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Firstlet’s look at what keeps cancer cells alive, then we will come back and
examine how the cannabinoids CBD (cannabidiol) and THC (tetrahydrocannabinol)
unravels cancer’s aliveness.
In every cell there is a family of interconvertible sphingolipids that specifically
manage the life and death of that cell. This profile of factors is called the
“Sphingolipid Rheostat.” If endogenous ceramide(a signaling metabolite of
sphingosine-1-phosphate) is high, then cell death (apoptosis) is imminent. If
ceramide is low, the cell is strong in its vitality.
Very simply, when THCconnects to the CB1 or CB2 cannabinoid receptor site on
the cancer cell, it causes an increase in ceramide synthesis which drives cell
death. A normal healthy cell does not produce ceramide in the presenceof THC,
thus is not affected by the cannabinoid.
The cancer cell dies, not becauseof cytotoxic chemicals, but becauseof a tiny
little shiftin the mitochondria. Within mostcells there is a cell nucleus, numerous
mitochondria (hundreds to thousands), and various other organelles in the
cytoplasm. The purposeof the mitochondria is to produceenergy (ATP) for cell
use. As ceramide starts to accumulate, turning up the Sphingolipid Rheostat, it
increases the mitochondrial membrane pore permeability to cytochromec, a
critical protein in energy synthesis. Cytochromec is pushed out of the
mitochondria, killing the sourceof energy for the cell.
Ceramide also causes genotoxic stress in the cancer cell nucleus generating a
protein called p53, whosejob it is to disrupt calcium metabolism in the
mitochondria. If this weren’tenough, ceramide disrupts the cellular lysosome, the
cell’s digestive systemthat provides nutrients for all cell functions. Ceramide, and
other sphingolipids, actively inhibit pro-survivalpathwaysin the cell leaving no
possibility at all of cancer cell survival.
The key to this process is the accumulation of ceramide in the system. This means
taking therapeutic amounts of CBD and THC, steadily, over a period of time,
keeping metabolic pressureon this cancer cell death pathway.
How did this pathway come to be? Why is it that the body can take a simple plant
enzymeand use it for profound healing in many different physiologicalsystems?
This endocannabinoid systemexists in all animal life, justwaiting for its matched
exocannabinoid activator. This is interesting. Our own endocannabinoid system
covers all cells and nerves; it is the messenger of information flowing between our
immune systemand the central nervous system(CNS). Itis responsiblefor
neuroprotection, and micro-manages the immune system. This is the primary
control systemthat maintains homeostasis; our well being.
Just out of curiosity, how does the work get done at the cellular level, and where
does the body make the endocannabinoids? Herewe see that endocannabinoids
have their origin in nerve cells right at the synapse. When the body is
compromised through illness or injury it calls insistently to the endocannabinoid
systemand directs the immune systemto bring healing. If thesehomeostatic
systems areweakened, it should be no surprisethat exocannabinoids are
therapeutic. Ithelps the body in the mostnatural way possible.
To see how this works wevisualizethe cannabinoid as a three dimensional
molecule, whereone part of the molecule is configured to fit the nerve or
immune cell receptor site justlike a key in a lock. There are at least two types of
cannabinoid receptor sites, CB1 (CNS) and CB2 (immune). In general CB1 activates
the CNS messaging system, and CB2 activates the immune system, butit’s much
more complex than this. Both THC and anandamide activate both receptor sites.
Other cannabinoids activate one or the other receptor sites. Among the strains of
Cannabis, C. sativa tends toward the CB1 receptor, and C. indica tends toward
CB2. So sativa is more neuroactive, and indica is more immunoactive. Another
factor here is that sativa is dominated by THC cannabinoids, and indica is
predominately CBD (cannabidiol).
Itis known that THC and CBD are biomimetic to anandamide, that is, the body can
use both interchangeably. Thus, when stress, injury, or illness demand more from
endogenous anandamide than can be produced by the body, its mimetic
exocannabinoids are activated. If the stress is transitory, then the treatment can
be transitory. If the demand is sustained, such as in cancer, then treatment needs
to provide sustained pressureof the modulating agent on the homeostatic
systems.
Typically CBD gravitates to the densely packed CB2 receptors in the spleen, home
to the body’s immunesystem. Fromthere, immune cells seek out and destroy
cancer cells. Interestingly, ithas been shown that THC and CBD cannabinoids have
the ability to kill cancer cells directly without going through immune
intermediaries. THC and CBD hijack the lipoxygenasepathway to directly inhibit
tumor growth. As a sidenote, it has been discovered that CBD inhibits
anandamide reuptake. Here we see that cannabidiol helps the body preserveits
own natural endocannabinoid by inhibiting the enzymethat breaks down
anandamide.
