Program Operations Manual System (POMS)
TN 1 (01-17)
DI 34225.009 Digestive Listings from 6/12/15 to 1/16/17
105.00 DIGESTIVE SYSTEM (Effective Date: 06/12/2015)
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A.
What kinds of disorders do we consider in the digestive system?
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Disorders of the digestive system include gastrointestinal hemorrhage, hepatic (liver)
dysfunction, inflammatory bowel disease, short bowel syndrome, and malnutrition. They
may also lead to complications, such as obstruction, or be accompanied by manifestations
in other body systems. Congenital abnormalities involving the organs of the gastrointestinal
system may interfere with the ability to maintain adequate nutrition, growth, and
development.
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B.
What documentation do we need?
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We need a record of your medical evidence, including clinical and laboratory findings.
The documentation should include appropriate medically acceptable imaging studies
and reports of endoscopy, operations, and pathology, as appropriate to each listing,
to document the severity and duration of your digestive disorder. We may also need
assessments of your growth and development. Medically acceptable imaging includes,
but is not limited to, x-ray imaging, sonography, computerized axial tomography (CAT
scan), magnetic resonance imaging (MRI), and radionuclide scans. Appropriate means that the technique used is the proper one to support the evaluation and diagnosis
of the disorder. The findings required by these listings must occur within the period
we are considering in connection with your application or continuing disability review.
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C.
How do we consider the effects of treatment?
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1. Digestive disorders frequently respond to medical or surgical treatment; therefore,
we generally consider the severity and duration of these disorders within the context
of the prescribed treatment.
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2. We assess the effects of treatment, including medication, therapy, surgery, or
any other form of treatment you receive, by determining if there are improvements
in the symptoms, signs, and laboratory findings of your digestive disorder. We also
assess any side effects of your treatment that may further limit your functioning.
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3. To assess the effects of your treatment, we may need information about:
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a. The treatment you have been prescribed (for example, the type of medication or
therapy, or your use of parenteral (intravenous) nutrition or supplemental enteral
nutrition via a gastrostomy);
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b. The dosage, method, and frequency of administration;
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c. Your response to the treatment;
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d. Any adverse effects of such treatment; and
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e. The expected duration of the treatment.
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4. Because the effects of treatment may be temporary or long-term, in most cases we
need information about the impact of your treatment, including its expected duration
and side effects, over a sufficient period of time to help us assess its outcome.
When adverse effects of treatment contribute to the severity of your impairment(s),
we will consider the duration or expected duration of the treatment when we assess
the duration of your impairment(s).
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5. If you need parenteral (intravenous) nutrition or supplemental enteral nutrition
via a gastrostomy to avoid debilitating complications of a digestive disorder, this
treatment will not, in itself, indicate that you have marked and severe functional
limitations. The exceptions are 105.07, short bowel syndrome, and 105.10, for children
who have not attained age 3 and who require supplemental daily enteral feedings via
a gastrostomy (see 105.00F and 105.00H).
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6. If you have not received ongoing treatment or have not had an ongoing relationship
with the medical community despite the existence of a severe impairment(s), we will
evaluate the severity and duration of your digestive impairment on the basis of current
medical and other evidence in your case record. If you have not received treatment,
you may not be able to show an impairment that meets the criteria of one of the digestive
system listings, but your digestive impairment may medically equal a listing or functionally
equal the listings.
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D.
How do we evaluate chronic liver disease?
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1. General. Chronic liver disease is characterized by liver cell necrosis, inflammation, or scarring (fibrosis or cirrhosis),
due to any cause, that persists for more than 6 months. Chronic liver disease may
result in portal hypertension, cholestasis (suppression of bile flow), extrahepatic
manifestations, or liver cancer. (We evaluate liver cancer under 113.03.) Significant
loss of liver function may be manifested by hemorrhage from varices or portal hypertensive
gastropathy, ascites (accumulation of fluid in the abdominal cavity), hydrothorax
(ascitic fluid in the chest cavity), or encephalopathy. There can also be progressive
deterioration of laboratory findings that are indicative of liver dysfunction. Liver
transplantation is the only definitive cure for end stage liver disease (ESLD).
