John P. Cleary, M.D.
Introduction
In diabetes, glucose metabolism via the Krebs cycle is impaired,
and this leads to reduced cellular energy and elevated blood sugar
levels. When a cell is damaged by oxidation injury, cytosol NAD
levels fall and ATP levels decrease, If the DNA strand breaks
can be repaired, and the cell regains lost NAD, the energy system
can function again, but frequently cell death ensues- Experimental
diabetes is caused by this same mechanism, except that a chemical
alkylating agent is used to cause the DNA strand breaks in the
cell nuclei. DNA strand breaks activate the enzyme poly ADP-ribose
synthetase which cleaves NAD, and cause NAD levels in the cytosol
to fall to zero. Schaufstetter (1985) has shown that oxidation
injury can act in the same manner with the same resultant low
NAD in the cytosol and low ATP
Antioxidant Defenses Affect Energy Production
The recent work on oxidant injury to cells, by Schaufstetter et
al (1985), (1986), Spragg (1985), and Wohaieb (1987), has provided
us with insight into the potential cause of most cases of diabetes,
as well as many other diseases formerly classified as being of
unknown etiology. Superoxides and peroxides are produced by the
mitochondria in the course of normal oxidation of nutrient molecules.
There is an antioxidant defense system which consists of superoxide
dismutase and catalase enzymes, ascorbic acid, vitamin E, glutathione,
beta carotene and the coenzymes NAD and NADP, that can deal with
oxygen radicals and prevent damage to the cell structures. When
the oxygen radicals are greater than the ability of the antioxidant
system to deactivate them, then there is oxidation injury.
Experimental oxidation injury was induced by Schaufstetter in
leukocytes with varying concentrations of peroxide which acted
as an oxidizing agent causing DNA strand breaks in the nuclei.
This caused activation of the enzyme poly(ADP-ribose) synthetase
which cleaves NAD, causing NAD and ATP levels to fall. Schaufstetter
measured an 80% fall in NAD levels in 20 minutes, in the cells,
after a dose of peroxide was O.1 to 2.5mM- Mitochondrial oxidation
is then stopped by the cytosol NAD levels being reduced to zero-
Repair of the DNA strand breaks proceeds while the cell is functioning,
but using an alternate energy pathway. Specialized cell functions
cease during this repair phase due to low ATP levels. If the repair
is completed properly the cell must acquire new NAD in the cytosol
to return to the mitochondrial oxidation which generates the majority
of the ATP in eukaryotic cells. If the NAD in the cytosol cannot
be restored or if they are oxidation damaged, the mitochondrial
membranes are not repaired, the cell remains in a low energy mode
of function that prevents specialized cell function necessary
for normal organ function- Thus organ failure is the result of
energy failure on a cellular level, because of oxidation damage
of the mitochondrial membranes and/or low NAD- In the case of
the beta cell in the pancreas this means that proinsulin production
ceases until NAD levels in the cytosol are restored. Giving niacin,
vitamin B3 provides a precursor for NAD
Robbins et al (1980) found superoxide dismutase l05 ug administered
50 minutes prior to 45 mg/kg STZ prevented the diabetogenic effect
that is seen when STZ alone is given. Superoxide dismutase is
an enzyme known to be part of the antioxidant defense system of
the cell, and a scavenger of free radicals, (Oberley 1986). Robbins
believes that the mechanism of action is the inactivation of free
radicals that are generated by STZ, before damage can be done
to DNA- This would prevent activation of poly (ADP-ribose) synthetase
and inactivation of mitochondria which prevents decline in ATP
and cessation of insulin production by the beta cells
Membrane Transport of Glucose and Sodium Impaired by Low ATP
When the cell reaches low ATP levels, the sodium pump is impaired
(Greene 1987)- Boquist (1988) shows that when the Krebs cycle
is inhibited, the Mitochondria swell up. This has an adverse effect
on the membrane transport of glucose, because glucose and sodium
are transported into the cell together. Then the sodium ion must
be pumped out via the NA+K+ ATPase or sodium pump. Sodium transport
requires ATP energy, thus membrane transport of glucose indirectly
uses ATP.
