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The human kidneys:
· are two bean-shaped organs, one on each side of the backbone.
· Represent about 0.5% of the total weight of the body,
· but receive 20%-25% of the total arterial blood pumped by the heart.
· Each contains from one to two million nephrons.
The nephron is a tube; closed at one end, open at the other. It consists of :
· Bowman's capsule ; Located at the closed end, the wall of the nephron is pushed in forming a double-walled chamber.
· Glomerulus ; A capillary network within the Bowman's capsule. Blood leaving the glomerulus passes into a second capillary network (not shown in the figure) surrounding the
· Proximal convoluted tubule. Coiled and lined with cells carpeted with microvilli and stuffed with mitochondria.
· Loop of Henle ; It makes a hairpin turn and returns to the
· Distal convoluted tubule, which is also highly coiled and surrounded by capillaries.
· Collecting tubule ; It leads to the pelvis of the kidney from where urine flows to the bladder and, periodically, on to the outside world.
Formation of Urine The nephron makes urine by
· filtering the blood of its small molecules and ions and then
· reclaiming the needed amounts of useful materials.
· Surplus or waste molecules and ions are left to flow out as urine.
In 24 hours the kidneys reclaim
· ~1,300 g of NaCl
· ~400 g NaHCO3
· ~180 g glucose
· almost all of the 180 liters of water that entered the tubules.
The steps:
· Blood enters the glomerulus under pressure.
· This causes water, small molecules (but not macromolecules like proteins) and ions to filter through the capillary walls into the Bowman's capsule. This fluid is called nephric filtrate. As the table shows, it is simply blood plasma minus almost all of the plasma proteins. Essentially it is no different from interstitial fluid
Composition of plasma, nephric filtrate, and urine (each in g/100 ml of fluid). These are representative values. The values for salts are especially variable, depending on salt and water intake. |
SComponent |
Plasma |
Nephric Filtrate |
Urine |
Concentration |
% Reclaimed |
Urea |
0.03 |
0.03 |
1.8 |
60X |
50% |
Uric acid |
0.004 |
0.004 |
0.05 |
12X |
91% |
Glucose |
0.10 |
0.10 |
None |
- |
100% |
Amino acids |
0.05 |
0.05 |
None |
- |
100% |
Total inorganic salts |
0.9 |
0.9 |
<0.9—3.6 |
<1—4X |
99.5% |
Proteins and other macromolecules |
8.0 |
None |
None |
- |
- |
· Nephric filtrate collects within the Bowman's capsule and then flows into the proximal tubule.
· Here all of the glucose, and amino acids, >90% of the uric acid, and ~60% of inorganic salts are reabsorbed by active transport.
· The active transport of Na+ out of the proximal tubule is controlled by angiotensin II.
· The active transport of phosphate is regulated (suppressed by) the parathyroid hormone.
· As these solutes are removed from the nephric filtrate, a large volume of the water follows them by osmosis (80–85% of the 180 liters deposited in the Bowman's capsules in 24 hours).
· As the fluid flows into the descending segment of the loop of Henle, water continues to leave by osmosis because the interstitial fluid is very hypertonic. This is caused by the active transport of Na+ out of the tubular fluid as it moves up the ascending segment of the loop of Henle.
· In the distal tubules, more sodium is reclaimed by active transport, and still more water follows by osmosis.
· Final adjustment of the sodium and water content of the body occurs in the collecting tubules.
Sodium
Although 97% of the sodium has already been removed, it is the last 3% that determines the final balance of sodium — and hence water content and blood pressure— in the body. The reabsorption of sodium in the distal tubule and the collecting tubules is closely regulated, chiefly by the action of the hormone aldosterone.
Water
· The hypertonic interstitial fluid surrounding the collecting tubules provides a high osmotic pressure for the removal of water.
· Transmembrane channels made of proteins called aquaporins are inserted in the plasma membrane greatly increasing its permeability to water. (When open, an aquaporin channel allows 3 billion molecules of water to pass through each second.)
· Insertion of aquaporin-2 channels requires signaling by the antidiuretic hormone (ADH also known as arginine vasopressin or AVP).
1.1 ADH binds to receptors (called V2 receptors) on the
asolateral surface of the cells of the collecting tubules.
1.2 Binding of the hormone triggers a rising level of CAMP
within the cell.
1.3 This "second messenger" initiates a chain of events
culminating in the insertion of aquaporin-2 channels in
the apical surface of the cell.
The release of ADH (from the posterior lobe of the pituitary gland) is regulated by the osmotic pressure of the blood.
