Big Pharma has corrupted your healthcare#mustread#Android#iPad

Medical researchers at Dartmouth have issued a dire warning about your doctor and the drugs he dishes out: They’re part of a system designed for profit not for improving your health.

Researchers at the Dartmouth Institute for Health Policy & Clinical Practice have issued a report that puts the spotlight on significant ways that international pharmaceutical corporations have bought off doctors and slanted research to favor their bottom lines. The researchers say that the entire health care system, as a result, has been distorted by “obvious corruption.”

As the scientists note, when it comes to research: “finance dictates the activity.” In other words money talks and studies on how drugs work are designed to prove their effectiveness even if the pharmaceuticals are basically worthless…

Continue to the Article Here

http://easyhealthoptions.com

California Infant Dies after 8 Vaccines, Family Gets Him Back from Hospital Cremated#Android#iPad#iBelieve

 by Augustino Ursino

 Parents in California are distraught after losing their infant son after being vaccinated. He died in his sleep and was taken to the hospital already deceased. Hospital staff ruled his death as sudden infant death syndrome. The couple was told an autopsy was required to be performed on their son.

After returning home, waiting to get an update, they never received one. Numerous phone calls were made to get answers. Weeks went by. Finally, they received verbal confirmation and told their son was best not to be seen prior to being cremated, because of the condition he was in. Once cremated, they could pick up the remains of their child from the crematory. They were not given the chance to say their goodbyes.

More than one year and four months have passed and the family has yet to receive his autopsy report. It turns out their son was given a vaccine not approved for his age and an extra dose of the hepatitis B vaccine that he shouldn’t have received until later on.

This harrowing story…

Continue to the Article Here

http://vactruth.com

Cervarix: Will my life ever be normal again?#Android#iBelieve#iPad

By Saskia from Devon, UK

Cervarix changed my life.

Cervarix changed my life: now I would never be able to manage the sort of day I took in my stride as a thirteen year old. I can’t even remember what a day with energy feels like.

Before receiving the HPV vaccine at 14, I was an active, mostly healthy child. As we lived some distance away from my school, I had fairly long days: I would leave the house at 7.30 am and return at 5.30 pm, but always came back with lots of energy. I enjoyed walking, swimming, horseback riding etc. after school. No matter how long my day was, I certainly never experienced the complete exhaustion I felt after the Cervarix vaccine.

The difference in energy was particularly noticeable because it happened immediately. The day I got the first HPV vaccination Cervarix, on the 28th September 2009, I came home feeling sick and incredibly tired and had to go straight to bed. The next day at school was a struggle because I felt nauseous and so low on energy, and once again I ‘crashed’ when I got home and had to go straight to sleep.

This happened every day for a week or so. My mum rang up the local health service to talk to them, but they said this wasn’t a possible side effect of the vaccine and there was no way of registering any side effects.

Eventually mum managed to get through to a central line where she could register the nausea and fatigue I was experiencing. They also told her it wasn’t a known side effect of Cervarix and claimed there was no connection.

The same symptoms happened after the other two injections of Cervarix (on 13th November 2009 and 24th April 2010) but each time it got worse. After the second vaccination I experienced the same sickness and exhaustion but it lasted for a fortnight.

After the third vaccination I honestly don’t think life was ever really ‘normal’ again. The fatigue became more and more constant. I struggled with low energy levels at school, would fall asleep at lunchtime and on the way home and often had to go to bed as soon as I got back.

The constant exhaustion became very limiting. I had to stop swimming which I had done at a competitive level and greatly enjoyed. I also had to turn down a World Challenge Trip to Kenya despite having started fundraising because I realized I simply would not have the energy to walk each day. My fatigue now is sometimes completely debilitating and I spend much of my time in bed. I have become used to having to turn opportunities down because of it.

Not long after the third injection, the chest pain started. The first time it happened I was in a class at school and suddenly got a crushing pressure and pain on my left side. I felt faint and dizzy and was in so much pain I could barely talk.

I ended up going to a local A&E where they did an ECG and found that I had a very fast and slightly abnormal heart-rate accompanying the pain and so I was transferred by ambulance to Torbay Hospital. The pain eventually subsided and further ECGs came back normal and so I was discharged.