Early observations by S, Soskin and R. Levine, as discussed by
Lehninger (l975) showed that the peripheral tissue of diabetic
animals are deficient in removal of hexose, (a 6 carbon sugar)
from the blood. This happened when the animals were tested at
normal blood sugar levels. If blood sugar is raised to fi00 mgm%
the hexose uptake by tissues is increased, This indicates that
the basic defect in diabetes is membrane transport of glucose
into the cell- M. B. Davidson (1986) discusses the pathogenesis
of the type II Diabetes Mellitus where there is often normal insulin
levels or even an excess of insulin and elevated blood sugar.
Insulin deficiency is not the cause of type 2 diabetes mellitus.
Diabetes is primarily an impairment of membrane transport of glucose,
causing a deficiency of glucose inside the cell and an elevated
level of glucose outside the cell.
In a study done with Etomoxir (Sandoz) used with and without Nicotinic
Acid, FFA levels and triglyceride levels go up in rat plasma when
Nicotinic Acid is not included. When Etomoxir is used with Nicotinic
Acid, glucose levels go down, FFA levels go down and triglyceride
levels go down- This study, (Reaven 1988) shows that NAD is needed
to reestablish the metabolism. Insulin levels did not change during
any stage of the experiment. Reaven's study created an animal
model of adult onset diabetes by using older adult rats and low
dose STZ treatment. They were able to lower blood sugar, FFA and
triglyceride levels to normal using boll) Nicotinic Acid and Etomoxir,
four hours after administering them both by gastric tube or injection
SQ, However, when Etomoxir was administered alone, the FFA and
triglyceride levels both went up considerably, although blood
sugar levels went down to normal levels. Nicotinic Acid administered
alone caused the FFA levels to return to normal, and triglyceride
levels to normal, but blood sugar was still somewhat elevated.
I feel prolonged use would lower blood sugar to normal, as this
has been my experience with Nicotinic Acid, just lowering blood
sugar will not cure diabetes and elevated FFA levels and triglyceride
levels, I believe, are symptoms of impaired cell metabolism. In
addition there is in the diabetic enhanced gluconeogenesis, which
is the formation of glucose in the liver from amino acids
The body is metabolizing protein to make glucose. Most of this
glucose ends up excreted in the urine and leads to the wasting
seen in diabetics. At the same time there is an almost complete
cessation of conversion of glucose to fatty acids via acetyl-CoA.
Normal animals convert about l/3 of ingested carbohydrate to fat-
The combination of excessive gluconeogenesis with absent fatty
acid formation leads to body wasting. Very little metabolism of
glucose for energy production occurs in the diabetic. What does
occur is mostly in the brain, which can use only glucose and in
emergency the kettle body beta hydroxybutarate can be used to
make energy.
Elevated blood glucose is therefore due to impaired membrane transport
of glucose into cells and into the mitochondria of the cells where
it is metabolized into energy, Impaired transport could lead to
further deficient energy levels inside the cell. We know that
in artificially induced diabetes, cytosol NAD levels become zero
preventing normal metabolism by the oxidative pathways involving
the citric acid cycle inside the mitochondria. When alternate
energy pathways are activated including the hexose monophosphate
shunt and fermentation,
of glucose to lactic acid. These path. ways are located in the
Cytosol Of the cell and do not use the mitochondria. The hexose
monophosphate shunt requires NADP as a coenzyme and this substance
is not split by the poly (ADP-ribose) synthetase enzyme.
