Chapter 8: Intestinal Ischemia |
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7.1 Etiology In contrast to mesenteric ischemia, where the cause of the disease is occlusion of major vessels, in nongangrenous ischemic bowel disease the hypo-oxygenation is caused by hypoperfusion of the gut wall microcirculation. Only occasionally is there secondary occlusion of intramural vessels. Many causes may precipitate this disorder. Hypoperfusion is most commonly caused by vascular diseases - e.g., collagen disease, vasculitis, diabetes, atherosclerosis - or by increased viscosity of the blood in sickle cell disease or polycythemia vera. Acute hypotension due to hemorrhage, myocardial infarct, congestive heart failure, sepsis or vasoconstricting drugs may precipitate local ischemia in patients who already have impaired local circulation. Because of an adequate collateral circulation, localization is usually segmental. The necrosis of the gut wall is rarely transmural, and as a result, peritonitis is a rare complication. In the small bowel nongangrenous ischemic bowel disease manifests as "focal segmental ischemia" and in the colon as "nongangrenous ischemic colitis." A list of the more common causes of nonocclusive ischemic bowel disease is provided in Table 1. TABLE 1. Causes of nonocclusive ischemic bowel disease A. Acute diminution of intramural blood flow 1. Small vessel disease 2. Nonocclusive hypoperfusion 1. Increased motility 2. Increased intraluminal pressure C. Idiopathic (spontaneous)
Ischemia to short segments of the small bowel results in a variable clinical course that depends on the severity of the infarct. For short segment involvement there is usually appropriate collateral circulation, and thus the disease involves only the mucosa and submucosal tissues. Limited necrosis may heal completely. Ongoing repeated injury may cause chronic enteritis, almost indistinguishable from Crohn's disease. In some patients the necrotic ulcer may lead to late stricture formation. Occasionally the process may become transmural, resulting in peritonitis. Diagnosis is difficult, as the symptoms may be those of chronic recurrent abdominal pain, bowel obstruction or frank peritonitis. Unless there is complete spontaneous resolution, the treatment of strictures and persistent ulcers is usually surgical. The diagnosis is often made only on histology of the resected small bowel.
7.3.1 PATHOGENESIS There
are two major forms of colonic ischemia: gangrenous (transmural) and
nongangrenous colitis (disease contained within the colonic wall).
These are in fact two different diseases, with different etiologies
and clinical courses, and require different approaches to their
management. Gangrenous ischemic colitis is caused by obstruction of
the major mesenteric vessels and is discussed in Section 4 (see Figure
1). Occasionally, transmural gangrene may develop when nongangrenous
ischemic colitis slowly progresses to transmural necrosis. The
recognition and management of this complication of the originally
nongangrenous disease is crucial, and as discussed below, depends on
careful ongoing observation of the patient with nongangrenous ischemic
colitis.
In contrast to the rarity of nonocclusive ischemia
of the small bowel is the relative frequency of local vascular
hypoperfusion of the colon. The cause of this relative frequency may
be related to the following factors: In comparison to the small
intestine, the colon receives less blood, has fewer vascular
collaterals, has susceptible "watershed areas" and possesses
an ongoing forceful motor activity. Elevated intramural pressure
during increased motility in patients with constipation, diverticular
disease and cancer of the colon may lead to diminished gut wall blood
flow. Similarly, distention with air during colonoscopy or barium
enema may temporarily reduce blood flow to the colon. The large bowel
also has a different neuroendocrine control. Evidence in our
laboratory has indicated that the vessels of the canine colon respond
more vigorously to hypotension than those of the small intestine and
that contrary to the latter, in the colon the major local
vasoconstrictory substance is angiotensin.
The
classic clinical presentation is characterized by a sudden onset of
severe crampy abdominal pain, diarrhea mixed with bright red blood,
and occasionally melena. Physical examination may reveal a distended
abdomen. Bowel sounds are present and there are no signs of peritoneal
involvement. The patient is usually elderly and may show signs of one
of the associated diseases such as hypotension, congestive heart
failure and atherosclerosis. Under specific conditions, nongangrenous
ischemic colitis can also occur in the young. This is often due to
iatrogenic or patient-induced causes such as contraceptive medication,
nonsteroidal anti-inflammatory agents, cocaine abuse, verapamil
overdose, etc. (for details see Table
1). In
the elderly, the specific event that precipitated the attack
occasionally cannot be determined. The early clinical presentation may
be so similar to that of infectious colitis, ulcerative colitis,
Crohn's colitis and pseudomembranous colitis that the diagnosis can be
established only by exclusion of infection, including Clostridium
difficile, and by demonstrating the classic radiographic (Figure
5 and Figure
6) and/or colonoscopic (Figure
7) findings of ischemic colitis. Because large vessels
are never involved, angiography has no place in the diagnosis of
nongangrenous ischemic colitis.
Radiographic and colonoscopic investigations have
to be carried out within 24-48 hours of the onset of the disease, as
the typical findings tend to disappear and are rapidly replaced by
nonspecific signs. The first radiologic examination should be an
abdominal survey film (Figure
5), which may demonstrate the classic intramural
hemorrhage-induced thumb-printing in an air-filled segment of the
colon. This finding, however, may not always be diagnostic, because
occasionally it can be mimicked by mucosal and submucosal edema caused
by severe inflammatory processes. Colonic involvement is usually
segmental in ischemic colitis. Although any part of the colon may be
affected, the "watershed" areas of the splenic flexure and
of the recto-sigmoid junction are most commonly involved.
