Glomerular Diseases
On this page:
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What
are the kidneys and what do they do?
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How
do glomerular diseases interfere
with kidney function?
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What
are the symptoms of glomerular
disease?
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How
is glomerular disease diagnosed?
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What
causes glomerular disease?
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What
are renal failure and end-stage
renal disease?
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Points to Remember
-
Definitions
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For
More Information
Many diseases
affect kidney function by attacking the
glomeruli, the tiny units within the
kidney where blood is cleaned.
Glomerular diseases include many
conditions with a variety of genetic and
environmental causes, but they fall into
two major categories:
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Glomerulonephritis (gloh-MEHR-yoo-loh-nef-RY-tis)
describes the inflammation of the
membrane tissue in the kidney that
serves as a filter, separating
wastes and extra fluid from the
blood.
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Glomerulosclerosis (gloh-MEHR-yoo-loh-skleh-ROH-sis)
describes the scarring or hardening
of the tiny blood vessels within the
kidney.
Although
glomerulonephritis and
glomerulosclerosis have different
causes, they can both lead to kidney
failure.
What are the kidneys and what do
they do?
The two kidneys
are bean-shaped organs located near the
middle of the back, just below the rib
cage to the left and right of the spine.
Each about the size of a fist, these
organs act as sophisticated filters for
the body. They process about 200 quarts
of blood a day to sift out about 2
quarts of waste products and extra water
that eventually leave the body as urine.
Blood enters the
kidneys through arteries that branch
inside the kidneys into tiny clusters of
looping blood vessels. Each cluster is
called a
glomerulus,
which comes from the Greek word meaning
filter. The plural form of the word is
glomeruli. There are approximately 1
million glomeruli, or filters, in each
kidney. The glomerulus is attached to
the opening of a small fluid-collecting
tube called a
tubule.
Blood is filtered in the glomerulus, and
extra water and wastes pass into the
tubule and become urine. Eventually, the
urine drains from the kidneys into the
bladder through larger tubes called
ureters.
Each glomerulus-and-tubule
unit is called a
nephron. Each kidney is composed of about
1 million nephrons. In healthy nephrons,
the glomerular membrane that separates
the blood vessel from the tubule allows
waste products and extra water to pass
into the tubule while keeping blood
cells and protein in the bloodstream.
How do glomerular diseases interfere
with kidney function?
Glomerular
diseases damage the glomeruli, letting
protein and sometimes red blood cells
leak into the urine. Sometimes a
glomerular disease also interferes with
the clearance of waste products by the
kidney, so they begin to build up in the
blood. Furthermore, loss of blood
proteins like albumin in the urine can
result in a fall in their level in the
bloodstream. In normal blood, albumin
acts like a sponge, drawing extra fluid
from the body into the bloodstream,
where it remains until the kidneys
remove it. But when albumin leaks into
the urine, the blood loses its capacity
to absorb extra fluid from the body.
Fluid can accumulate outside the
circulatory system in the face, hands,
feet, or ankles and cause swelling.
What are the symptoms of glomerular
disease?
The signs and
symptoms of glomerular disease include
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proteinuria: large amounts
of protein in the urine
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hematuria:
blood in the urine
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reduced
glomerular filtration rate:
inefficient filtering of wastes from
the blood
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hypoproteinemia: low blood
protein
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edema:
swelling in parts of the body
One or more of
these symptoms can be the first sign of
kidney disease. But how would you know,
for example, whether you have
proteinuria? Before seeing a doctor, you
may not. But some of these symptoms have
signs, or visible manifestations:
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Proteinuria may
cause foamy urine.
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Blood may cause
the urine to be pink or
cola-colored.
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Edema may be
obvious in hands and ankles,
especially at the end of the day, or
around the eyes when awakening in
the morning, for example.
How is glomerular disease diagnosed?