The Non-Obese Diabetic Mouse Model
Nakajima, H., and Yamada, K., et al, have documented that when
the NOD mice become spontaneously diabetic they also develop antibodies
to the beta cells ~1986). (Perhaps the body does this in an effort
to remove the damaged beta cells from the pancreas-) These researchers
also show that this antibody dependent cell-mediated cytotoxicity
can be stopped with nicotinamide (1986). Yamada, K., et al, had
previously shown (l982) that the nicotinamide inhibits the poly-ADP-ribosylation,
a reaction which depletes NAD levels, and which in the beta cells
can result in no insulin production and even beta cell death
A Single Metabolic Defect is the Cause of All Complications Seen
in Diabetes
Dr. Albert Winegrad in the 1986 Banting Lecture on diabetes, (Diabetes,
Vol- 36, March 1986) attempts to show how a single mechanism,
the activated Polyol pathway, can cause all the complications
seen in all types of diabetes- His whole concept is that a defect
in the metabolism leads to activation of this abnormal metabolism,
however the low NAD levels in diabetes (Spies l939) allows a more
complete explanation in regard to the Polyol pathway defect, since
the pathway depends upon an excess of NADPH being present. This
was demonstrated by the Russian researcher Obrosova, (l985) Nicotinamide
given in experimental STZ diabetes in rats corrected the sorbitol
pathway defect. The nicotinamide induced an increase in NAD+/NADH
and NADP+/NADPH ratios which was accompanied by a decrease in
sorbitol formation. There was inhibition of the aldose reductase
which leads to sorbitol formation and an increase in the sorbitol
dehydrogenase reaction which metabolizes sorbitol to fructose.
Yeh et al (1987) also suggests that sorbinil does not correct
the sodium pump defect in diabetic rats by raising the myo-inositol.
It is however interesting to follow the path to the sorbitol buildup.
Excess hydrogen ion accumulates in the cytosol causing NAD and
NADP to be reduced to NADPH-H+ and NADH-H+. There would be reduction
in ATP production and a fall in pH in the available NAD or NADP.
This would keep NAD and NADP at low to non-existent levels, Energy
production in the cell then switches to the hexose monophosphate
pathway which operates in the cytosol and uses NADPH. I hypothesize
that the excess NADPH also drives the Aldose Reductase enzyme
to make sorbitol, but does not go on to make fructose because
of the NAD deficiency. Sorbitol accumulates in the cells and serves
as a means of reducing the excess H+ ion,
Dr. Wingrad does not address the problem of the impairment of
NA+K+ATPase which leads to impaired glucose transport. Glucose
is transported with Na+ ion into the cell, then Na+ must be transported
back across the membrane by the sodium potassium ATPase. In a
sense the movement of Na+ provides the source of energy to move
glucose and impairment of sodium transport impairs glucose transport.
Insulin alone does not correct impaired membrane transport of
glucose, as is seen in adult onset diabetes there is often high
or normal insulin levels and still elevated blood glucose from
impaired membrane transport of glucose.
NAD Deficiency is the Other Half of the Story in Diabetes
Because insulin was discovered in l922 and niacin in l937, no
one realized the importance of NAD deficiency in diabetes, even
though a small group headed by Tom Spies in l939 published their
study of low NAD levels in diabetics. Controlling blood sugar
will not prevent the progress of the disease diabetes since it
is really a subclinical form of pellagra. Wahlberg (1985) showed
that nicotinamide has a protective effect against nephropathy
in diabetic rats. If 20% of patients with type 1 diabetes of more
than 26 years duration do not develop clinical microangiopathy
even though their blood sugar may not have been optimal, it means
that long term complications in diabetes are not only related
to high blood sugar concentration, but also to other metabolic
disturbances- When nicotinamide was given to rats with STZ diabetes
of 6 months duration there was a lowering of blood sugar and a
decrease in nephropathy as measured IgG immunofluorescent staining
of the glomeruli. They found a deficiency of oxidized pyridine
nucleotides (NAD+NADP+) which could account for the metabolic
impairment of diabetes,
These discoveries should lay to rest any attempts to use aldose
reductase inhibitors to block sorbitol synthesis- When a vitamin
will correct the metabolic defect, why resort to a drug which
can only create more side effects and complications? Any aldose
reductase inhibitors now under development must prove they are
more effective than nicotinamide or nicotinic acid to warrant
their use
Spies, Sydenstricker (1939), Vilter (l939) found diabetics to
suffer from extremely low NAD levels. Early researchers such as
Evans (l939), Sutton (1940) and Spies (l939) had extensive experience
with the many subtle symptoms of pellagra. But a lapse of niacin
research during and after World War 11 gave the pharmaceutical
companies a voice of unquestioned authority over the new practicing
clinicians who had no real experience with niacin deficiency cases
and had not lived through events of the Pellagra years in the
South, indeed did not recognize the symptoms of pellagra. I discuss
this disease in my recent publication on the NAD Deficiency Diseases,
wherein I describe the subclinical pellagras (Cleary 1986), and
their response to the administration of niacin
There was a further study of diabetes niacin therapy done in England
in l943 (Neuwahl) using niacinamide. Incipient cases of diabetes
could often be removed from insulin and could actually be cured
of diabetes, according to Neuwahl, and some long standing cases
had improvement with a lowering of the insulin requirement. Since
niacin could not be patented to make a large profit, I believe
the then aggressive marketing of the stilfonylurea compounds by
the drug companies also tended to obscure the pursuit of the true
cause and treatment of diabetes.
