The 37 Genes And Their 1098 Protein Products...the 100 Hz Fat Burn

The 50 Hz field affect the calcium uniporter that all mitochondria have except fungi.

When a mitochondria uptakes calcium into the matrix guess what is signaled?

The TCA cycle.

This is why Dr. Nora Volkow research has shown the nnEMF is associated
with up regulation of AMPK and glucose metabolism = Otto Warburg.

The reason is simple. nnEMF blocks the ability to fat burn via beta oxidation
because the oscillation of 100 Hz is the key to this ability not the FOOD you eat.

The seminal work on the calcium uniporter was done by researcher Vamsi Mootha.

Google his youtube presentations.

To understand mitochondria you have to understand the 37 genes
and their 1098 protein products.

13 of these proteins are key to making the cytochrome proteins that control electron tunneling
and the ability to make energy in a cell.

Complex cells need to fat burn to make enough energy to support their physiology
but simple cells like bacteria and Archea do not and they rely on glucose metabolism.

Bacteria and Archea divide fast naturally and complex eukaryotes do not.

The ability to fat burn is the BRAKING mechanism on unfettered mitosis
that is associated with oncogenesis.

The essence of understanding the Warburg effect is relaizing fat burning
and beta oxidation stop uncontrolled cell division.

To date we know there is 1098 proteins from the 37 genes
but we only have proteomics data in 300-400 of these proteins.

This means we don't know enough about mitochondria yet.

This is why I tell people to read Dr. Doug Wallace and Jodi Nunnari's work.

You must begin to look at this work to get well.

It appears a metazoan protein called "Emre" links MICU1 to MICU 2 mitochondrial proteins
to make the MCU pore through which mitochondrial permeability becomes a deep problem
with electric and magnetic fields.

It also appears that blue light affects the uniporter too.

When you dive deeper you begin to learn more than the food guru's. Information
is buried in the free radical signals that mitochondria create and use to direct
the structure of cells and tissues.

All ROS and RNS are free radical signals all born in mitochondria. People seem to forget this very fundamental tenet. This implies that tissue level diseases can result SOLELY from global energy deficits WITHOUT any GENOMIC change. It also implies that non-Mendelian genetics that is prevalent in mitochondrial DNA directly controls nuclear DNA expression via the epigenome.

This is a huge paradigm shift in medicine because our entire intellectual library
in medicine is being attacked by this new data from bio-energenics of mitochondria.

Nick Lane and Doug Wallace are leading this charge on both sides of the Atlantic
while clinicians do not even know who these guys are.

This is the data missing in the vaccine and autism debate.

Our current constructs in medicine only reflects what we do believe to be true,
but it lacks the insights to even ask the question what is it, that we do not know,
or what we don't know that we don't know, that might be behind modern diseases?

This question is rarely entertained because we focus solely on beliefs
WE THINK are true and mighty today.

What if all that we believe is based upon a house of cards?

IF you read my page enough you know it is a house of cards.

This is an unsettling idea to most, but when you understand that a neuro-hormone like
melatonin controls mitochondrial DNA, you begin to see why light and its absence at night
is the most important thing for proper bio-energetics to occur in mitochondria.

This is the primary mitochondrial insult that is causing children to be born to women
already with high heteroplasmy rates.

The children are already in deep trouble before they ever get a vaccine or an antibiotic.

Be sure though those "STIMULI" are gasoline on the fire burning in those kids mitochondria.

The corollary to this concept, is that light would then be seen to exert massive control
over the expression of nuclear genes leading to many disease phenotypes.

That has been what the basic science blueprint has foreshadowed for 100 years now,
and medicine is CLUELESS about it because of HOW we FUND RESEARCH
because of BIG PHARMA influence $$$$$.

Our public problem is that our scientists and clinicians cannot fathom this just yet
because of the germ theory of man and drug therapy mindset of healthcare.

As a result, the public's health is in a catastrophic state on many fronts,
as my page threads show today, because our research and clinical focus is off the mark.

This lack of focus is brought into sharp focus by modern mitochondrial science and bio-physics.

They have both been pointing to this inconvenient truth for 100 years, but the powers in biology,
instead, have been mesmerized by the 1953 discovery of DNA and the ancient practice
of anatomical dissection (Vesalius) to gain reductive insights about life and food macro's.

This is a bad way to view the modern world. Read some of Lane's old work to gain a new insight.

Ponder this before you rest your head so melatonin can work in your mitochondria
to help you learn new things.

Ted Fish
windows, glasses, are blockers of light
- we are children of light
YOU ARE LIGHT!
1Th_5:5 Ye are all the children of light,
and the children of the day:
we are not of the night,
nor of darkness.


A critical approach to the therapy of mitochondrial respiratory chain and oxidative phosphorylation diseases - ScienceDirect
https://www.sciencedirect.com/scien...vPlVaMBf_WgmD5C33uaFS3SEZxFapTUQYeKpmqICAHfhI

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  A critical approach to the therapy of mitochondrial respiratory chain and oxidative phosphorylation diseases
  https://www.sciencedirect.com/scien...nrniDI39zdU4cst9oo7Z1AaUWhvVA1Yh5j8IdGWCaDqio
  
  
• 
  
  A critical approach to the therapy of mitochondrial respiratory chain and oxidative phosphorylation diseases
  https://www.sciencedirect.com/scien...vPlVaMBf_WgmD5C33uaFS3SEZxFapTUQYeKpmqICAHfhI
  
  
  

 

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