Patients with
glomerular disease have significant
amounts of protein in the urine, which
may be referred to as ?nephrotic range?
if levels are very high. Red blood cells
in the urine are a frequent finding as
well, particularly in some forms of
glomerular disease. Urinalysis provides
information about kidney damage by
indicating levels of protein and red
blood cells in the urine. Blood tests
measure the levels of waste products
such as creatinine and urea nitrogen to
determine whether the filtering capacity
of the kidneys is impaired. If these lab
tests indicate kidney damage, the doctor
may recommend ultrasound or an x ray to
see whether the shape or size of the
kidneys is abnormal. These tests are
called renal imaging. But since
glomerular disease causes problems at
the cellular level, the doctor will
probably also recommend a kidney
biopsy?a procedure in which a needle is
used to extract small pieces of tissue
for examination with different types of
microscopes, each of which shows a
different aspect of the tissue. A biopsy
may be helpful in confirming glomerular
disease and identifying the cause.
What causes glomerular disease?
A number of
different diseases can result in
glomerular disease. It may be the direct
result of an infection or a drug toxic
to the kidneys, or it may result from a
disease that affects the entire body,
like diabetes or lupus. Many different
kinds of diseases can cause swelling or
scarring of the nephron or glomerulus.
Sometimes glomerular disease is
idiopathic, meaning that it occurs
without an apparent associated disease.
The categories
presented below can overlap: that is, a
disease might belong to two or more of
the categories. For example, diabetic
nephropathy is a form of glomerular
disease that can be placed in two
categories: systemic diseases, since
diabetes itself is a systemic disease,
and sclerotic diseases, because the
specific damage done to the kidneys is
associated with scarring.
Autoimmune
Diseases
When the body?s
immune system functions properly, it
creates protein-like substances called
antibodies and immunoglobulins to
protect the body against invading
organisms. In an autoimmune disease, the
immune system creates autoantibodies,
which are antibodies or immunoglobulins
that attack the body itself. Autoimmune
diseases may be systemic and affect many
parts of the body, or they may affect
only specific organs or regions.
Systemic
lupus erythematosus (SLE)
affects many parts of the body:
primarily the skin and joints, but also
the kidneys. Because women are more
likely to develop SLE than men, some
researchers believe that a sex-linked
genetic factor may play a part in making
a person susceptible, although viral
infection has also been implicated as a
triggering factor. Lupus nephritis is
the name given to the kidney disease
caused by SLE, and it occurs when
autoantibodies form or are deposited in
the glomeruli, causing inflammation.
Ultimately, the inflammation may create
scars that keep the kidneys from
functioning properly. Conventional
treatment for lupus nephritis includes a
combination of two drugs,
cyclophosphamide, a cytotoxic agent that
suppresses the immune system, and
prednisolone, a corticosteroid used to
reduce inflammation. A newer
immunosuppressant, mychophenolate
mofetil (MMF), has been used instead of
cyclophosphamide. Preliminary studies
indicate that MMF may be as effective as
cyclophosphamide and has milder side
effects.
Goodpasture?s syndrome
involves an autoantibody that
specifically targets the kidneys and the
lungs. Often, the first indication that
patients have the autoantibody is when
they cough up blood. But lung damage in
Goodpasture?s syndrome is usually
superficial compared with progressive
and permanent damage to the kidneys.
Goodpasture?s syndrome is a rare
condition that affects mostly young men
but also occurs in women, children, and
older adults. Treatments include
immunosuppressive drugs and a
blood-cleaning therapy called
plasmapheresis that removes the
autoantibodies.
IgA
nephropathy
is a form of glomerular disease that
results when immunoglobulin A (IgA)
forms deposits in the glomeruli, where
it creates inflammation. IgA nephropathy
was not recognized as a cause of
glomerular disease until the late 1960s,
when sophisticated biopsy techniques
were developed that could identify IgA
deposits in kidney tissue.
The most common
symptom of IgA nephropathy is blood in
the urine, but it is often a silent
disease that may go undetected for many
years. The silent nature of the disease
makes it difficult to determine how many
people are in the early stages of IgA
nephropathy, when specific medical tests
are the only way to detect it. This
disease is estimated to be the most
common cause of primary
glomerulonephritis?that is, glomerular
disease not caused by a systemic disease
like lupus or diabetes mellitus. It
appears to affect men more than women.
