Bernardo Alberto Houssay – Nobel Lecture
Nobel Lecture, December 12, 1947
The role of the hypophysis in carbohydrate metabolism and in
diabetes
The nutritive substances used in greatest
quantities by mammals are carbohydrates. - These are ingested with
the food or produced by the liver, and after being converted into
glucose they are utilized by all the cells of the organism,
specially by the muscles, which constitute nearly half the mass of
the body.
Production and consumption of carbohydrates is
so well regulated that there is a constant blood sugar level; any
accidental increase or fall in blood sugar is rapidly compensated.
The constancy of the blood sugar level is maintained by a complex
physiological mechanism, a homeostatic mechanism of the same order
as those which maintain the body temperature, the blood pressure or
the heart rate at normal levels and control many other functions.
The blood sugar level itself is an important factor in many chemical
and physiological processes.
The liver is the principal organ in the
regulation of the blood sugar level. If the liver is removed there
is a progressive hypoglycemia which ends in death. After hepatectomy
it is not possible to provoke hyperglycemia, whatever the agent or
procedure employed, whether the animal were diabetic or not before
the liver was removed. Nor is it possible to produce any form of
diabetes in hepatectomized animals. On the other hand, when there is
hyperglycemia the liver diminishes or ceases the production of
sugar, and stores it.
The production and consumption of glucose and
hence the blood sugar level, are controlled by a functional
endocrine equilibrium. This mechanism acts on the liver - the organ
which produces and stores glucose - and on the tissues which are the
consumers of glucose, by means of hormones which play a part in the
chemical processes of carbohydrate metabolism.
The secretion of each endocrine organ is
controlled by a physiological mechanism. For instance, the pancreas
secretes insulin in adequate quantities so as to maintain a normal
blood sugar level, and the blood sugar level regulates the amount of
insulin secreted. Thus hyperglycemia increases the secretion of
insulin and hypoglycemia diminishes or completely inhibits it. This
regulation of insulin secretion is maintained even when the pancreas
is surgically reduced to one seventh of its normal mass, or when
besides the intact pancreas in situ four others are grafted
into the circulation. In both cases the blood sugar is kept
constantly at a normal level. The extrinsic innervation of the
pancreas is not necessary for the regulation of insulin secretion;
the response of the denervated pancreas to changes in blood sugar
differs only in minor details from the response of the normal
pancreas.
Not only is the secretion of each gland
regulated according to the organic needs of each moment, but there
is also an equilibrium between the secretions of the different
glands. The blood sugar and the production and consumption of
glucose are kept within normal bounds, therefore there is an
equilibrium between the glands of internal secretions which reduce
the blood sugar (pancreas) and those which raise it
(anterohypophysis, adrenals, thyroid, etc.).
In 1907, when I was a medical student, I was
attracted to the study of the hypophysis because the microscopic
picture showed glandular activity and its lesions were accompanied
by serious organic disturbances, such as acromegaly, dwarfism,
etc.
The frequency of glycosuria or diabetes in
acromegaly has been reported many times; Atkinson found it in 32.8%
of 817 cases of the disease published up to 1938. Moreover, extracts
of the posterior lobe of the hypophysis produce rapid
pharmacological effects, amongst which is a transitory hyperglycemia
(Borchardt, 1908). Therefore it was commonly accepted that if the
hypophysis played a part in carbohydrate metabolism, it would be due
to the activity of its posterior lobe.
One year after the discovery of insulin a
systematic study of the influence of endocrine glands on its
activity was organized in my laboratory. With Magenta
(1924-1927-1929) I found that hypophysectomized dogs were
hypersensitive to the toxic and hypoglycemic action of insulin. In
1925, I found the same fact in the toad (with Mazzocco and Rietti);
and in 1929, assisted by Miss Potick I saw that the administration
of pars distalis prevented or corrected hypersensitiveness to
insulin in hypophysectomized toads.
The next step consisted in the removal of the
pancreas in hypophysectomized dogs and toads (with Biasotti in
1930). The removal of the hypophysis or of its pars distalis
produced a considerable attenuation of the severity of pancreatic
diabetes. The injection or implantation of anterior hypophyseal lobe
reestablished or even increased the usual severity of diabetes.
This work, done in 1930, showed that: (a) the
anterior lobe of the hypophysis has an important part in the
physiological control of metabolism; (b) the hypophysis is a factor
conditioning the severity of diabetes; (c) the injection of anterior
lobe of the hypophysis has a diabetogenic effect.