A New Look at the Problem
In 198 1 Japanese biochemists studying artificial diabetes in
lab animals using the alkylating agents alloxan and streptozotocin
found that an enzyme in the cell was activated by single strand
breaks of DNA (Yamamoto 198l). This enzyme, poly (ADP-ribose)
synthetase split the NAD in the cytosol reducing NAD cytosol to
zero and thus inactivating the citric acid cycle energy production
of the mitochondria. Pancreatic beta cells, with no NAD and inactive
mitochondria stopped functioning, insulin was not produced, and
the diabetic condition induced. Further experiments by this group
in Japan showed that pretreating the rats with niacinamide, zinc,
picolinic acid or benzamide before giving the alkylating agent
would prevent the development of diabetes. The outcome depended
on whether the pancreatic cells could repair the single strand
breaks in the DNA and then obtain new NAD resume insulin production,
or whether, the cells were seriously damaged or unable to build
up cytosol NAD levels necessary to resume function.
Spies (l939) found that diabetics in ketoacidosis had NAD levels
as low as pellagrins, and this leads to impairment of the normal
oxidative pathways like the Krebs cycle. In other words, they
had pellagra and this is the real cause of ketoacidosis.
How the Heart and Vascular Complications Result from the Impaired
Cellular Energy of Pellagra by Oxygen Injury
Accelerated atherosclerosis is a facet of the diabetic disease
progression; it changes the blood vessels of the entire body,
and combined with the impairments of the immune system, this vascular
restriction leads to tissue breakdown and gangrene. Jackson (l985)
estimates that 80% of diabetic deaths are from vascular disease
secondary to the abnormal metabolism found in diabetes.
Hypertension as a cause of some of the pathology of diabetes is
also demonstrated by Hommel et al (1986). They show that acute
reduction of arterial blood pressure reduces urinary albumin excretion
in type 1 diabetic patients with incipient nephropathy, They demonstrate
this same result in human insulin dependent diabetic, upon whom
Clonidine was used to reduce arterial blood pressure and there
was a decrease in urinary albumin excretion
Roberto Zarz, et al, in discussing the prevention of diabetic
glomerulophathy by pharmacological amelioration of glomerular
capillary hypertension (1986), also indicate this- Experimental
diabetes in rats demonstrate that kidney damage associated with
diabetes can be prevented by lowering blood pressure and especially
glomerular capillary pressure. Apparently in diabetes there is
increased blood pressure to kidney capillaries with increases
in blood filtration in the glomerulus. This results in loss of
albumin in the urine and destruction of glomeruli. Blood pressure
in the rats in this study was lowered by angiotensin I converting
enzyme inhibitor called endaprin. Kidney damage is prevented by
reducing glomerular hypertension. The albuminuria was also prevented
by lowering the glomerular pressure- When niacin is given to hypertensives
the blood pressure is gradually reduced, as in my case number
2 discussed below, to normal, and the mechanism of action is believed
to involve the improved action of the sodium pump that results
from providing adequate ATP levels to the cells. This same mechanism
would be involved in correcting the hypertension of diabetics
and thus preventing renal damage and albuminuria
Myocardiopathy is Due to Low ATP
In diabetic rats low ATP levels have been found in the myocardium
(Jenkins et at 1986), (Jackson l985) and this could account for
the myocardiopathy seen in diabetes. The low ATP levels in cardiac
tissue provides us with insight into the basic problems in diabetes
which is impaired energy production leading to organ failure,
including the heart, and death.