Although IgA nephropathy is found in all
age groups, young people rarely display
signs of kidney failure because the
disease usually takes several years to
progress to the stage where it causes
detectable complications.
No treatment is
recommended for early or mild cases of
IgA nephropathy when the patient has
normal blood pressure and less than 1
gram of protein in a 24-hour urine
output. When proteinuria exceeds 1
gram/day, treatment is aimed at
protecting kidney function by reducing
proteinuria and controlling blood
pressure. Blood pressure
medicines?angiotensin-converting enzyme
inhibitors (ACE inhibitors) or
angiotensin receptor blockers
(ARBs)?that block a hormone called
angiotensin are most effective at
achieving those two goals
simultaneously.
Hereditary
Nephritis?Alport Syndrome
The primary
indicator of Alport syndrome is a family
history of chronic glomerular disease,
although it may also involve hearing or
vision impairment. This syndrome affects
both men and women, but men are more
likely to experience chronic kidney
disease and sensory loss. Men with
Alport syndrome usually first show
evidence of renal insufficiency while in
their twenties and reach total kidney
failure by age 40. Women rarely have
significant renal impairment, and
hearing loss may be so slight that it
can be detected only through testing
with special equipment. Usually men can
pass the disease only to their
daughters. Women can transmit the
disease to either their sons or their
daughters. Treatment focuses on
controlling blood pressure to maintain
kidney function.
Infection-related
Glomerular Disease
Glomerular disease
sometimes develops rapidly after an
infection in other parts of the body.
Acute
post-streptococcal glomerulonephritis
(PSGN)
can occur after an episode of strep
throat or, in rare cases, impetigo (a
skin infection). The
Streptococcus
bacteria do not attack the kidney
directly, but an infection may stimulate
the immune system to overproduce
antibodies, which are circulated in the
blood and finally deposited in the
glomeruli, causing damage. PSGN can
bring on sudden symptoms of swelling
(edema), reduced urine output
(oliguria), and blood in the urine
(hematuria). Tests will show large
amounts of protein in the urine and
elevated levels of creatinine and urea
nitrogen in the blood, thus indicating
reduced kidney function. High blood
pressure frequently accompanies reduced
kidney function in this disease.
PSGN is most
common in children between the ages of 3
and 7, although it can strike at any
age, and it most often affects boys. It
lasts only a brief time and usually
allows the kidneys to recover. In a few
cases, however, kidney damage may be
permanent, requiring dialysis or
transplantation to replace renal
function.
Bacterial endocarditis,
infection of the tissues inside the
heart, is also associated with
subsequent glomerular disease.
Researchers are not sure whether the
renal lesions that form after a heart
infection are caused entirely by the
immune response or whether some other
disease mechanism contributes to kidney
damage. Treating the heart infection is
the most effective way of minimizing
kidney damage. Endocarditis sometimes
produces chronic kidney disease (CKD).
HIV,
the virus that leads to AIDS, can also
cause glomerular disease. Between 5 and
10 percent of people with HIV experience
kidney failure, even before developing
full-blown AIDS. HIV-associated
nephropathy usually begins with heavy
proteinuria and progresses rapidly
(within a year of detection) to total
kidney failure. Researchers are looking
for therapies that can slow down or
reverse this rapid deterioration of
renal function, but some possible
solutions involving immunosuppression
are risky because of the patients?
already compromised immune system.
Sclerotic
Diseases
Glomerulosclerosis
is scarring (sclerosis) of the
glomeruli. In several sclerotic
conditions, a systemic disease like
lupus or diabetes is responsible.
Glomerulosclerosis is caused by the
activation of glomerular cells to
produce scar material. This may be
stimulated by molecules called growth
factors, which may be made by glomerular
cells themselves or may be brought to
the glomerulus by the circulating blood
that enters the glomerular filter.