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2. Examples of chronic liver disease include, but are not limited to, biliary atresia, chronic hepatitis, non-alcoholic
steatohepatitis (NASH), primary biliary cirrhosis (PBC), primary sclerosing cholangitis
(PSC), autoimmune hepatitis, hemochromatosis, drug-induced liver disease, Wilson’s
disease, and serum alpha-1 antitrypsin deficiency. Children can also have congenital
abnormalities of abdominal organs or inborn metabolic disorders that result in chronic
liver disease. Acute hepatic injury is frequently reversible as in viral, drug-induced,
toxin-induced, and ischemic hepatitis. In the absence of evidence of a chronic impairment,
episodes of acute liver disease do not meet 105.05.
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3. Manifestations of chronic liver disease.
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a. Symptoms may include, but are not limited to, pruritis (itching), fatigue, nausea, loss of
appetite, or sleep disturbances. Children can also have associated developmental delays
or poor school performance. Symptoms of chronic liver disease may have a poor correlation
with the severity of liver disease and functional ability.
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b. Signs may include, but are not limited to, jaundice, enlargement of the liver and spleen,
ascites, peripheral edema, and altered mental status.
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c. Laboratory findings may include, but are not limited to, increased liver enzymes, increased serum total
bilirubin, increased ammonia levels, decreased serum albumin, and abnormal coagulation
studies, such as increased International Normalized Ratio (INR) or decreased platelet
counts. Abnormally low serum albumin or elevated INR levels indicate loss of synthetic
liver function, with increased likelihood of cirrhosis and associated complications.
However, other abnormal lab tests, such as liver enzymes, serum total bilirubin, or
ammonia levels, may have a poor correlation with the severity of liver disease and
functional ability. A liver biopsy may demonstrate the degree of liver cell necrosis,
inflammation, fibrosis, and cirrhosis. If you have had a liver biopsy, we will make
every reasonable effort to obtain the results; however, we will not purchase a liver
biopsy. Imaging studies (CAT scan, ultrasound, MRI) may show the size and consistency
(fatty liver, scarring) of the liver and document ascites (see 105.00D6).
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4. Chronic viral hepatitis infections.
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(i) Chronic viral hepatitis infections are commonly caused by hepatitis C virus (HCV), and to a lesser extent,
hepatitis B virus (HBV). Usually, these are slowly progressive disorders that persist
over many years during which the symptoms and signs are typically nonspecific, intermittent,
and mild (for example, fatigue, difficulty with concentration, or right upper quadrant
pain). Laboratory findings (liver enzymes, imaging studies, liver biopsy pathology)
and complications are generally similar in HCV and HBV. The spectrum of these chronic
viral hepatitis infections ranges widely and includes an asymptomatic state; insidious
disease with mild to moderate symptoms associated with fluctuating liver tests; extrahepatic
manifestations; cirrhosis, both compensated and decompensated; ESLD with the need
for liver transplantation; and liver cancer. Treatment for chronic viral hepatitis
infections varies considerably based on age, medication tolerance, treatment response,
adverse effects of treatment, and duration of the treatment. Comorbid disorders, such
as HIV infection, may affect the clinical course of viral hepatitis infection(s) or
may alter the response to medical treatment.
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(ii) We evaluate all types of chronic viral hepatitis infections under 105.05 or any
listing in an affected body system(s). If your impairment(s) does not meet or medically
equal a listing, we will consider the effects of your hepatitis when we assess whether
your impairment(s) functionally equals the listings.
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b. Chronic hepatitis B virus (HBV) infection.
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(i) Chronic HBV infection is diagnosed by the detection of hepatitis B surface antigen (HBsAg) in the blood
for at least 6 months. In addition, detection of the hepatitis B envelope antigen
(HBeAg) suggests an increased likelihood of progression to cirrhosis and ESLD.
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(ii) The therapeutic goal of treatment is to suppress HBV replication and thereby
prevent progression to cirrhosis and ESLD. Treatment usually includes a combination
of interferon injections and oral antiviral agents. Common adverse effects of treatment
are the same as noted in 105.00D4c(ii) for HCV, and generally end within a few days
after treatment is discontinued.
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c. Chronic hepatitis C virus (HCV) infection.