Nomikos et al (1986) conclude that oxygen derived free radicals
may be the cause of most diabetes, with a reference to Okomoto's
(l98l) model for beta cell damage having a common final pathway
for toxic agents such as streptozotocin, alloxan, and inflammatory
tissue damage. Oxygen injury in the beta cell would indeed muse
cessation of specialized cell function producing insulin deficiency.
Simultaneous oxygen injury to other cells such as the myocardium
would produce the heart disease. Oxidation damage is most severe
in mitochondria because mitochondria oxidize the majority of the
nutrients, the membranes are therefore most likely to be impaired
because the superoxides and peroxides are formed there, leading
to peroxidation of the lipids of that mitochondria causing the
cell to turn to alternate energy pathways, such as the pentose
shunt, as a means of continuing energy production. Okomoto's model
(198l, page 57) shows his concept of a final common pathway for
cell injury by alloxan and streptozotocin causing damage to proinsulin
synthesis in the beta cell. Additionally there is the superoxide
as another cause of free radical formation as per Schaufstetter
(1986), vitamin C and E and beta carotene as additional free radical
scavengers; and the zinc ion (ZN2+) as an additional inhibitor
of the poly (ADP-ribose) synthetase
Measures that also help restore cell energy production because
they are also free radical scavengers include Vitamin C in daily
doses of 3 to 20 grams (Lehninger l975), Vitamin E in daily doses
of 12001600 IU (Lehninger l975), Linseed oil 30 to 60 mL daily,
fish oil or cod liver oil, and beta carotene and niacin 500 mg
daily as a precursor to NAD. Although Okamoto used niacinamide
as a free radical scavenger and NAD precursor, there is an advantage
to using niacin instead which is that it doesn't inhibit the DNA
repair process, i.e. the poly (ADP-ribose) synthetase reaction.
If you use niacinamide you may stop the repair of the DNA strand
breaks, by inhibiting the poly (ADP-ribose) synthetase and this
would cause abnormal DNA and therefore tumor formation (Yamamoto
198l).
Mitochondrial type oxidation is the Krebs cycle, which relies
upon NAD to function. If the cell fails in mitochondrial oxidation
and declines to dependence upon the pentose phosphate shunt pathway,
the result will be an excessive fatty acid production at the expense
of glycogen- Fatty acids are the storage form for the pentose
shunt and they tend to be overproduced when mitochondria are impaired,
at the same time the burning of these fatty acids is also limited.
Overproduction plus limited use leads to a massive accumulation
of fat in the blood, cells, arteries, liver, kidney, etc. Fatty
degeneration of tissues and arteriosclerosis is therefore caused
by mitochondrial membrane damage by oxygen, Alternately, a decrease
in the use of the pentose shunt causes a decrease in the fatty
acid synthesis and an increase in glycogen as an energy storage
molecule
Smith reports (l98l) a case of severe hypertriglyceridemia in
an alcoholic with diabetes, The combination of insulin therapy
and nicotinic acid 1200 mg daily returned the triglyceride levels
to normal. Insulin alone could not do this and Smith demonstrates
the effectiveness of including nicotinic acid in diabetes therapy
to correct defects not influenced by insulin alone, Niacin releases
insulin from the beta cells because it returns them to functioning
organs, it generates a coenzyme which restores the mitochondrial
Krebs cycle.