This was the start of an incredibly scary and difficult journey to getting diagnosed. I have experienced debilitating, severe and intermittent chest pain ever since. It has taken years and lots of time and energy to get a diagnosis.

The sickness and nausea is also something which started with the vaccine and has never really gone away. I spend most of the day feeling very queasy, sometimes to the point that I cannot eat anything. Despite trying many different anti-nausea medicines, I have yet to find one that works. I also started getting dizzy and fainting, particularly on standing or exertion, which has been very unpleasant and scary. Recently, my fainting has become significantly worse and now happens almost daily which is frightening and dangerous, and has led to several concussions.

Along with the horrible, debilitating symptoms of fatigue, nausea, chest pain, dizziness, fainting and gastrointestinal issues which are all linked, has come the struggle to get a diagnosis and adequate medical support.

I have been in and out of doctors’ appointments and hospitals since I was thirteen. There have been countless blood tests, ECGs and scans. Both my parents and I have had to spend so much time and energy researching and pushing for some help.

Despite the severity of my symptoms, they were initially dismissed as anxiety, then food intolerances, and later, because nothing was structurally wrong with my heart, the medical support became virtually non-existent and I was even told it was all in my head. One example of this treatment is when I went to a GP to ask for something to help with my frequent vomiting and was instead given the name of a book about ‘psychosomatic illness’. I can’t begin to describe how painful that is.

It was 4 years after my symptoms had started that I was finally put on a week-long heart monitor. This monitor picked up severe spikes in my heart rate. It showed times when my heart rate was quickly accelerating from 70 bpm to 180 bpm. These ‘spikes’ coincided with when I was experiencing chest pain or fainting. I was given a probable diagnosis of Postural Orthostatic Tachycardia Syndrome (POTS) which has since been confirmed by a specialist in Derriford Hospital following further testing.

I am now nineteen years old and despite finally being on various medication to help manage my symptoms, I am severely limited by my ill-health. I have no energy and often had to miss lectures, supervisions, social events and various opportunities because I am either too fatigued, too faint, or in too much pain to participate. Recently my ill-health has forced me into the incredibly difficult decision to drop out of my second year at Cambridge University, because studying has become impossible.

I have gone from enjoying exercise and loving long walks on the moors to sometimes fainting after a short flight of stairs, being reliant on taxis, and having to spend much of my time in bed.

I have gone from being a normal teenager to a disabled one, and it seems to have all been triggered by the vaccine.

Since the Cervarix injections and since developing POTS I have lost count of how many times I have been in hospital, experienced severe chest pain, fainted, missed important opportunities, and been sick.

In fact, I have actually forgotten what having a healthy day feels like as I am never symptom-free anymore.

This article in its entirety is compliments of www.sanevax.org

Saskia, I am so sorry you are going through this painful time.  It is a shame that the medical establishment has let you down in so many ways and the psychosomatic illness suggestion just adds insult to injury.  Just a lazy, weak cop-out. It is so much more pleasant when a doctor just admits when they do not know what is wrong.

I have good news for you, there are doctors that are experienced in this area, and will take you under their wing.  Distance is not an issue in most instances.  The team at SaneVax Inc. has wonderful contacts, and I have some as well within the Featured Doctors menu option on my blog. There are many others that have received relief and healing from Cervarix and Gardasil injuries.

I hope you are soon to be able to receive better care and to resume your studies at Cambridge University.

You can tell you are strong and patient, and I know that as you remember who you are, that you will continue to be guided on this healing path. 

Here is a musical gift that I hope lifts your spirits at this time. My ten year-old daughter was watching me work and I asked her which musical group I should pick a song from.  She felt this would be a good group.  Hang in there, your friend jen.

 

 

 

The Scary Facts Most Parents Don’t Know About Vaccine Injury Compensation#Family#Android#iPad

by Missy Fleugge

Vaccine injures and adverse reactions are massively under-reported, as admitted by the Centers for Disease Control. Estimates show that only one to ten percent of vaccine injuries and deaths are actually filed with the government.

In the United States, the government has created a database to keep track of hundreds of kinds of reactions to vaccinations, including fevers, soreness, seizures, swelling of the brain, arthritis, and death. Since its inception, this program has awarded over $2.5 billion to individuals and families who have suffered vaccine injury and death. These awards are funded by taxes on vaccines.  [1]

Even though health care providers are required by law to report vaccine injuries, most of these adverse events are not made public in this database, known as the Vaccine Adverse Event Reporting System (VAERS). Parents may not know that common reactions to vaccines, including fevers, long bouts of crying, or rashes following vaccination should be reported to their child’s doctor. When a more serious adverse event occurs, parents may be too overwhelmed to make sure a report is filed.

