Yes, the case is strong. I'll post here a synthesis of what has been discussed for the last few years.
“Junk” DNA includes a whole subset of names such as introns, retrotransposable elements, and non-coding RNAs (ncRNAs). In fact, ncRNAs are often located near genes known to be important to both stem cells and cancer, to serve as enhancer elements which promote their gene expression. Stem cells are the cells that have the potential to turn into lots of other cells. So this junk DNA can influence how stem cells specifically differentiate into multiple cell types and in this sense it is now estimated that 80% of our genome is biologically active with only 1% of our genome encoding for proteins:
_http://www.medicalnewstoday.com/articles/250006.php
A staggering batch of over 30 papers published in Nature, Science, and other journals this month, firmly rejects the idea that, apart from the 1% of the human genome that codes for proteins, most of our DNA is "junk" that has accumulated over time like some evolutionary flotsam and jetsam.
The papers, representing 10 years of work of the ENCODE ("Encyclopedia of DNA Elements") project, completed by hundreds of scientists from dozens of labs around the world, reveal that 80% of the human genome serves some purpose and is biochemically active, for example, in regulating the expression of genes situated nearby.
That was known for some time, but it is now official since the last couple of weeks or so.
Evolutionary speaking, it makes a lot of sense… From the information posted in this session:
http://cassiopaea.org/forum/index.php/topic,27027.msg330775.html#msg330775 , we learned that the greatest shocks of genomic science was to find that the human genome contains more viral than "human" genes. That is, the human genome is made from thousands of viruses that infected our distant ancestors. They got there by infecting eggs or sperm, inserting their own DNA into ours. Hyperdimensional engineering...
Most of the genetic diversity can be found in virus genes. Scientists agree that there are some 1,000,000,000,000,000,000,000,000,000,000 viruses in the ocean and it matches almost nothing to any gene from any microbe, animal, plant or other organism, even from any other known virus.
All living things have hundreds or thousands of genes imported by viruses. There are a group of viral species known as retroviruses which insert their genetic material into the host cell’s DNA. When the host cell divides, it copies the virus’s DNA along with its own. Retroviruses have “on switches” that prompt their host cell to make proteins out of nearby genes. Sometimes their switches turn on host genes that ought to be kept shut off, and cancer can result. This is precisely what our junk DNA –ncRNA- seems to be doing “next” to genes that have to do with stem cells and cancer cells.
What is known as endogenous retrovirus – endogenous meaning generated within, are the viruses that lurk in the genomes of just about every major group of vertebrates, from fish to reptiles to mammals. Virologists have found retrovirus-like segments in our human genome and they were able to track its genetic code down to an original functioning virus. The virus was called Phoenix, for the mythical bird that rose from its own ashes.
It is known that part of our junk DNA, the retrotransposable elements, are viral in its origin. It includes the endogenous retroviruses. But it is now argued that ncRNA might be viral in its origin as well. This has interesting implications in the sense that
epigenetic control of gene expression involves this junk DNA – ncRNAs. It would mean that our entire junk DNA (98%) might well be very functional epigenetically speaking, and in the induction of regulatory genes that code for stem cells, or for reprogramming o modulating genes known to response to oxidative stress, DNA damage and p53 – a protein that regulates the cell cycle and is implicated in about half of all human cancers.
Evil lectins from carbs can initiate a cascade of events once they attach to the cell “mem-brain” that may lead to attraction of the immune system, cell death, production of chemicals, multiplication of the cell and so forth. It depends. And it might well depend on the adaptation response from the viral-like properties inside the cell, our “junk” DNA.
Harmful lectins - such as the ones found in gluten, soy, dairy, corn – cause inflammation and damage without a defense/immune response which end up being secondary to the initial damage. Some response in quite a drastic way (i.e. autoimmune diseases) others respond in a milder way, constituting thus the wide nature of symptoms among people.
Moreover, wheat’s evil lectin (WGA) and viruses share similar properties. For instance, when the influenza virus incorporates its own genetic material into our cells, the defense/immune system must attack its own virally transformed cell in order to fight the infection. WGA has access to our bodies and to our cells “mem-brain’s” through viral ports. Then they influence gene expression and trigger autoimmune attacks like viruses do. As John B. Symes, D.V.M. pointed out back in 2007 :
http://dogtorj.com/main-course/viruses-friend-or-foe/viruses-and-lectins/
Our medical histories all line up with this once the role (and ultimate purpose) of viruses in nature and our bodies is grasped. They are not the malicious entities that we have labeled them to be. They are simply doing their job. The noxious stimuli being thrown at them is the real issue. We are literally forcing them into becoming pathogens. In addition to the plethora of obvious offending agents being imbibed, most individuals are compounding matters through poor nutrition, polluted environments, fast-paced lifestyles, and lack of sleep. All of these things add up to self-induced misery. [...]
I have suggested many times that, when reading a paper of genetics, the word “gene” be replaced with the word “virus” to see if that treatise makes more sense. Suddenly, answers to the above questions start coming. Coupled with the knowledge of viral stimulants (e.g. carcinogens, lectins, and other viruses), we can start to see what…or who…the real culprit is.
Mutations in ncRNA are associated with cancer, autism, and Alzheimer’s disease AND ncRNA can sense a viral infection within the cell, giving off signals that indicate the pathogenic virus presence.
An endogenous retrovirus has also been associated with multiple sclerosis, meaning that viral genes that are part of our genome can be “woken up”. As the authors of
this study say, "retroviral infections often develop into running battles between the immune system and virus, with the virus mutating repeatedly to avoid the immune system, and the immune system repeatedly catching up. One can see the episodic nature of multiple sclerosis as such a running battle."
It is crucial to understand that what we eat is information the effect epigenetic changes that regulate gene expression, and that can be passed from generation to generation.
Also, the one thing that may be contributing to mitochondrial dysfunction is latent viral infections such as the ones of the herpes family. That plus, our toxic food and environment makes a very bad combination.
Herpes simplex virus is a widespread human pathogen and it goes right after our mitochondrial DNA. A latent viral infection might be driving the brain cell loss in neurodegenerative diseases such as Alzheimer's disease. Members of the herpes virus family, including cytomegalovirus and Epstein-Barr virus which are most have, can go after our mitochondrial DNA, causing neurodegenerative diseases by mitochondrial dysfunction. But a ketogenic diet is the one thing that would help stabilize mDNA since mitochondria runs the best on fat fuel. As it happens, Alzheimer's disease is the one condition where a ketogenic diet has a profound positive effect.
Our mitochondrial energetic sources are essential if we are to heal from chronic ailments and we need to stabilize our "viral" genome so that epigenetic changes can be unlocked in a beneficial way.
It is our mitochondria the one that lies at the interface between the fuel from foods that come from our environment and our bodies’ energy demands. And it is a metabolism based on fat fuel, a ketone metabolism, the one which signals epigenetic changes that maximizes energetic output within our mitochondria and help us heal.
A ketogenic diet promotes the die-off of pathogenic viruses through autophagy. It seems to be the key to stabilize our junk DNA ("viral" DNA) and activate it in a positive way.