The importance of fat metabolism in diabetes is shown by Kamada
(1986) who found diabetics to have impaired membrane fluidity
due to deficient unsaturated fatty acids, This deficiency in the
linolenic l8:3 omega 5 essential fatty acid is the dietary deficiency
commonly found in our modern western diet according to Rudin (l981)
which complicates the diagnosis and evaluation of diabetes, the
deficiency must be corrected also. When sardine oil was given
the membranes were restored to normal. O'Dea (l984) found Australian
aborigines who were suffering from diabetes on the Western diet
and lifestyle were cured by returning them to their old native
lifestyle and diet of fish, kangaroo meat, and vegetation, which
included a high amount of omega 3 EFA and niacin, not found in
our modern western diet, Membrame fluidity of damaged mitochondrial
membranes can be restored by the essential fatty acids, the cellular
ATP production is improved, and the cell functions once again.
There is improved sodium pumping and improved membrane transport
of the nutrient molecules like glucose and amino acids that enter
cells and the mitochondria by co-transport with sodium ion. The
energy for membrane transport of glucose and amino acids comes
from the ATP used to pump sodium back across the membrane in exchange
for potassium inside the allows active transport of glucose into
the cell by cotransport with sodium. In the cell with low ATP,
sodium tends to accumulate inside the cell, The cells are swollen
and when niacin is given to diabetics the most dramatic change
noticed by patient and doctor alike is the movement of fluid out
of the body.
A Biochemical Model for Insulin Resistance
Trishitta (1984) shows ATP inhibits insulin binding to cell receptor
sites- it provides a biochemical model to explain "insulin resistance".
This concept is applicable to both type I and II diabetes. In
type I or insulin dependent diabetes there is often a worsening
of the clinical course with the need to raise the amount of insulin
injected. Sometimes even a large increase in the amount causes
little or no change in hyperglycemia. The reason is that low ATP
levels in the cells causes an increase in the need for insulin
binding to receptors- Ordinarily this results in an increase in
cell membrane transport of nutrient molecules like glucose, amino
acids, and fat globules but if the mitochondria of the cell are
inactivated due to low NAD in the cytosol or damaged membranes
from oxidation injury, or nonfunctioning due to omega 3 EFA deficiency,
the increased insulin is not effective in raising ATP levels which
then decreases insulin requirement. Instead the body seems to
require more and more insulin as the ATP levels fall in the cells
with impaired mitochondrial oxidation
As Applied to Porphyria
Streptozotocin and alloxan have been used extensively to induce
experimental diabetes in animals. At one time it was believed
that they had action only on the beta cell of the pancreas, but
this is not true. The beta cell is just the most sensitive to
these agents. Other cells can also be alkylated in the same way
with the same outcome; decreased cytosol NAD, low ATP, and cessation
of specialized cell function. Porphyria can be induced by STZ,
alloxan, and mycotoxins which alkylate hepatocytes and induce
the same reaction seen in the cured by returning them to their
old native lifestyle and diet of fish, and vegetation, which included
a high amount of omega 3 EFA and niacin, not found in our modern
western diet. Membrane fluidity of damaged mitochondrial membranes
can be restored by the essential fatty acids, the cellular ATP
production is improved, and the cell functions once again. There
is improved sodium pumping and improved membrane transport of
the nutrient molecules like glucose and amino acids that enter
cells and the mitochondria by cotransport with sodium ion. The
energy for membrane transport of glucose and amino acids comes
from the ATP used to pump sodium back across the membrane in exchange
for potassium inside the allows active transport of glucose into
the cell by cotransport with sodium. In the cell with low ATP,
sodium tends to accumulate inside the cell. The cells are swollen
and when niacin is given to diabetics the most dramatic change
noticed by patient and doctor alike is the movement of fluid out
of the body.
Massive production of porphyrins is the hepatocytes response to
low ATP levels. Gadjos (l969) used glucose to elevate ATP and
cure porphyria in rats. Pinelli (1972) reversed STZ-induced porphyria
with nicotinic acid, Spies (1938, l938, 1939) gave a single dose
of niacin 500 mg orally to diabetic patients with porphynuria
and the porphynuria cleared for three days. So we have a model
in the beta cell for studying oxidation injury and the resultant
organ failure, and the restoration of function with vitamin B3
which we can apply to porphyria also- Rather, we should probably
say porphyria is a stage of diabetes, or the two are a form of
pellagra, or substrate pellagras Rudin (l987) discusses it, Sato
(l987) has used STZ to produce hypertension and diabetes in an
animal model which confirms our experience in humans that they
are both caused by low NAD.