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(i) Chronic HCV infection is diagnosed by the detection of hepatitis C viral RNA in the blood for at least 6
months. Documentation of the therapeutic response to treatment is also monitored by
the quantitative assay of serum HCV RNA (‘‘HCV viral load’’). Treatment usually includes
a combination of interferon injections and oral ribavirin; whether a therapeutic response
has occurred is usually assessed after 12 weeks of treatment by checking the HCV viral
load. If there has been a substantial reduction in HCV viral load (also known as early
viral response, or EVR), this reduction is predictive of a sustained viral response
with completion of treatment. Combined therapy is commonly discontinued after 12 weeks
when there is no early viral response, since in that circumstance there is little
chance of obtaining a sustained viral response (SVR). Otherwise, treatment is usually
continued for a total of 48 weeks.
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(ii) Combined interferon and ribavirin treatment may have significant adverse effects
that may require dosing reduction, planned interruption of treatment, or discontinuation
of treatment. Adverse effects may include: Anemia (ribavirin-induced hemolysis), neutropenia,
thrombocytopenia, fever, cough, fatigue, myalgia, arthralgia, nausea, loss of appetite,
pruritis, and insomnia. Behavioral side effects may also occur. Influenza-like symptoms
are generally worse in the first 4 to 6 hours after each interferon injection and
during the first weeks of treatment. Adverse effects generally end within a few days
after treatment is discontinued.
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d. Extrahepatic manifestations of HBV and HCV. In addition to their hepatic manifestations, both HBV and HCV may have significant
extrahepatic manifestations in a variety of body systems. These include, but are not
limited to: Keratoconjunctivitis (sicca syndrome), glomerulonephritis, skin disorders
(for example, lichen planus, porphyria cutanea tarda), neuropathy, and immune dysfunction
(for example, cryoglobulinemia, Sjögren’s syndrome, and vasculitis). The extrahepatic
manifestations of HBV and HCV may not correlate with the severity of your hepatic
impairment. If your impairment(s) does not meet or medically equal a listing in an
affected body system(s), we will consider the effects of your extrahepatic manifestations
when we determine whether your impairment(s) functionally equals the listings.
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5. Gastrointestinal hemorrhage (105.02 and 105.05A). Gastrointestinal hemorrhaging can result in hematemesis (vomiting
of blood), melena (tarry stools), or hematochezia (bloody stools). Under 105.02, the
required transfusions of at least 10 cc of blood/kg of body weight must be at least
30 days apart and occur at least three times during a consecutive 6-month period.
Under 105.05A, hemodynamic instability is diagnosed with signs such as pallor (pale skin), diaphoresis (profuse perspiration),
rapid pulse, low blood pressure, postural hypotension (pronounced fall in blood pressure
when arising to an upright position from lying down) or syncope (fainting). Hemorrhaging
that results in hemodynamic instability is potentially life threatening and therefore
requires hospitalization for transfusion and supportive care. Under 105.05A, we require
only one hospitalization for transfusion of at least 10 cc of blood/kg of body weight.
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6. Ascites or hydrothorax (105.05B) indicates significant loss of liver function due to chronic liver disease.
We evaluate ascites or hydrothorax that is not attributable to other causes under
105.05B. The required findings must be present on at least two evaluations at least
60 days apart within a consecutive 6-month period and despite continuing treatment
as prescribed.
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7. Spontaneous bacterial peritonitis (105.05C) is an infectious complication of chronic liver disease. It is diagnosed
by ascitic peritoneal fluid that is documented to contain an absolute neutrophil count
of at least 250 cells/mm3. The required finding in 105.05C is satisfied with one evaluation documenting peritoneal
fluid infection. We do not evaluate other causes of peritonitis that are unrelated
to chronic liver disease, such as tuberculosis, malignancy, and perforated bowel,
under this listing. We evaluate these other causes of peritonitis under the appropriate
body system listings.
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8. Hepatorenal syndrome (105.05D) is defined as functional renal failure associated with chronic liver disease
in the absence of underlying kidney pathology. Hepatorenal syndrome is documented
by elevation of serum creatinine, marked sodium retention, and oliguria (reduced urine
output). The requirements of 105.05D are satisfied with documentation of any one of
the three laboratory findings on one evaluation. We do not evaluate known causes of
renal dysfunction, such as glomerulonephritis, tubular necrosis, drug-induced renal
disease, and renal infections, under this listing. We evaluate these other renal impairments
under 106.00ff.