Later the diabetogenic effect was also
demonstrated in dogs with a surgically reduced pancreas (Houssay,
Biasotti, Di Benedetto, and Rietti, 1932) or with an intact pancreas
(Evans et al., 1932, etc.). A permanent diabetes was produced
by prolonged treatment with the extract of anterior lobe of
hypophysis in dogs with a reduced (Houssay, Biasotti, Di Benedetto,
and Rietti, 1932) or an intact pancreas (Young, 1937).
After total hypophysectomy, or removal of the
pars distalis, when the animals are kept fasting, a severe,
and sometimes fatal, hypoglycemia easily occurs. These animals are
also very sensitive to hypoglycemic agents, such as insulin and
phloridzin. Hyperglycemia produced by adrenaline or by glucose
administration is followed in some cases by intense hypoglycemia and
convulsions.
The injection of pars distalis increases the
resistance to insulin and phloridzin. This effect has been called
glycotropic by Young (1936-1938).
Hepatic and muscular glycogen falls rapidly in
fasting hypophysectomized animals. Hypophyseal injections inhibit
this decrease specially in respect to muscle glycogen and this
action is also produced in absence of the adrenals (Russell,
Bennett); The mobilization of hepatic glycogen by insulin or
adrenaline is in some species slower in hypophysectomized than in
normal animals.
Extirpation of the hypophysis, or of the pars
distalis, markedly attenuates the severity of pancreatic and
phloridzin diabetes. Hypophysectomized pancreatectomized dogs show
the following differences with respect to pancreatectomized dogs:
(a) they survive a long time, the wounds heal well and infection is
much less frequent; (b) there is a slow gradual loss of weight; (c)
the loss of nitrogen is less considerable; (d) hyperglycemia and
glycosuria are less marked and are sometimes absent; fasting
produces a notable fall in blood sugar and decrease in glycosuria;
(e) spontaneous hypoglycemic crises occur, usually due to
underfeeding or fasting and there is hypersensitiveness to insulin;
(f) hypoglycemic crises can be prevented by carbohydrate or
protein-rich diets, but not by fats; injection of glucose saves the
animal's life when it has fallen into a hypoglycemic crisis; (g)
there is little decrease in hepatic and muscle glycogen if the
diabetes is not severe, and in some cases the same concentrations as
in the controls are found; (h) when glucose is injected only part of
it and sometimes none, is excreted in the urine; (i) the blood sugar
curve following glucose administration is intermediate between those
of pancreatectomized and normal dogs; (j) after glucose is given,
there is a moderate rise in the respiratory quotient in some cases,
but not in all; (k) the increase in ketonemia and ketonuria is
remarkably small; (l) the increase in lipemia and cholesterolemia is
not considerable; (m) the rise in the basal metabolic rate is less
than in the pancreatectomized controls; (n) the D/N ratio in urine
is also lower than in the controls.
Hypophysectomized pancreatectomized animals
utilize more glucose than pancreatectomized, but less than normal
animals. Protein consumption does not increase as much as in the
pancreatectomized; the small amount of ketonuria points to a
diminished consumption of fat.
The diabetogenic effect of the hypophysis was
first observed in animals in which both the hypophysis and the
pancreas had been removed. Later, in 1937, it was demonstrated in:
(a) dogs with a surgically reduced pancreas (Houssay, Di Benedetto,
and Rietti); (b)normal rabbits (Baumann and Marine); (c) normal
puppies.
Daily injections of anterohypophyseal extract
provoke after two or three days a rise in blood sugar and
hypophyseal diabetes in cats and dogs. In the dog the blood sugar
rises from normal to 150 to 300 mg per cent; there is glycosuria;
ketonemia and ketonuria increase; and there is polyuria and
polydipsia. Injection of glucose is followed by a typical diabetic
blood sugar curve and the respiratory quotient does not rise or
rises very little. The animal becomes insulin resistant.
The hypophysis of all vertebrates has this
diabetogenic effect on animals of its own and other species. The
pars distalis is responsible for the diabeto-genie effect,
the posterior lobe has little activity in this respect. The
diabeto-genie principle is rapidly destroyed at room temperature,
therefore the extracts should be stored at a temperature near
0°C.
The active principle is a protein. Young has
obtained a concentrated extract, but it has not been prepared in a
pure form, so it is not yet possible to say if it is a separate
hypophyseal hormone, different from those already known. I am
mistakenly supposed to have described a diabetogenic hormone. I have
described a diabetogenic property, or factor, or action of the
extract, without having said this effect was due to a diabetogenic
hormone. The regulation of carbohydrate metabolism is a normal
function of the hypophysis, but certainly the production of diabetes
is not one of its normal functions. Nevertheless an active
hypophysis, even when it is functioning normally, increases the
severity of diabetes.