Unfortunately, rather than educating doctors and parents about the importance of reporting all adverse reactions to vaccines to the VAERS database, the US government has just tightened the requirements for reporting an adverse reaction, making the process even more difficult…

Continue to the www.vactruth.com article here

Update: HPV vaccines and the Supreme Court of India#HPV#Vaccines#Android

 By Norma Erickson

January 2013, the government of India was ordered by their Supreme Court to file an answer to allegations put forth in a petition filed on behalf of Gramya Resource Centre for Women from Andhra Pradesh. This petition challenged the licensing of Gardasil and Cervarix for use in the private sector as well as attempts to introduce HPV vaccines for use in the public sector. The petition implicated the Drugs Controller for having licensed the vaccines without adequate research on safety and efficacy;  the Health Ministry for not carrying out an enquiry into licensing of these vaccines as ordered by the Parliamentary Standing Committee on Health and Family Welfare in April 2010 and not taking any action on the report of the internal enquiry committee despite all alleged irregularities associated with the PATH project being confirmed.

October 2014, India’s Supreme Court Justices issued instructions for all petitioners and respondents in the ongoing case against to either serve the opposition with copies of affidavits filed and/or file any affidavits and rejoinder affidavits pertinent to the case within the next four weeks. The matter was then set for what was supposed to be a final hearing on January 13, 2015.

When the ’final’ hearing date arrived, several respondents had still not complied with these instructions. At least one of them went so far as to hold their two-and-a-half-foot tall affidavit for presentation to the Court on  January 13th. The Honorable Supreme Court Justices did not seem to be amused.

After hearing the evidence presented on January 13th, Justices Dipak Misra and Prafulla C. Pant issued an order reminding all participants of concerns raised in a prior hearing on 12 August 2014. Those concerns are as follows:

  • Did the Drugs Controller of India and the ICMR (Indian Council on Medical Research) follow proper protocol for the introduction of HPV vaccines prior to the use of said vaccines in the demonstration projects in India?
  • What actions were taken after the submission of the Parliamentary Committee’s 72nd report on August 30, 2014?
  • What were the reasons for choosing certain places in Gujarat and Andhra Pradesh for the HPV vaccine demonstration projects?
  • What actually caused the deaths and other ailments experienced after HPV vaccine administration in said demonstration projects?
  • What steps were taken to monitor the safety of HPV vaccines by the Union of India and the State Governments who have an equal role in guarding the health of the nation?
  • Was proper consent given by the parents/guardians of all girls who were administered HPV vaccines, as the Justices been apprised?
  • What protocol is required to be observed/followed when this type of vaccination program is conducted?

The Honorable Supreme Court Justices deemed it appropriate to grant permission for the State of Gujarat, State of Andhra Pradesh, and State of Telangana to be added as parties to the current case.

The Justices also agreed to M/S Glaxosmithkline Asia Pvt. Ltd. and MSD Pharmaceuticals Pvt. Ltd., the companies responsible for manufacturing HPV vaccines, being served as respondents in the proceedings.

Justices Misra and Pant granted permission for the attorneys representing the petitioners to serve papers on the concerned Ethics Committees of all three States involved in the HPV demonstration projects.

In view of the fact that the above mentioned concerns had still not been adequately addressed, some respondents had failed to appear for prior hearings, and others had ignored requests for information or failed to submit affidavits in a timely manner the Justices included the following statements in the current order:

  • This Court hopes and trust(s) that on the next date of hearing, the Standing Counsel of all the States shall remain present and argue the matter.
  • The Union of India shall direct its competent authority to produce the file by which the Drugs Controller General of India approved HPV vaccines for use along with any other relevant documents to the Court and the Counsellors for the Petitioners in this case.
  • Learned Counsel for the Union of India shall apprise this Court what steps have been taken to comply with the recommendations put forth in the Parliamentary Committee’s Report on HPV vaccine demonstration projects in India.
  • Counsel for the State shall file their counter-affidavits within a period of four weeks.
  • The Union of India shall file their counter-affidavit (case #921/2013) within four weeks. Rejoinder affidavit, if any, within two weeks therefrom.
  • By the same time, rejoinder affidavit to the counter-affidavit filed by PATH International to be filed.
  • The Advocate for ICMR shall produce the file dealing with HPV vaccines by the next date.
  • Regarding the ’concept of consent’ and the resultant deaths: it has been submitted that though innovative explanations have been given stating that some girls in the States of Gujarat and Telangana expired due to snake bite and fever, in actuality, it is due to the administration of vaccinations.
  • It was noted that though HPV vaccines were administered for the purpose of experimentation, there is no data with regard to the adverse effects faced by the young girls.
  • Counsel for the Union of India, the State of Gujarat, and the State of Telangana shall state by way of affidavit what the procedure and protocols are to be followed while obtaining informed consent. The stand taken by the Union of India and the States shall be clear and in consonance with law, for the affidavit is not expected to be filed in contravention of that has been envisaged in law.
  • The present public interest litigation has to be perceived from the point of view of rectification and caution for the future.
  • The ’caution’ would convey what steps have to be taken in the future so that this kind of grievances do not arise.

In conclusion, the Supreme Court order states:

Learned counsel appearing for the Union of India and the States of Gujarat and Telangana shall file their respective affidavits keeping in view the directions given herein-above. To elucidate, the affidavit filed by the Union of India shall contain explicitly (i) what steps they intend to take on the basis of the report given by the Parliamentary Standing Committee, (ii) what is the procedure to be followed for the purposes of consent and what steps are required to be taken to find out the sufferings, if any, by the persons who were vaccinated, and (iii) the liability of compensation, if any, to be paid and whose liability it would be.

Justices set the next hearing date for April 21, 2015.

 

References:

India: HPV vaccines Gardasil and Cervarix make it to the Supreme Court

India: Supreme Court HPV Vaccine Controversy Continues

Original Supreme Court Documentation, go to this link – http://courtnic.nic.in/supremecourt/casestatus_new/caseno_new_alt.asp then select “Writ Petition (civil)” as the case type; 558 as the case number; and 2012 as the year. Then click submit. Follow links from there to access original documents.

 Continue to the Article Here

This article in it’s entirety is compliments of www.sanevax.org

The FDA Approves a New HPV Vaccine Containing Over Twice as Much Aluminum As its Predecessor#HPV#iBelieve#halftime

You can expect that the FDA has received a lot of correspondence from parents, advocates, physicians, researchers and so forth in regards to the significant injuries following the Gardasil and Cervarix vaccines.  It is stunning that they have once again approved this vaccine and now with even higher amounts of aluminum.  

A clear message that they do not have your best interests in mind.

by Christina England

 According to recent reports, the FDA has approved yet another HPV vaccine, despite documented safety issues and the new vaccine containing an exceptionally high level of aluminum, a known neurotoxin.

Until now, only two vaccines have been manufactured to protect men and women against human papillomavirus (HPV), a virus believed to be the leading cause of cervical cancer: Cervarix, which is believed to protect against strains 16 and 18 of the virus, and Gardasil, which is believed to protect against strains 6, 11, 16 and 18…

Many are skeptical and have begun to question whether or not this vaccine is yet another unsafe, fast-tracked vaccine.

Parents Question Whether or Not They Can Really Trust the FDA’s Claims…

Continue to the Article Here

www.vactruth.com

Related Articles:

My Daughters Life Altering Changes after Gardasil

Warning Gardasil Injuries can have a Permanent Impact

My Gardasil Survivor

HPV Vaccines: SaneVax Message to Columbia

FDA Approved Gardasil 9: Malfeasance or Stupidity

What if HPV does NOT cause cervical cancer?#HPV#HearThisWell#cdcwhistleblower

The title of a paper recently published by McCormack et al in Molecular Cytogenetics says it all, ”Individual karyotypes at the origins of cervical carcinomas.” If the findings in this paper are true, a vaccine against human papillomavirus (HPV) is extremely unlikely to protect against cervical cancer.

According to this paper neither genetic predisposition nor HPV infections are necessary for the development of cervical cancer. All cervical cancer cells investigated during the course of this study contained  new abnormal karyotypes. The clonality (genetic makeup) of these new abnormal karyotypes indicates the cervical cancers originated with these karyotypes – NOT from a virus.