The Case Reports
Case 1. Hypertension brought under control with niacin
A fifty-four year old Negro man with diabetes, hypertension and
early heart failure, was on Tolinase 250 mg daily for diabetes,
Lasix 40 mg daily, Aldomet 250 mg qid, Apresaline 50 mg daily.
The diabetes was well corrected when measured by blood sugar levels.
The patient however, had developed early heart failure and less
of control of the hypertension with the blood pressure at 180/l2O
with medication. He felt very lethargic and suffered headaches-
Niacin 750 mg P.O. daily was given in three doses of 250 mg. Within
six days his blood pressure was l40/9O and he felt much better-
At four weeks blood pressure was l20/86 and medication remained
with Tolinase 250 mg, Lasix 40 mg daily, Aldomet 250 mg daily,
and Apresaline 50 mg daily- At eight weeks he had blood pressure
130/90 but he had also eliminated the Apresaline 50 mg daily.
The patient had a feeling of increasing well being, and began
to walk several miles each day.
Case 2. Diabetes and Gout.
A forty-seven year old white man with hypertension who was taking
four different drugs for his hypertension, arthritis, and gout.
He then was found to have elevated blood sugar and could not accept
the idea of going on five different medications so he stopped
taking all of them, by himself. A few days later he consulted
me about his condition, flatly stating he would not take the usual
regime of pharmaceuticals. I started him on niacin 500 mg daily.
In addition he took vitamin C, 1000 mg daily,
zinc 50 mg tab daily, as well as one multiple vitamin daily. After
four weeks a glucose tolerance test was done which measured as
normal. His hypertension was gone also- There was no evidence
of gout or arthritis and the patient seemed to feel more energetic
and slept better than before. Six months later he continued on
just niacin 300 mg with normal blood pressure and blood sugar,
no gout or arthritis.
Case 3.
A sixty-four year old white male with an earlier history of alcoholism
and now with adult onset diabetes, presenting with emphysema,
insomnia, a pre-gangrenous condition on his left middle toe, chronic
productive cough and shortness of breath, and edema with abdominal
distention (his waist had increased seven inches in size). He
had been on Tolinase 250 mg per day for two years and Theodur
600 mg per day for his emphysema for several years. His edema
was at this point life-threatening, his enlarged heart was failing-
Although he had been treated for hypertension in the past years,
his blood pressure appeared normal, because his heart was unable
in heart failure to raise the blood pressure. During that time
that he was being treated with thiazides he developed diabetes,
and in as much as the thiazides do not cure the original problem,
and diabetes is but another step of the pellagra and omega 3 EFA
deficiency that he actually had, his pellagra was progressing
to its terminal stages. A pharmaceutical diuretic would have improved
superficially his edema but niacin is an effective diuretic and
as my diagnosis was that of pellagra, I used niacin very successfully
on this patient. He had a pellagra type skin breakdown on his
elbows, not very significant alone, but also an unhealing blister
on his hand, an area exposed to the sunlight. He was irrational,
his urine was noted to be dark at times, both very significant
pellagra symptoms- Also classical for pellagra was his insomnia,
he slept only a few hours each night- He was unable to cat except
for very small amounts, also indicative- I did not have to check
for low NAD levels, he had pellagra written all over him. I put
him on 500 mg niacin per day, 2000 mg vitamin C per day, and a
multiple vitamin. He quit all of his prior medicines and at first
for three months took only the niacin- With only the niacin his
pregangrenous condition on his middle left toe cleared up in a
matter of days. The pressing problem of his edema improved slowly,
the first month he lost 10 pounds and three inches off his waist
and the swelling in his ankles was cured. The second month he
lost another 10 pounds and two more inches off his waist. At six
months he takes no pharmaceutical medicines, only his vitamins.
His blood sugar is normal, he is eating well, he is rational,
his urine is not dark, he feels in excellent health,
Case 4.