Diabetic
nephropathy
is the leading cause of glomerular
disease and of total kidney failure in
the United States. Kidney disease is one
of several problems caused by elevated
levels of blood glucose, the central
feature of diabetes. In addition to
scarring the kidney, elevated glucose
levels appear to increase the speed of
blood flow into the kidney, putting a
strain on the filtering glomeruli and
raising blood pressure.
Diabetic
nephropathy usually takes many years to
develop. People with diabetes can slow
down damage to their kidneys by
controlling their blood glucose through
healthy eating with moderate protein
intake, physical activity, and
medications. People with diabetes should
also be careful to keep their blood
pressure at a level below 130/85 mm Hg,
if possible. Blood pressure medications
called ACE inhibitors and ARBs are
particularly effective at minimizing
kidney damage and are now frequently
prescribed to control blood pressure in
patients with diabetes and in patients
with many forms of kidney disease.
Focal
segmental glomerulosclerosis (FSGS)
describes scarring in scattered regions
of the kidney, typically limited to one
part of the glomerulus and to a minority
of glomeruli in the affected region.
FSGS may result from a systemic disorder
or it may develop as an idiopathic
kidney disease, without a known cause.
Proteinuria is the most common symptom
of FSGS, but, since proteinuria is
associated with several other kidney
conditions, the doctor cannot diagnose
FSGS on the basis of proteinuria alone.
Biopsy may confirm the presence of
glomerular scarring if the tissue is
taken from the affected section of the
kidney. But finding the affected section
is a matter of chance, especially early
in the disease process, when lesions may
be scattered.
Confirming a
diagnosis of FSGS may require repeat
kidney biopsies. Arriving at a diagnosis
of idiopathic FSGS requires the
identification of focal scarring and the
elimination of possible systemic causes
such as diabetes or an immune response
to infection. Since idiopathic FSGS is,
by definition, of unknown cause, it is
difficult to treat. No universal remedy
has been found, and most patients with
FSGS progress to total kidney failure
over 5 to 20 years. Some patients with
an aggressive form of FSGS reach total
kidney failure in 2 to 3 years.
Treatments involving steroids or other
immunosuppressive drugs appear to help
some patients by decreasing proteinuria
and improving kidney function. But these
treatments are beneficial to only a
minority of those in whom they are
tried, and some patients experience even
poorer kidney function as a result. ACE
inhibitors and ARBs may also be used in
FSGS to decrease proteinuria. Treatment
should focus on controlling blood
pressure and blood cholesterol levels,
factors that may contribute to kidney
scarring.
Other Glomerular
Diseases
Membranous nephropathy,
also called membranous glomerulopathy,
is the second most common cause of the
nephrotic syndrome (proteinuria, edema,
high cholesterol) in U.S. adults after
diabetic nephropathy. Diagnosis of
membranous nephropathy requires a kidney
biopsy, which reveals unusual deposits
of immunoglobulin G and complement C3,
substances created by the body?s immune
system. Fully 75 percent of cases are
idiopathic, which means that the cause
of the disease is unknown. The remaining
25 percent of cases are the result of
other diseases like systemic lupus
erythematosus, hepatitis B or C
infection, or some forms of cancer. Drug
therapies involving penicillamine, gold,
or captopril have also been associated
with membranous nephropathy. About 20 to
40 percent of patients with membranous
nephropathy progress, usually over
decades, to total kidney failure, but
most patients experience either complete
remission or continued symptoms without
progressive kidney failure. Doctors
disagree about how aggressively to treat
this condition, since about 20 percent
of patients recover without treatment.
ACE inhibitors and ARBs are generally
used to reduce proteinuria. Additional
medication to control high blood
pressure and edema is frequently
required. Some patients benefit from
steroids, but this treatment does not
work for everyone. Additional
immunosuppressive medications are
helpful for some patients with
progressive disease.