In order to grasp the potential significance of these statements, one must have a basic understanding of karyotypes. Most living things have chromosomes, or units of genetic information, in their cells.  The human-karyogramnumber and appearance of chromosomes varies from one species to another. A karyotype is the number, size, and shape of chromosomes in any given organism.

See the graphic representation of the human karyotype to the right. Every human has 23 pairs of chromosomes (46 total) as illustrated, with the last pair on the bottom right determining the sex of any particular human. Any different number would indicate a different species. For example, apes have 48 chromosomes and kangaroos 20. The number, size and shape of the chromosomes in any given cell reveals the species of origin for that cell.

Cancer-specific karyotypes explained

All cancers have individual clonal (cells descended from and genetically identical to the parent cell) karyotypes (number, size and shape of chromosomes) and thus phenotypes (expressed physical traits).  No two cancers are the same.  See the karyotype arrays in the paper named above and referenced at the end of this article.

The karyotype determines the phenotype via thousands of messenger RNAs (about a thousand per chromosome), which in turn make thousands of proteins – at concentrations (copy numbers) that are cancer karyotype-specific – all cancer cells are individually very different from normal cells. In this respect, cancer cells resemble a new cellular species existing within the human body, much like a parasite.

The genes and proteins within cancer cells are expressed at very abnormal concentrations when compared to the normal cells surrounding them. However, since all genes and proteins expressed within cancer cells originated from human cells, cancers are not immunogenic (able to produce an immune response) – despite their huge biological differences from surrounding normal cells.  This is the reason the immune system cannot “see” cancers.

Since the new carcinoma karyotypes express thousands of normal genes abnormally they generate numerous new cancer-specific phenotypes that correlate one-to-one with the new karyotypes of cancer cells.  Cervical cancer cells are one example.

Think about Down syndrome as a model; one extra small 21 chromosome changes a lot.  Cancers typically have 60-70 chromosome variations compared the 46 +1 of Down syndrome.

The Human Papillomavirus (HPV) Causes Cervical Cancer Hypothesis

This hypothesis states that HPV encodes proteins which cause cancers as the virus replicates.  Having common transforming proteins, all cervical carcinomas would be more or less the same if this were accurate.  Since viral proteins are foreign to humans, viruses, virus-infected cells and possibly virus-transformed tumor cells would inevitably be immunogenic and as such eliminated by the host’s immune system within weeks to months after infection.

This is the reason why HPV-induced warts are eliminated by the immune system within weeks to months after infection.

This hypothesis raises four questions:

  1. Why would only 1 in 10,000 HPV-infected women develop cervical cancer?
  2. Why would cervical cancers only develop 20 to 50 years after infection? – In other words, why would the virus not cause cancers when it is biochemically active and causing warts, namely before it is neutralized by natural anti-viral immunity?
  3. Why are cervical carcinomas individually very distinct from each other in terms of malignancy, drug-resistance, cell histology, as originally described by Papanicolaou et al. in Science in 1952, although they are presumably caused by the same viral proteins?
  4. Why are cervical carcinomas that are presumably generated by Human Papillomavirus proteins not immunogenic and thus not eliminated by natural antibodies?

Despite over 25 years of research on the HPV causes cancer hypothesis, there are no direct answers to these questions.

Instead poorly defined “co-factors” are mentioned as “collaborators” of HPV in the causation of carcinomas.  Poorly defined cellular mutations are mentioned as the causes of the cervical carcinomas of HPV-negative women.

Moreover, about 30% of cervical cancers are virus-free.   In these cases the virus couldn’t even theoretically be responsible for the cancer.

The Karyotypic Speciation Theory of Cervical Cancer Development

The McCormack et al. study, ”Individual karyotypes at the origins of cervical carcinomas” advances the theory that carcinogenesis is a form of speciation (See Duesberg et al., “Is carcinogenesis a form of speciation?” Cell Cycle 2011).