This brief survey touches lightly on a few essential concepts. Mostly I would like
to leave you with an appreciation that nature has designed the perfect medicine
that fits exactly with our own immune systemof receptors and signaling
metabolites to providerapid and complete immune responsefor systemic
integrity and metabolic homeostasis. -

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  • 1. Firstlet’s look at what keeps cancer cells alive, then we will come back and examine how the cannabinoids CBD (cannabidiol) and THC (tetrahydrocannabinol) unravels cancer’s aliveness. In every cell there is a family of interconvertible sphingolipids that specifically manage the life and death of that cell. This profile of factors is called the “Sphingolipid Rheostat.” If endogenous ceramide(a signaling metabolite of sphingosine-1-phosphate) is high, then cell death (apoptosis) is imminent. If ceramide is low, the cell is strong in its vitality. Very simply, when THCconnects to the CB1 or CB2 cannabinoid receptor site on the cancer cell, it causes an increase in ceramide synthesis which drives cell death. A normal healthy cell does not produce ceramide in the presenceof THC, thus is not affected by the cannabinoid. The cancer cell dies, not becauseof cytotoxic chemicals, but becauseof a tiny little shiftin the mitochondria. Within mostcells there is a cell nucleus, numerous mitochondria (hundreds to thousands), and various other organelles in the cytoplasm. The purposeof the mitochondria is to produceenergy (ATP) for cell use. As ceramide starts to accumulate, turning up the Sphingolipid Rheostat, it increases the mitochondrial membrane pore permeability to cytochromec, a critical protein in energy synthesis. Cytochromec is pushed out of the mitochondria, killing the sourceof energy for the cell. Ceramide also causes genotoxic stress in the cancer cell nucleus generating a protein called p53, whosejob it is to disrupt calcium metabolism in the mitochondria. If this weren’tenough, ceramide disrupts the cellular lysosome, the cell’s digestive systemthat provides nutrients for all cell functions. Ceramide, and other sphingolipids, actively inhibit pro-survivalpathwaysin the cell leaving no possibility at all of cancer cell survival. The key to this process is the accumulation of ceramide in the system. This means taking therapeutic amounts of CBD and THC, steadily, over a period of time, keeping metabolic pressureon this cancer cell death pathway.
  • 2. How did this pathway come to be? Why is it that the body can take a simple plant enzymeand use it for profound healing in many different physiologicalsystems? This endocannabinoid systemexists in all animal life, justwaiting for its matched exocannabinoid activator. This is interesting. Our own endocannabinoid system covers all cells and nerves; it is the messenger of information flowing between our immune systemand the central nervous system(CNS). Itis responsiblefor neuroprotection, and micro-manages the immune system. This is the primary control systemthat maintains homeostasis; our well being. Just out of curiosity, how does the work get done at the cellular level, and where does the body make the endocannabinoids? Herewe see that endocannabinoids have their origin in nerve cells right at the synapse. When the body is compromised through illness or injury it calls insistently to the endocannabinoid systemand directs the immune systemto bring healing. If thesehomeostatic systems areweakened, it should be no surprisethat exocannabinoids are therapeutic. Ithelps the body in the mostnatural way possible. To see how this works wevisualizethe cannabinoid as a three dimensional molecule, whereone part of the molecule is configured to fit the nerve or immune cell receptor site justlike a key in a lock. There are at least two types of cannabinoid receptor sites, CB1 (CNS) and CB2 (immune). In general CB1 activates the CNS messaging system, and CB2 activates the immune system, butit’s much more complex than this. Both THC and anandamide activate both receptor sites. Other cannabinoids activate one or the other receptor sites. Among the strains of Cannabis, C. sativa tends toward the CB1 receptor, and C. indica tends toward CB2. So sativa is more neuroactive, and indica is more immunoactive. Another factor here is that sativa is dominated by THC cannabinoids, and indica is predominately CBD (cannabidiol). Itis known that THC and CBD are biomimetic to anandamide, that is, the body can use both interchangeably. Thus, when stress, injury, or illness demand more from endogenous anandamide than can be produced by the body, its mimetic exocannabinoids are activated. If the stress is transitory, then the treatment can be transitory. If the demand is sustained, such as in cancer, then treatment needs
  • 3. to provide sustained pressureof the modulating agent on the homeostatic systems. Typically CBD gravitates to the densely packed CB2 receptors in the spleen, home to the body’s immunesystem. Fromthere, immune cells seek out and destroy cancer cells. Interestingly, ithas been shown that THC and CBD cannabinoids have the ability to kill cancer cells directly without going through immune intermediaries. THC and CBD hijack the lipoxygenasepathway to directly inhibit tumor growth. As a sidenote, it has been discovered that CBD inhibits anandamide reuptake. Here we see that cannabidiol helps the body preserveits own natural endocannabinoid by inhibiting the enzymethat breaks down anandamide. This brief survey touches lightly on a few essential concepts. Mostly I would like to leave you with an appreciation that nature has designed the perfect medicine that fits exactly with our own immune systemof receptors and signaling metabolites to providerapid and complete immune responsefor systemic integrity and metabolic homeostasis. -