Thumb-printing can be demonstrated by barium enema (Figure
6), but differentiation between edema and submucosal
hemorrhage can be done only by colonoscopy, where hemorrhage can be
recognized as large dark red submucosal blebs (Figure
7). Because distention of the colon with air may compress
intramural blood vessels and thus further decrease blood flow, barium
enema and colonoscopy must be carried out carefully with minimal air
insufflation. After 24-48 hours, the hemorrhage resolves and the
mucosa becomes necrotic. If colonoscopy is done at this stage, the
endoscopist may be unable to differentiate the necrosis and
ulcerations resulting from ischemic colitis from those caused by
Crohn's disease or pseudomembranous enterocolitis. The pathologist
reviewing biopsies taken a few days after the onset of the disease may
have similar difficulties. Not infrequently, only time will tell
whether the patient has inflammatory bowel disease (IBD) or ischemia.
It is not impossible that some elderly patients with what is thought
to be late-onset IBD or young women on contraceptive medication who
are thought to have Crohn's are actually suffering from ischemic
colitis.
The disease can progress in four different ways (Figure
1). Mild disease may resolve spontaneously. In patients
with involvement of only small segments, the symptoms and physical
findings subside within 24-48 hours and complete resolution can occur
within two to three weeks. In some, the disease does not resolve and
may progress to ongoing or recurrent chronic colitis. As the
pathological response of colonic tissue to chronic injury is
restricted to a very few modalities, such as infiltration with
leukocytes, crypt abscess, hemorrhage, necrosis, ulceration and
regeneration of crypts, the pathologist may also have difficulty in
differentiating ongoing ischemic colitis from Crohn's disease.
Hemosiderin, a sign of previous bleeding, is often considered a
typical manifestation of ischemic colitis (Figure
8). Unfortunately, this finding is not restricted to
ischemic colonic disease, as it can be found in any type of colitis,
including IBD, if hemorrhage has occurred sometime in the past.
Once ischemic colitis has become chronic, it may
resolve, relapse or progress to deeper intramural inflammation and
necrosis. In severe disease the patient may exhibit toxic symptoms
with chills, fever, severe bloody diarrhea and abdominal distention
with diminished bowel sounds. The patient may develop leukocytosis,
anemia, elevated platelet count and electrolyte disturbances. If the
necrosis does not progress further, the process will heal first with
granulation tissue, which is replaced by fibrous tissue, scarring and
finally a stricture. In some instances the disease progresses to toxic
megacolon, and if the intramural necrosis becomes transmural, acute
peritonitis will ensue. This progression may take only a few hours or
several days to develop, and as the patient must be surgically treated
well before peritonitis develops, this process must be detected early
by careful, sometimes hourly, follow-up of the patient.
Infectious
enteropathies, IBD and other precipitating causes such as
diverticulitis, cancer, etc. have to be detected and appropriately
treated. Therapy for ischemic colitis can be considered under the
following three categories: (1) nonspecific supportive therapy, (2)
specific medical treatment and (3) surgical therapy.
Nonspecific supportive therapy. Fluid and
electrolyte balance must be carefully maintained. Oral intake should
be restricted according to the severity of disease. Well-nourished
patients can be maintained for a few days without specific nutritional
support, except for what they receive in intravenous solutions.
Severely undernourished patients may require enteral nutrition, or if
this is poorly tolerated, total parenteral nutrition (TPN). Bleeding
is rarely severe enough to require blood transfusion, but if anemia is
present it may have to be corrected even in elderly patients with poor
cardiovascular reserve. This requires careful balancing, so that an
already precariously maintained circulation is not overloaded.
Usually, the patient will request medication to relieve diarrhea and
abdominal pain. However, the use of analgesics, antispasmodic or
antidiarrheal agents is contraindicated, because they may lead to an
inert bowel, which may result in a toxic megacolon.
As the patient improves, a low-residue diet may be
slowly started. If this is not well tolerated, enteric feeding may be
required. However, in some patients the diarrhea and abdominal pain
may become worse on enteric nutrition. This may be overcome with the
use of an iso-osmotic product, dilution of the solution and constant
slow administration over 24 hours.
Patients have to be carefully followed to detect
deterioration, as they may progress to toxic megacolon or perforation.
In patients who show signs of deterioration, the use of antibiotics
may be justified. If there is further progression and the patient
develops increasing peritoneal signs, surgery becomes imperative, even
in an elderly patient who appears to be a poor surgical risk.
Specific medical treatment. There is no need
for specific therapy for mild self-limiting disease. For chronic
ongoing disease there is no proven specific therapy and no
experimental data exist to assess the usefulness of any of the drugs
utilized in IBD. Because of the relatively low incidence of ischemic
colitis, up to now it has not been possible to design a valid
prospective double-blind study to assess the efficacy of these drugs.
However, patients with long-standing progressive disease have been
treated with variable results using 5-aminosalicylic acid (5-ASA) by
oral and/or (depending on the location of the disease) rectal
administration. For patients who do not respond to 5-ASA, a trial with
oral or local steroids may be attempted. There is no experience with
metronidazole or immunosuppressive agents. In contrast to acute
mesenteric arterial occlusion, there is no evidence in nongangrenous
ischemic colitis that vasodilators (papaverine, ACE inhibitors,
nitrites, etc.) are useful. By the time the patient is seen the
intramural ischemic injury has already occurred and vasodilators
cannot reverse the pathological changes. Treatment of heart disease,
change of digitalis to other medication, discontinuation of estrogens,
management of diabetes, recognition and treatment of vasculitis,
polycythemia, etc., may not necessarily alter the outcome of already
established chronic disease, but may prevent future recurrences.
Surgical therapy. Indications for immediate
surgery are toxic megacolon and transmural necrosis leading to
peritoneal signs. Usually within six months after onset of the disease
a considerable number of patients with severe ischemic colitis will
develop strictures. They present with symptoms of partial obstruction.
One should attempt colonoscopic dilation, but if this fails
stricturoplasty or surgical resection may be necessary. |
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