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9. Hepatopulmonary syndrome (105.05E) is defined as arterial deoxygenation (hypoxemia) that is associated with
chronic liver disease due to intrapulmonary arteriovenous shunting and vasodilatation,
in the absence of other causes of arterial deoxygenation. Clinical manifestations
usually include dyspnea, orthodeoxia (increasing hypoxemia with erect position), platypnea
(improvement of dyspnea with flat position), cyanosis, and clubbing. The requirements
of 105.05E are satisfied with documentation of any one of the findings on one evaluation.
In 105.05E1, we require documentation of the altitude of the testing facility because
altitude affects the measurement of arterial oxygenation. We will not purchase the
specialized studies described in 105.05E2; however, if you have had these studies
at a time relevant to your claim, we will make every reasonable effort to obtain the
reports for the purpose of establishing whether your impairment meets 105.05E2.
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10. Hepatic encephalopathy (105.05F).
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a. General. Hepatic encephalopathy usually indicates severe loss of hepatocellular function. We
define hepatic encephalopathy under 105.05F as a recurrent or chronic neuropsychiatric
disorder, characterized by abnormal behavior, cognitive dysfunction, altered state
of consciousness, and ultimately coma and death. The diagnosis is established by changes
in mental status associated with fleeting neurological signs, including ‘‘flapping
tremor’’ (asterixis), characteristic electroencephalographic (EEG) abnormalities,
or abnormal laboratory values that indicate loss of synthetic liver function. We will
not purchase the EEG testing described in 105.05F3b. However, if you have had this
test at a time relevant to your claim, we will make every reasonable effort to obtain
the report for the purpose of establishing whether your impairment meets 105.05F.
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b. Acute encephalopathy. We will not evaluate your acute encephalopathy under 105.05F if it results from conditions
other than chronic liver disease, such as vascular events and neoplastic diseases.
We will evaluate these other causes of acute encephalopathy under the appropriate
body system listings.
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11. End stage liver disease (ESLD) documented by scores from the SSA Chronic Liver Disease
(SSA CLD) calculation (105.05G1) and SSA Chronic Liver Disease-Pediatric (SSA CLD-P)
calculation (105.05G2).
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(i) If you are age 12 or older, we will use the SSA CLD score to evaluate your ESLD
under 105.05G1. We explain how we calculate the SSA CLD score in a(ii) through a(vii)
of this section.
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(ii) To calculate the SSA CLD score, we use a formula that includes three laboratory
values: Serum total bilirubin (mg/dL), serum creatinine (mg/dL), and International
Normalized Ratio (INR). The formula for the SSA CLD score calculation is:
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9.57 [Loge (serum creatinine mg/dL)]
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+3.78 [Loge (serum total bilirubin mg/dL)]
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(iii) When we indicate ‘‘Loge’’ in the formula for the SSA CLD score calculation, we mean the ‘‘base e logarithm’’ or ‘‘natural logarithm’’ (ln) of a numerical laboratory value, not the
‘‘base 10 logarithm’’ or ‘‘common logarithm’’ (log) of the laboratory value, and not
the actual laboratory value. For an example of SSA CLD calculation, see 5.00D11c.
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(iv) For any SSA CLD score calculation, all of the required laboratory values must
have been obtained within 30 days of each other. If there are multiple laboratory
values within the 30-day interval for any given laboratory test (serum total bilirubin,
serum creatinine, or INR), we will use the highest value for the SSA CLD score calculation.
We will round all laboratory values less than 1.0 up to 1.0.
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(v) Listing 105.05G requires two SSA CLD scores. The laboratory values for the second
SSA CLD score calculation must have been obtained at least 60 days after the latest
laboratory value for the first SSA CLD score and within the required 6-month period.
We will consider the date of each SSA CLD score to be the date of the first laboratory
value used for its calculation.
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(vi) If you are in renal failure or on dialysis within a week of any serum creatinine
test in the period used for the SSA CLD calculation, we will use a serum creatinine
of 4, which is the maximum serum creatinine level allowed in the calculation, to calculate
your SSA CLD score.
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(vii) If you have the two SSA CLD scores required by 105.05G1, we will find that your
impairment meets the criteria of the listing from at least the date of the first SSA
CLD score.
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(i) If you have not attained age 12, we will use the SSA CLD-P score to evaluate your
ESLD under 105.05G2. We explain how we calculate the SSA CLD-P score in b(ii) through
b(vii) of this section.