According to this theory karyotypic evolutions generate new cancer species from normal cells after exposure to carcinogens (e.g. cigarette smoke or X-rays) or after spontaneous mitotic accidents. The common function of carcinogens is the induction of aneuploidy (chromosomal disruption, either gains or losses).  By unbalancing thousands of genes aneuploidy automatically destabilizes the normal human cell karyotype and thus catalyzes random karyotypic variations.  Selections of variants with proliferative phenotypes form nonclonal pre-neoplastic hyperplasias (enhanced growth of non-neoplastic cells in a tissue or an organ) with persistently varying karyotypes. Very rare karyotypic variations form autonomous (capable of replicating without influence from surrounding host cells) new cancer species with individual clonal karyotypes.  Cancer karyotypes are stabilized within narrow margins of variation by clonal selections for cancer-specific autonomy.  Since this mechanism is very inefficient, it predicts long latent periods from carcinogen exposures to cancers with individual clonal cancer karyotypes.

In agreement with this theory, the authors discovered new, cancer-specific karyotypes and phenotypes in all cervical carcinomas tested so far – both in HPV-DNA-positive and negative carcinomas.

Furthermore, they discovered the individual karyotypes of each carcinoma correspond 1 to 1 to their individual phenotypes (e.g. invasiveness and resistance to chemotherapeutic drugs).  This is proof-of-principle that these karyotypes determine the phenotypes of cancers – rather than the defective and latent Papilloma-virus DNAs.

According to the karyotypic speciation theory, the defective viral DNAs of “HPV DNA-positive” carcinomas are functionally irrelevant, because they are not expressing any viral proteins.  Instead they are non-immunogenic fossils of long past Papilloma-virus infections.  As such they are no matches for the thousands of cellular genes that are abnormally expressed in cervical carcinomas.

Karyotypic speciation theory explains paradoxes presented by the HPV causes cancer hypothesis

Why would only 1 in 10,000 HPV-infected women develop cervical cancer? 

According to the karyotypic carcinoma theory this discrepancy is the result of the facts that HPV infection and carcinogenesis are two entirely independent events:

  • No specific correlation exists between HPV and cervical carcinoma. HPV is very common, about 70 to 80% endemic in the American population.  The rest of the population is HPV-free.  The virus is typically sexually transmitted at young age.  Since cervical carcinomas occur in both HPV-positive and HPV-negative females, there is no specific correlative evidence that HPV plays any role in causing cervical cancer.
  • There is also no specific functional correlation between HPV-infection and carcinogenesis. As shown from the clonal karyotypes of cervical cancers, cancers originate from a major rearrangement of the karyotypes of normal cells.  Since this is true for cervical carcinomas of HPV-positive and of HPV-negative females – and is indeed true for all cancers – there is no functional evidence that HPV plays a role in the development of carcinomas.  This conclusion is consistent with the fact that carcinomas with new clonal karyotypes arise only 20 to 50 years (!) after infection by HPV, which we discuss next.

Thus there is neither a specific correlation between the presence and/or the functions; or lack of functions of HPV and carcinogenesis.

Why would cervical cancers only develop 20 to 50 years after HPV infection?

The karyotypic cancer theory sheds light on the presumed long latent periods from HPV infection to cancer. This huge latent period suggests evidence of two entirely unrelated events:

  • Infection with a sexually transmitted, benign Human Papillomavirus at young age, and
  • A cervical cancer diagnosis – 90% of which occur over the age of 50

The presumed long latent period could be a result of the low probability of forming a new autonomous cancer species from a normal somatic cell by random karyotypic rearrangements.  The evolution of a new individual species of cells (cervical cancer cells) with the ability to reproduce independent of influence from surrounding human cells by random karyotypic variations of precursor cells takes time.

The very low probability of evolving a new autonomous cancer species by random karyotypic evolution explains not only the long and unpredictable time intervals between HPV infection (if it occurs) and cervical carcinomas, but aso the classical age bias of all cancers.  The age bias of cancer says that over 90% of all cancers only occur at ages over 50 years.

The authors concluded the chronological discrepancies between HPV infection and carcinogenesis exclude a direct mechanism of action connecting viral infection and the development of cancer.   Instead the time-dependent evolution of a new cancer-specific karyotype supports the karyotypic theory of the origin of cervical carcinomas.

Why do cervical carcinomas have individual karyotypes and phenotypes – rather than common phenotypes as predicted by the virus hyothesis?

The probability of forming the karyotype of a new autonomous cancer-species by random karyotype variations is very low and thus unlikely to ever generate the same new species twice – much again as in conventional speciation.  Thus all cancers caused by karyotypic speciation will have individual, if sometimes similar phenotypes.