The diabetogenic effect of the hypophysis is
dependent on the liver. It can not be obtained in the
hypophysectomized pancreatectomized toad if the liver has been
removed. Hepatectomy causes a rapid fall in the blood sugar of dogs
or toads with a hypophyseal diabetes. On the other hand, destruction
of the diencephalon or removal of the whole brain, or extirpation of
the kidneys, the adrenals, the thyroid, the lungs and all the
digestive tract do not prevent the diabetogenic effect.
In the toad and in the dog, adrenalectomy
diminishes but does not suppress the diabetogenic effect of the
anterior lobe extract, which can be obtained in adrenalectomized
dogs, in which the pancreas has been surgically reduced, and which
are kept alive by treatment with desoxycorticosterone and salt or
even with sodium chloride alone. The experiments of Long show that
the adrenocorticotrophic hormone of the hypophysis by releasing
corticoadrenal hormones, plays a part in the diabetogenic effect;
but my own experiments prove there is a hypophyseal diabetogenic
action which takes place when there are no adrenals.
There are pancreatic and extrapancreatic factors
in the production of hypophyseal diabetes.
Extrapancreatic: factors are demonstrated by:
(1) the diabetogenic effect obtained in pancreatectomized
hypophysectomized animals; (2) the increase in the severity of
diabetes in pancreatectomized dogs treated with anterohypophyseal
extract; (3) the increase in resistance to insulin which precedes
and accompanies hypophyseal diabetes; (4) the fact that
hyperglycemia and diabetes occur before that there are visible
lesions in the beta cells of the islets, and before insulin
secretion diminishes.
After two to four days of hyperglycemia provoked
by the injection of an terohypophyseal extracts the beta cells show
signs of damage and insulin secretion diminishes. The beta cells are
degranulated, they swell, become vacuolized and go into hydropic
degeneration. In most cases there is no insulin secretion or it is
considerably reduced. This can be demonstrated by grafting the
pancreas from these animals into the circulation of a diabetic
animal. A normal pancreas reestablishes the normal blood sugar level
in three to five hours and maintains it there, while the pancreas
taken from an animal in hypophyseal diabetes has little or no effect
on the blood sugar.
If after a few days the anterohypophyseal
treatment is discontinued the diabetic condition disappears, the
blood sugar returns to a normal level, and later the beta cells
regain their normal aspect. If daily injections of anterohypo
physeal extracts are continued for several weeks, beta cells first
show pycnotic nuclei and then gradually disappear in great numbers.
At this stage even if the hypophyseal treatment is discontinued the
animals remain permanently diabetic, degeneration of the beta cells
continues and the pancreas ceases to secrete insulin.
The diabetic condition which appears during
hypophyseal treatment and which disappears when this treatment is
discontinued should be called hypophyseal diabetes. The lesions in
the beta cells are reversible.
The diabetic conditions which persists when the
hypophyseal treatment is discontinued, should be called
metahypophyseal diabetes. It is a pancreatic diabetes due to
irreversible lesions of the beta cells. It is produced by the
injection of hypophyseal extract, but persists without this
treatment.
In hypophyseal diabetes there is a marked
increase in insulin resistance, while in metahypophyseal diabetes
the resistance to the action of insulin is normal or only slightly
increased. It is possible that in acromegaly, in some stages of the
disease there may be a hypophyseal diabetes and at others a
metahypophyseal diabetes.
There is a certain antagonism between the
hypophysis and the pancreas. Thus as the mass of the pancreas is
progressively reduced by extirpation of increasingly larger
portions, the dose of hypophyseal extract needed to provoke diabetes
diminishes. Reciprocally in hypophysectomized animals there is
hypersensitiveness to insulin, and in fasting, their blood sugar and
glycogen falls more rapidly and markedly than in normal animals.
The anterohypophysis is not necessary for the
normal development and maintenance of the pancreas, therefore there
is no physiologic pancreatotrophic effect of the hypophysis on the
pancreas. Hypophysectomy does not cause a loss in the weight of the
pancreas in dogs, nor of the insular mass in several species in
which it has been examined; on the contrary, there is an increase in
the islets. The pancreatic content and secretion of insulin are
normal.
Anterohypophyseal extracts can produce two
opposite effects on the islets: (a) stimulation and hyperplasia; (b)
atrophy and hypofunction. One or other effect is observed according
to the dose given, the amount of islet tissue and the animal
species.