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(ii) To calculate the SSA CLD-P score, we use a formula that includes four parameters:
Serum total bilirubin (mg/dL), International Normalized Ratio (INR), serum albumin
(g/dL), and whether growth failure is occurring. The formula for the SSA CLD-P score
calculation is:
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4.80 [Loge (serum total bilirubin mg/dL)]
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-6.87 [Loge (serum albumin g/dL)]
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+6.67 if the child has growth failure (<-2 standard deviations for weight or height)
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(iii) When we indicate ‘‘Loge’’ in the formula for the SSA CLD-P score calculation, we mean the ‘‘base e logarithm’’ or ‘‘natural logarithm’’ (ln) of a numerical laboratory value, not the
‘‘base 10 logarithm’’ or ‘‘common logarithm’’ (log) of the laboratory value, and not
the actual laboratory value. For example, if a female child is 4.0 years old, has
a current weight of 13.5 kg (10th percentile for age) and height of 92 cm (less than the third percentile for age),
and has laboratory values of serum total bilirubin 2.2 mg/dL, INR 1.0, and serum albumin
3.5 g/dL, we will compute the SSA CLD-P score as follows:
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4.80 [Loge (serum total bilirubin 2.2 mg/dL) = 0.788]
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+18.57 [Loge (INR 1.0) = 0]
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-6.87 [Loge (serum albumin 3.5 g/dL) =1.253]
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= 3.78 + 0 -8.61 + 6.67= 1.84, which is then rounded to an SSACLD-P score of 2.
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(iv) For any SSA CLD-P score calculation, all of the required laboratory values (serum
total bilirubin, INR, or serum albumin) must have been obtained within 30 days of
each other. We will not purchase INR values for children who have not attained age
12. If there is no INR value for a child under 12 within the applicable time period,
we will use an INR value of 1.1 to calculate the SSA CLD-P score. If there are multiple
laboratory values within the 30-day interval for any given laboratory test, we will
use the highest serum total bilirubin and INR values and the lowest serum albumin
value for the SSA CLD-P score calculation. We will round all laboratory values less
than 1.0 up to 1.0.
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(v) The weight and length/height measurements used for the calculation must be obtained
from one evaluation within the same 30-day period as in D11b(iv).
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(vi) Listing 105.05G2 requires two SSA CLD-P scores. The laboratory values for the
second SSA CLD-P score calculation must have been obtained at least 60 days after
the latest laboratory value for the first SSA CLD-P score and within the required
6-month period. We will consider the date of each SSA CLD-P score to be the date of
the first laboratory value used for its calculation.
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(vii) If you have the two SSA CLD-P scores required by listing 105.05G2, we will find
that your impairment meets the criteria of the listing from at least the date of the
first SSA CLD-P score.
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12. Extrahepatic biliary atresia (EBA) (105.05H) usually presents in the first 2 months of life with persistent jaundice.
The impairment meets 105.05H if the diagnosis of EBA is confirmed by liver biopsy
or intraoperative cholangiogram that shows obliteration of the extrahepatic biliary
tree. EBA is usually surgically treated by portoenterostomy (for example, Kasai procedure).
If this surgery is not performed in the first months of life or is not completely
successful, liver transplantation is indicated. If you have had a liver transplant,
we will evaluate your impairment under 105.09.
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13. Liver transplantation (105.09) may be performed for metabolic liver disease, progressive liver failure,
life-threatening complications of liver disease, hepatic malignancy, and acute fulminant
hepatitis (viral, drug-induced, or toxin-induced). We will consider you to be disabled
for 1 year from the date of the transplantation. Thereafter, we will evaluate your
residual impairment(s) by considering the adequacy of post-transplant liver function,
the requirement for post-transplant antiviral therapy, the frequency and severity
of rejection episodes, comorbid complications, and all adverse treatment effects.
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E.
How do we evaluate inflammatory bowel disease (IBD)?
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1. Inflammatory bowel disease (105.06) includes, but is not limited to, Crohn’s disease and ulcerative colitis.
These disorders, while distinct entities, share many clinical, laboratory, and imaging
findings, as well as similar treatment regimens. Remissions and exacerbations of variable
duration are the hallmark of IBD. Crohn’s disease may involve the entire alimentary
tract from the mouth to the anus in a segmental, asymmetric fashion. Obstruction,
stenosis, fistulization, perineal involvement, and extraintestinal manifestations
are common. Crohn’s disease is rarely curable and recurrence may be a lifelong problem,
even after surgical resection. In contrast, ulcerative colitis only affects the colon.
