab made genetic viruses that mimick natural virus in order to fix the cancer that we got by being artificially stimulating our immune system by be vaccinated.

VLA Comment:  The above protocol uses genetically modified virus.  But as Doctor Palevsky writes…”The assumption among these people is that the genetic information of the micro-organisms that cause these diseases does not already exist inside the human body before the injection occurs. This assumption is one of the deepest flaws in current scientific ‘thinking.’ Any attempt to protect against diseases by injecting them into the body, especially since so much of what comprises human DNA is reportedly of viral genetic origin, is a set-up to destroy the human species. It’s possible, and even likely, that the genetic material of these wide ranges of diseases, may already be a part of the human genome, even if the diseases are not present, and even if the people have never been exposed to anyone with the diseases”

MUMPS: Researchers investigated whether mumps might engender immunity to ovarian cancer through antibodies against the cancer-associated antigen MUC1 abnormally expressed in the inflamed parotid gland.  Read more….

MEASLES:  Albonico et al found that adults are significantly protected against non-breast cancers — genital, prostate, gastrointestinal, skin, lung, ear-nose-throat, and others — if they contracted measles (odds ratio, OR = 0.45), rubella (OR = 0.38) or chickenpox (OR = 0.62) earlier in life. [Med Hypotheses 1998; 51(4): 315-20].

MEASLES: Montella et al found that contracting measles in childhood reduces the risk of developing lymphatic cancer in adulthood [Leuk Res 2006; 30(8): 917-22].

MEASLES: Alexander et al found that infection with measles during childhood is significantly protective — it cuts the risk in half — against developing Hodgkin’s disease (OR = 0.53) [Br J Cancer 2000; 82(5): 1117-21].

MEASLES: Glaser et al also found that lymph cancer is significantly more likely in adults who were not infected with measles, mumps or rubella in childhood [In J Cancer 2005; 115(4): 599-605].

COMMON INFECTIONS: Gilham et al found that infants with the least exposure to common infections have the greatest risk of developing childhood leukemia [BMJ 2005; 330: 1294].

EARLY EXPOSURE TO INFECTIONS:Urayama et al also found that early exposure to infections is protective against leukemia [Int J Cancer 2011; 128(7): 1632-43].  Read more….

CHICKEN POX (VARICELLA Canniff J., Donson A.M., Foreman N.K., Weinberg A. Cytotoxicity of glioblastoma cells mediated ex vivo by varicella-zoster virus-specific T cells. J Neurovirol. 2011;17(October (5)):448–454. [PubMed] Canniff et al. reported an association between those individuals with clinical or laboratory evidence of varicella-zoster virus (VZV) infection and lower risk of glioma.A glioma is a type of tumor that starts in the brain or spine. It is called a glioma because it arises from glial cells.

CHICKEN POX IN CHILDHOOD: Silverberg J.I., Kleiman E., Silverberg N.B., Durkin H.G., Joks R., Smith-Norowitz T.A. Chickenpox in childhood is associated with decreased atopic disorders, IgE, allergic sensitization, and leukocyte subsets. Pediatr Allergy Immunol. 2012;23(February (1):50–58. [PubMed Silverberg et al. also reported that wild-type VZV infection up to 8 years of age was found to be protective against atopic disorders that are thought to be “mediated by suppression of IgE production and allergic sensitization, as well as altered leukocyte distributions.

Chicken Pox references taken from Goldman, King STUDY

INFLUENZA VACCINES Influenza Virus Infection Elicits Protective Antibodies and T Cells Specific for Host Cell Antigens Also Expressed as Tumor-Associated Antigens: A New View of Cancer ImmunosurveillanceUzoma K. Iheagwara, Pamela L. Beatty, Phu T. Van, Ted M. Ross, Jonathan S. Minden, and Olivera J. Finn
Cancer Immunology, March 1, 2014; 2: 263 – 273.