· Anything that dehydrates the body, such as perspiring heavily,
1.1 increases the osmotic pressure of the blood;
1.2 turns on the ADH -> V2 receptors ->aquaporin-2 pathway.
The result:
1.1 As little as 0.5 liter/day of urine may remain of the
original 180 liters/day of nephric filtrate.
1.2 The concentration of salts in the urine can be as much as
four times that of the blood. (But not high enough to
enable humans to benefit from drinking sea water, which
is saltier still.)
· If the blood should become too dilute (as would occur after drinking a large amount of water),
1.1 ADH secretion is inhibited
1.2 The aquaporin-2 channels are taken back into the cell by
endocytosis.
1.3 The result: a large volume of watery urine is formed (with
a salt concentration as little as one-fourth of that of the
blood).
This disorder is characterized by:
· excretion of large amounts of a watery urine (as much as 30 liters — about 8 gallons — each day!
· Unremitting thirst.
It can have several causes:
· Insufficient secretion of ADH
· Inheritance of two mutant genes for the ADH receptor (V2).
· Inheritance of two mutant genes for aquaporin-2.
The most obvious effect of this rare, inherited disorder is extremely high blood pressure (hypertension). It is caused by a single mutant allele (therefore the syndrome is inherited as a dominant trait) encoding the aldosterone-activated sodium channel in the collecting tubules. The defective channel is always “on” so too much Na+ is reabsorbed and too little is excreted. The resulting elevated osmotic pressure of the blood produces hypertension.
Although urine formation occurs primarily by the filtration-reabsorption mechanism described above, an auxiliary mechanism, called tubular secretion, is also involved.
The cells of the tubules remove certain molecules and ions from the blood and deposit these into the fluid within the tubules.
Example: Both hydrogen ions (H+) and potassium ions (K+) are secreted directly into the fluid within the distal and collecting tubules. In each case the secretion is coupled to the ion-for-ion uptake of sodium ions (Na+).
Tubular secretion of H+ is important in maintaining control of the pH of the blood.
· When the pH of the blood starts to drop, more hydrogen ions are secreted.
· If the blood should become too alkaline, secretion of H+ is reduced.
· In maintaining the pH of the blood within its normal limits of 7.3–7.4, the kidney can produce a urine with a pH as low as 4.5 or as high as 8.5.
While we think of the kidney as an organ of excretion, it is more than that. It does remove wastes, but it also removes normal components of the blood that are present in greater-than-normal concentrations. When excess water, sodium ions, calcium ions, potassium ions, and so on are present, the excess quickly passes out in the urine. On the other hand, the kidneys step up their reclamation of these same substances when they are present in the blood in less-than-normal amounts. Thus the kidney continuously regulates the chemical composition of the blood within narrow limits. The kidney is one of the major homeostatic devices of the body.
The human kidney is also an endocrine gland secreting two hormones:
· Erythropoietin (EPO)
· Calcitriol (1,25[OH]2 VitaminD3), the active form of vitamin D
as well as the enzyme renin.
The artificial kidney uses the principle of dialysis to purify the blood of patients whose own kidneys have failed.Artificial kidneys have proved of great benefit in helping patients of acute kidney malfunction survive the crisis until their own kidneys resume operation. They have also enabled people suffering from chronic kidney failure to remain alive, though at an enormous expense of time (often three sessions of 6 or more hours per week), money, and psychological well-being. Furthermore, although dialysis does a good job at removing wastes, it cannot perform the other functions of the kidney:
· providing precise homeostatic control over the concentration of such vital ingredients as glucose and Na+
· secreting its hormones
An artificial kidney of the future?
In an attempt to solve these problems, a research team at the University of Michigan is experimenting with adding a "Bioreactor unit" to the dialysis unit. The bioreactor consists of many hollow, porous tubes on the inner wall of which is attached a monolayer of proximal tubule cells (derived from pigs). The dialysis bath fluid passes through the lumen of the tubes where molecules and ions can be picked up by the apical surface of the cells. Discharge of essential molecules and ions (as well as hormones) at the basolateral surface of the cells places these materials back in the blood (just as the proximal tubule cells in the nephron normally do). So far, all the testing has been done using dogs, but the results seem promising.The ideal alternative to long-term dialysis is transplantation of a new kidney. The operation is technically quite easy. The major problems are:
· the shortage of donors suitably matched for histocompatibility molecules
· the problem of graft rejection by the recipient's immune system that — unless the donor and recipient are identical twins — "sees" the kidney as "foreign" even when they share the same major histocompatibilitymolecules.