The lesions in the islets and the decrease in
insulin secretion are due to two factors: (a) the effect of the
anterohypophyseal extract; and (b) hyperglycemia. They are not due
exclusively to hyperglycemia as proved by the fact that the same
levels of blood sugar have been maintained during four days by
continuous injection of glucose and by hypophyseal extracts
injections. Only the hypophyseal treatment produced lesions of the
islets and decrease or absence of insulin secretion.
The mechanism by which the anterohypophysis
controls carbohydrate metabolism is still imperfectly known.
Hypophysectomized dogs utilize protein and
carbohydrate ingested in the food, but during complete fasting, or
protein fasting, the disintegration of body protein is slower than
in normal dogs. Hypophysectomy also reduces the disintegration of
body protein in pancreatic and phloridzin diabetes. It would seem
therefore that hypophysectomy diminishes the capacity of the
organism to catabolize body protein and to form glucose from this
protein.
Ketonuria is also below normal in
hypophysectomized animals in basal conditions and in the diabetic
state, whatever its origin, therefore the consumption of fat also
seems to be reduced. There is good utilization of carbohydrate in
hypophysectomized animals. Experiments in rats (Fisher, Russel, and
Cori, 1936) and rabbits (Greeley, 1935-1940) show there is a
preferential consumption of glucose, above the normal. These workers
believe this to be the fundamental metabolic disturbance produced by
hypophysectomy. In the dog this supernormal, preferential
consumption of glucose has not been demonstrated. Moreover, it could
be the effect of the subnormal and insufficient catabolism of
proteins and fats.
The pituitary is a very important regulator of
the homeostatic function of the liver. In hypophyseal insufficiency
glucose formation by the liver does not increase during hypoglycemia
as it does in normal animals. During fasting or diabetes, the
glucose formation from proteins is also lower. On the other hand an
excess of anterior pituitary produces hyperglycemia due to
diminished peripheral consumption of glucose and to lack of
inhibition of its hepatic formation.
Recently, Price, Cori, and Colowick (1945-1947)
have shown that the anterohypophysis inhibits hexokinase and that
insulin counteracts this inhibition. It is the first case in which
it has been shown that a hormone, or rather two hormones, act on an
enzymatic process of importance in carbohydrate metabolism.
Nevertheless, this important discovery does not explain all the
facts, e.g. the hypersensitiveness to insulin of hypophysectomized
animals.
One of the most important metabolic functions of
the hypophysis is the part it plays in the formation of protein on
which growth depends. The growth hormone increases the fixation of
nitrogenous substances and body protein formation. Hypophysectomized
rats with forced feeding form more fat and less protein than the
controls. Ingested protein is catabolized in a greater proportion
than in normal animals.
Young (1940-1944)supposes that the growth
hormone of the hypophysis induces the fixation of nitrogen and the
utilization of glucose when insulin is present and in this way
causes growth. When there is not enough insulin, sugar is not
utilized but excreted, i.e. there is a diabetogenic effect. His main
arguments are the following: (1) a dose of hypophyseal extract which
is rapidly diabetogenic in the adult diabetic animal causes only
growth in puppies; these young animals do not become diabetic until
after several months of treatment they cease to grow; (2) in the rat
the extract increases the islet tissue, the animal grows and there
is no diabetes; (3) extracts which are diabetogenic for the dog only
cause growth in the rat; (4) pure growth hormone increases
glycosuria in subtotally pancreatectomized rats; (5) the fixation of
nitrogen caused by hypophyseal extract is conditioned by the amount
of islet tissue or of insulin.
Long (1942) believes that the metabolic action
of the hypophysis depends on the growth hormone, the adrenotrophic
and the thyrotrophic hormones.
The work that has been done in my laboratory on
this subject has been carried out with the collaboration of Drs.
Lewis, Giusti, Mazzocco, Rietti, Potick, Biasotti, Braier, Di
Benedetto, Gerschman, Aubrun, Campos, Lanari, Curutchet, Cicardo,
Etcheverry, Foglia, Sammartino, Magdalena, Ferrer- Zanchi, Savino,
Hug, Novelli, Orias, Parodi, Leloir, Artundo, Lascano-Gonzalez,
Gofialons, Riet-Correa, Stoppani, Dambrosi, Dosne, Fernandez, A.
Houssay, H. Houssay, Smyth, Pasqualini, Marenzi, De Robertis, and
others.
Carbohydrate metabolism and other metabolic
processesare regulated by the balance maintained between the
secretion of several endocrine glands. Diabetes and other metabolic
diseases are a disturbance in this endocrine equilibrium. There are
still many problems to be solved, but undoubtedly the hypophysis is
one of the most important organs in the regulation of metabolism and
the center of the endocrine constellation.
From
Nobel Lectures, Physiology or Medicine 1942-1962.
|
1946