Minimal
change disease (MCD)
is the diagnosis given when a patient
has the nephrotic syndrome and the
kidney biopsy reveals little or no
change to the structure of glomeruli or
surrounding tissues when examined by a
light microscope. Tiny drops of a fatty
substance called a lipid may be present,
but no scarring has taken place within
the kidney. MCD may occur at any age,
but it is most common in childhood. A
small percentage of patients with
idiopathic nephrotic syndrome do not
respond to steroid therapy. For these
patients, the doctor may recommend a
low-sodium diet and prescribe a diuretic
to control edema. The doctor may
recommend the use of nonsteroidal
anti-inflammatory drugs to reduce
proteinuria. ACE inhibitors and ARBs
have also been used to reduce
proteinuria in patients with
steroid-resistant MCD. These patients
may respond to larger doses of steroids,
more prolonged use of steroids, or
steroids in combination with
immunosuppressant drugs, such as
chlorambucil, cyclophosphamide, or
cyclosporine.
What are renal failure and end-stage
renal disease?
Renal failure is
any acute or chronic loss of kidney
function and is the term used when some
kidney function remains. Total kidney
failure, sometimes called end-stage
renal disease (ESRD), indicates
permanent loss of kidney function.
Depending on the form of glomerular
disease, renal function may be lost in a
matter of days or weeks or may
deteriorate slowly and gradually over
the course of decades.
Acute Renal
Failure
A few forms of
glomerular disease cause very rapid
deterioration of kidney function. For
example, PSGN can cause severe symptoms
(hematuria, proteinuria, edema) within 2
to 3 weeks after a sore throat or skin
infection develops. The patient may
temporarily require dialysis to replace
renal function. This rapid loss of
kidney function is called acute renal
failure (ARF). Although ARF can be
life-threatening while it lasts, kidney
function usually returns after the cause
of the kidney failure has been treated.
In many patients, ARF is not associated
with any permanent damage. However, some
patients may recover from ARF and
subsequently develop CKD.
Chronic Kidney
Disease
Most forms of
glomerular disease develop gradually,
often causing no symptoms for many
years. CKD is the slow, gradual loss of
kidney function. Some forms of CKD can
be controlled or slowed down. For
example, diabetic nephropathy can be
delayed by tightly controlling blood
glucose levels and using ACE inhibitors
and ARBs to reduce proteinuria and
control blood pressure. But CKD cannot
be cured. Partial loss of renal function
means that some portion of the patient?s
nephrons have been scarred, and scarred
nephrons cannot be repaired. In many
cases, CKD leads to total kidney
failure.
Total Kidney
Failure
To stay alive, a
patient with total kidney failure must
go on dialysis?hemodialysis or
peritoneal dialysis?or receive a new
kidney through transplantation. Patients
with CKD who are approaching total
kidney failure should learn as much
about their treatment options as
possible so they can make an informed
decision when the time comes. With the
help of dialysis or transplantation,
many people continue to lead full,
productive lives after reaching total
kidney failure.
Points to Remember
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The kidneys
filter waste and extra fluid from
the blood.
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The filtering
process takes place in the nephron,
where microscopic blood vessel
filters, called glomeruli, are
attached to fluid-collecting
tubules.
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A number of
different disease processes can
damage the glomeruli and thereby
cause kidney failure.
Glomerulonephritis and
glomerulosclerosis are broad terms
that include many forms of damage to
the glomeruli.
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Some forms of
kidney failure can be slowed down,
but scarred glomeruli can never be
repaired.
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Treatment for the
early stages of kidney failure
depends on the disease causing the
damage.
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Early signs of
kidney failure include blood or
protein in the urine and swelling in
the hands, feet, abdomen, or face.
Kidney failure may be silent for
many years.
The Nephrotic
Syndrome
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The nephrotic
syndrome is a condition marked by
very high levels of protein in the
urine; low levels of protein in the
blood; swelling, especially around
the eyes, feet, and hands; and high
cholesterol.
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The nephrotic
syndrome is a set of symptoms, not a
disease in itself. It can occur with
many diseases, so prevention relies
on controlling the diseases that
cause it.