Why are presumably viral cervical carcinomas not immunogenic and thus not eliminated by natural antibodies?

The karyotypic speciation theory explains why presumably viral cervical carcinomas are not immunogenic and are thus able to grow in HPV-DNA-positive people, which contain anti-HPV antibodies produced as a result of prior infection(s) by the virus.

According to the karyotypic cancer theory, carcinomas are generated de novo from cellular chromosomes, genes and proteins, which are not immunogenic in the host of origin (just like all other cancers).  By contrast, hypothetical cancer cells generated by viral proteins would be immediately eliminated by antiviral immunity.

Since cervical carcinomas have clonal carcinoma-specific karyotypes, we know they were generated via chromosomal rearrangements of thousands of normal cellular genes, which are not immunogenic.

According to the authors, fragments of inert HPV DNA found in 70 to 80% of cervical cancers (and in 70 to 80% of all women in the US!) are left-overs of by-gone infections or warts that occurred 20-50 years prior to carcinogenesis.  Infections and resultant symptoms were eliminated by natural anti-HPV antibodies.

Should the Karyotypic Speciation Theory be proven correct, HPV vaccines could not possibly reduce the incidence of cervical cancer – or any other type of cancer for that matter.

What do we do now?

Until such time as scientists can verify or disprove the Karyotypic Speciation Theory of cervical cancer development, medical comsumers must proceed with caution.

This is a scientific debate which cannot be ignored. Public health authorities and medical professionals must apply the precautionary principal by suspending the use of HPV vaccines and supporting the already proven, safe and effective method of controlling cervical cancer – Pap screening.

It is this method which, after its introduction by George Papanicolaou et al. in Science in 1952, reduced the incidence of cervical cancer in the US from the most common of the 10 most common cancers of women to one that no longer belongs to this list.

Moreover, this proven test for cervical carcinomas, termed Pap screen after Papanicolaou, costs only a small fraction of the $300-500 for the Gardasil and Cervarix vaccines and has NO serious adverse effects.

Immediate independent studies must be conducted to discover which of the theories discussed above is accurate. If HPV does not cause cancer – HPV vaccines are useless.

If HPV vaccines are useless, it is certainly not worth submitting yourself (or your loved ones) to the 2.3 to 2.5% risk of serious adverse reactions AND the 2.4 to 3.3% risk of developing a new medical condition potentially indicative of autoimmune disorders experienced by Merck’s Gardasil 9 clinical trial participants.

ALL RISK AND NO BENEFIT IS NOT A WISE MEDICAL CHOICE UNDER ANY CIRCUMSTANCES.

 

References:

This article in it’s entirety, is compliments of www.SaneVax.org

Judges demand answers after children die in controversial cancer vaccine trial in India#cdcwhistleblower#HearThisWell#Vaccines

There have been over 37,000. adverse events and 214 deaths from the Gardasil/Cervarix vaccines with no evidence of any benefit from the vaccine.  These figures are off of the November 2014 VAERS report and estimated to be only 1-10% of actual cases.  

By GETHIN CHAMBERLAIN IN INDORE, INDIA,

  •  Tribal girls were given shots of cervical cancer vaccines during trial
  • Children given Merck’s Gardasil and Cervarix vaccines
  • Petitioners also asked judges to investigate trials of new drug Gardasil 9
  • Drug has allegedly caused side-effects in children as young as nine
  • Investigation claims children were used as unwitting human guinea pigs
  • Supreme Court has given the government one month to provide answers

Judges in India’s Supreme Court have demanded answers after children died during a controversial cervical cancer vaccine trial.

Young tribal girls received shots of pharmaceutical company Merck’s Gardasil vaccine and Cervarix, manufactured by GlaxoSmithKline.

The vaccines are given to girls as young as nine in many countries – including the UK and the US – to protect against the human papilloma virus, one of the major causes of cervical cancer.

But the Indian court yesterday heard a challenge by campaigners who claim the study – funded by the Bill & Melinda Gates Foundation – failed to obtain the informed consent of the children or their parents.

They say that a ‘study’ carried out for the foundation by a US organisation was in fact an illegal drugs trial.

Continue to the Article Here

http://www.dailymail.co.uk/