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CARDIOVASCULAR DISEASE PROTECT BY EARLY CHILDHOOD MEASLESREAD STUDY…

UPDATE ON GENETICALLY ENGINEERED MEASLES VIRUS to CURE CANCER (MAYO CLINIC)

Dr. Stephen Russell, a professor of molecular medicine at the Mayo Clinic who spearheaded the treatment, said his research has failed to live up to his initial hope to use an engineered form of the measles virus as a kind of guided missile against multiple myeloma, a cancer that attacks white blood cells. Even though…. READ…

POLIOThe early polio vaccine that was given to millions of children in the 1950s contained a cancer causing virus, SV40.  This virus has been found in biopsies of cancer tissue today. Read more…

Researchers have found the SV40 virus in 60% of the human lung tumors he was studying, (SV40 stands for Simian Virus the 40th virus found). Eventually, sixty different labs confirmed the results. THE ATLANTIC.COM ARTICLE Riveting

NEUROLOGICAL COMPLICATIONS OF VACCINATION

Poser C.M. Neurological complications of vaccinations. Mealey’s Litigation Report. Thimerosal Vaccin. 2003;1(April (10))

CLINICAL INFECTIOUS DISEASES JOURNAL: NYC Outbreak: Measles transmission from a twice vaccinated individual.

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Conclusions. This is the first report of measles transmission from a twice vaccinated individual. The clinical presentation and laboratory data of the index were typical of measles in a naïve individual. Secondary cases had robust anamnestic antibody responses. No tertiary cases occurred despite numerous contacts. This outbreak underscores the need for thorough epidemiologic and laboratory investigation of suspected measles cases regardless of vaccination status.

“Tell friends and family who are sick, or have recently had a live vaccine (such as chicken pox, measles, rubella, intranasal influenza, polio or smallpox) not to visit.”

 

Starting in 2012 Vermont had declared a statewide epidemic of whooping cough. To date there has been a total of 612 confirmed cases of pertussis, of which 90 percent have been vaccinated against the bacteria with the Tdap vaccine.

 

According to CSN.Philly.com, the New York State Department of Health reports that 18 of 20 people infected in a recent measles outbreak in New York City were children who had been vaccinated.

 

According to USA Today, since August 107 American children have polio symptoms, such as paralyzed limbs (Non-polio acute flaccid paralysis, NPAFP). According to National Geographic, all the children had been successfully immunized against polio. In 2011 there were an extra 47,500 new cases of NPAFP in India. Clinically indistinguishable from polio paralysis but twice as deadly, the incidence of NPAFP was directly proportional to doses of oral polio received.

 

In a study published in the Journal of Pediatrics, “Adverse Events following Haemophilus influenzae Type b Vaccines in the Vaccine Adverse Event Reporting System, 1990-2013” CDC and FDA researchers identified 749 deaths linked to the administration of the Hib vaccine, 51 percent of which were sudden infant death (SIDS)

 

Blaming the unvaccinated

Instead of blaming the unvaccinated, if there is such a concern about infectious disease outbreaks, why aren’t health officials requiring a two-week quarantine of all children and adults who receive vaccination and shedding the vaccine virus. Two weeks is the minimum amount of time required to prevent transmission of infectious diseases.

Excerpt:  St. Jude’s Hospital patient guide

Avoid live virus vaccines and people who have received one

Some vaccines are made from live viruses. Currently, these include oral polio, smallpox, MMR (measles, mumps, and rubella), and nasal flu vaccines.

These vaccines may pose a threat to your child’s health. Any person with a weakened immune system, including patients with cancer or HIV infection should not receive live virus vaccines.

Do not allow people to visit your child if:

  • They have received oral polio or smallpox vaccines within 4 weeks;
  • They have received the nasal flu vaccine within one (1) week; or
  • They have rashes after receiving the chickenpox (varicella) vaccine or MMR (measles, mumps, rubella) vaccine.

3. Outbreak of Measles Among Persons With Prior Evidence of Immunity, New York City, 2011 http://cid.oxfordjournals.org/content/early/2014/02/27/cid.ciu105