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Treatment of the
nephrotic syndrome focuses on
identifying and treating the
underlying cause, if possible, and
reducing high cholesterol, blood
pressure, and protein in the urine
through diet, medication, or both.
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The nephrotic
syndrome may go away once the
underlying cause, if known, is
treated. However, often a kidney
disease is the underlying cause and
cannot be cured. In these cases, the
kidneys may gradually lose their
ability to filter wastes and excess
water from the blood. If kidney
failure occurs, the patient will
need to be on dialysis or have a
kidney transplant.
Definitions
Signs and
Symptoms of Glomerulonephritis
edema
(eh-DEE-muh):
Swelling caused by the accumulation of
fluid in cells and tissues. In kidney
failure, fluid may collect in the feet,
hands, abdomen, or face.
hematuria (HEE-muh-TOOR-ee-uh):
Blood in the urine. Blood may turn the
urine pink or cola-colored.
hypoproteinemia
(HY-po-PRO-teen-EE-mee-uh):
Reduced levels of protein in the blood.
proteinuria (PRO-tee-NOOR-ee-uh):
Large amounts of protein in the urine.
uremia
(yoo-REE-mee-uh):
Accumulation of urea and other wastes in
the blood. These wastes, which become
toxic in large amounts, are normally
eliminated through urination.
Diseases and
Conditions
autoimmune (AW-toh-ih-MYOON) disease:
A disease in which the body?s own
disease-fighting cells attack the body
itself.
hypertension (HY-per-TEN-shun):
High blood pressure, a condition that
can cause kidney damage or be caused by
kidney disease.
idiopathic (id-ee-o-PATH-ik) disease:
A disease that occurs without a known
cause.
nephrotoxic (NEF-ro-TOKS-ik):
Damaging to the kidneys.
sclerotic (skleh-ROT-ik) disease:
A disease in which tissues become
hardened or scarred.
systemic
(sis-TEM-ik) disease:
A disease that affects multiple parts of
the body, often as a result of
substances circulating in the blood.
Treatments and
Procedures
biopsy
(BY-op-see):
A procedure in which a needle is used to
obtain small pieces of tissue from an
organ for examination under different
types of microscopes, each of which
shows a different aspect of the tissue.
dialysis
(dy-AL-ih-sis):
A medical treatment that removes wastes
and extra fluid from the blood after the
kidneys have stopped working.
immunosuppressant
(im-YOON-oh-suh-PRESS-unt):
A medicine given to block the body?s
immune system.
plasmapheresis (PLAZ-muh-fer-EE-sis):
A medical treatment in which the blood
is treated outside the body to remove
harmful antibodies, and then returned to
the patient.
Kidney Parts and
Organic Substances
antibody
(AN-tee-BOD-ee):
A molecule that protects the body
against disease by attacking foreign
tissues or organisms. Antibodies are
also called immunoglobulins.
antigen
(AN-tih-jen):
A substance that triggers a response
from the body?s immune system.
autoantibody (AW-toh-AN-tee-bod-ee):
An antibody that attacks the body
itself.
creatinine (kree-AT-ih-nin):
A waste product in the blood that
results from the normal breakdown of
muscle. Healthy kidneys filter
creatinine from the blood.
glomerulus (gloh-MEHR-yoo-lus):
The tiny cluster of looping blood
vessels in the nephron, where wastes are
filtered from the blood.
lipid
(LIP-id):
One of several fatty substances used in
cells. Excess lipids in the blood may
result in harmful deposits in blood
vessels.
nephron
(NEF-rahn):
One of a million tiny filtering units in
each kidney. Each nephron is made up of
both a glomerulus and a fluid-collecting
tubule that processes extra water and
wastes.
protein
(PRO-teen):
A substance found in food and used by
the body to grow, repair tissue, and
fight disease.
urea
(yoo-REE-uh):
A waste material found in blood after
protein has been broken down. Healthy
kidneys remove urea from the blood.
Damaged kidneys may allow urea to
accumulate in the blood, thus causing
uremia.