A sixty-two year old white man with a long history of gout and
a recently discovered diabetes based on a blood sugar of 1190
mg% and 540 mg%- He usually took Butazolidin for his gout when
it flared up but decided to experiment with niacin. He was given
250 mg bid. In four days his gout pain was gone and never returned,
which was better than the results he had experienced with Butazolidin
treatment. He continued on niacin 500 mg daily for one month,
then he began testing his urine with a test tape and noted 0 sugar
at 7:00 a.m. and 1+ sugar two hours after meals. This was much
better than anticipated based on the blood sugar readings at onset
of treatment. That he was improving was obvious to us both. After
six weeks of therapy he developed a visual disturbance, inability
to focus, which may have been due to decreases in internal pressure
in the eye from the diuretic effect of niacin. He had a 5 diopter
change in his glasses and then could see well again. At eight
weeks the blood sugar fasting was l56 mg%. At ten weeks the two
hour postprandial blood sugar was 120 mg%. At sixteen weeks he
had a 95 mg% blood sugar, and the blood pressure was 118/78.
Discussion of Case Studies
If diabetes results from low cell ATP, then attempts to restore
the energy production system should improve or cure diabetes.
Complete recovery depends on the number of viable beta cells left
in the pancreas that can be restored to insulin production, however
the complications of diabetes may be ameliorated by restoring
normal energy production to the rest of the body even though insulin
must be given in addition.
My clinical trial was limited to four cases of adult onset diabetes
and of these, two were old cases treated with oral antidiabetic
agents- The reason antidiabetic agents work is that they mimic
the action of NAD which is very low in diabetes, causing a release
of insulin from the beta cells, but they do not restore function
of the mitochondrial Krebs cycle as NAD does, they do not cure
this problem. Two of the cases were newly discovered cases not
yet treated. All four cases responded to therapy with nicotinic
acid (vitamin B3), The old cases stopped taking their oral agent,
and the new cases took no pharmaceutical drugs, only vitamin supplements.
Blood sugar levels return to normal and the patients all experienced
a water diuresis over a period of several months that resulted
in a loss of 20 to 30 pounds. Nicotinic acid was given in oral
doses of 500 mg day for the first month to attempt to restore
depleted NAD levels in the cells. It takes 3 or 4 weeks on the
500 mg a day level to do this, and this is the same dose used
to treat pellagra, the known NAD deficiency disease. After a month,
250 mg per day is given long term- If the antioxidant system of
the body could be totally repaired, it is possible that niacin
supplements would not be necessary long term, but persons with
diabetes have a lot of oxidation damage that causes a higher niacin
intake to be required to prevent relapses.
Infants born to diabetic mothers have long been known to suffer
a higher than normal perinatal mortality rate They are usually
heavier than normal as a result of fluid accumulation due to defective
membrane transport of sodium and glucose. These infants could
be quickly restored to normal metabolism by giving them nicotinic
acid and raising the depleted NAD levels of their cells
Biochemical abnormalities of diabetes include excessive ketone
body formation with ketonuria and acidosis or excessive H+ ion
accumulation- When normal metabolic pathways of the citric acid
cycle are disrupted, the oxidation of hydrogen ion and the combining
with oxygen in the cytochrome system of the mitochondria is defective.
Niacin corrects this.
Why are the eyes of a diabetic more susceptible to vascular damage?
We know that the retina uses only fermentation of glucose to lactate
to obtain energy. Is lactate concentration more elevated in the
retinal vessels of a diabetic? Are the cell membranes of a diabetic
damaged also by excess H+ ions? Membrane "fluidity" is dependent
upon maintaining unsaturated fatty acids in the membranes. Excess
H+ ion seen in diabetic acidosis may combine with unsaturated
fatty acids to make them more saturated and less fluid. Less fluid
membranes are not able to be effective in membrane transport.
Since diabetes is the leading cause of blindness, treatment with
nicotinic acid and the omega 3 fatty acids may reverse the abnormal
metabolism and prevent blindness in diabetes
References