The inflammatory process may be limited to the rectum, extend proximally to include
any contiguous segment, or involve the entire colon. Ulcerative colitis may be cured
by total colectomy.
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2. Symptoms and signs of IBD include diarrhea, fecal incontinence, rectal bleeding,
abdominal pain, fatigue, fever, nausea, vomiting, arthralgia, abdominal tenderness,
palpable abdominal mass (usually inflamed loops of bowel) and perineal disease. You
may also have signs or laboratory findings indicating malnutrition, such as weight
loss, edema, anemia, hypoalbuminemia, hypokalemia, hypocalcemia, or hypomagnesemia.
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3. IBD may be associated with significant extraintestinal manifestations in a variety
of body systems. These include, but are not limited to, involvement of the eye (for
example, uveitis, episcleritis, iritis); hepatobiliary disease (for example, gallstones,
primary sclerosing cholangitis); urologic disease (for example, kidney stones, obstructive
hydronephrosis); skin involvement (for example, erythema nodosum, pyoderma gangrenosum);
or non-destructive inflammatory arthritis. You may also have associated thromboembolic
disorders or vascular disease. These manifestations may not correlate with the severity
of your IBD. If your impairment does not meet any of the criteria of 105.06, we will
consider the effects of your extraintestinal manifestations in determining whether
you have an impairment(s) that meets or medically equals another listing, and we will
also consider the effects of your extraintestinal manifestations when we determine
whether your impairment(s) functionally equals the listings.
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4. Surgical diversion of the intestinal tract, including ileostomy and colostomy,
does not very seriously interfere with age-appropriate functioning if you are able
to maintain adequate nutrition and function of the stoma. However, if you are not
able to maintain adequate nutrition, we will evaluate your impairment under 105.08.
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F.
How do we evaluate short bowel syndrome (SBS)?
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1. Short bowel syndrome (105.07) is a disorder that occurs when congenital intestinal abnormalities, ischemic
vascular insults (for example, necrotizing enterocolitis, volvulus), trauma, or IBD
complications require surgical resection of more than one-half of the small intestine,
resulting in the loss of intestinal absorptive surface and a state of chronic malnutrition.
The management of SBS requires long-term parenteral nutrition via an indwelling central
venous catheter (central line); the process is often referred to as hyperalimentation or total parenteral nutrition (TPN). Children with SBS can also feed orally, with variable amounts of nutrients
being absorbed through their remaining intestine. Over time, some of these children
can develop additional intestinal absorptive surface, and may ultimately be able to
be weaned off their parenteral nutrition.
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2. Your impairment will continue to meet 105.07 as long as you remain dependent on
daily parenteral nutrition via a central venous catheter for most of your nutritional
requirements. Long-term complications of SBS and parenteral nutrition include abnormal
growth rates, central line infections (with or without septicemia), thrombosis, hepatotoxicity,
gallstones, and loss of venous access sites. Intestinal transplantation is the only
definitive treatment for children with SBS who remain chronically dependent on parenteral
nutrition.
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3. To document SBS, we need a copy of the operative report of intestinal resection,
the summary of the hospitalization(s) including: Details of the surgical findings,
medically appropriate postoperative imaging studies that reflect the amount of your
residual small intestine, or if we cannot get one of these reports, other medical
reports that include details of the surgical findings. We also need medical documentation
that you are dependent on daily parenteral nutrition to provide most of your nutritional
requirements.
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G.
How do we evaluate growth failure due to any digestive disorder?
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1. To evaluate growth failure due to any digestive disorder, we require documentation
of the laboratory findings of chronic nutritional deficiency described in 105.08A
and the growth measurements in 105.08B within the same consecutive 12-month period.
The dates of laboratory findings may be different from the dates of growth measurements.
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2. Under 105.08B, we evaluate a child’s growth failure by using the appropriate table
for age and gender.
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a. For children from birth to attainment of age 2, we use the weight-for-length table
(see Table I or Table II).
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b. For children age 2 to attainment of age 18, we use the body mass index (BMI)-for-age
table (see Table III or Table IV).
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c. BMI is the ratio of a child’s weight to the square of the child’s height. We calculate
BMI using one of the following formulas:
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BMI = [Weight in Pounds / (Height in Inches x Height in Inches)] x 703
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BMI = Weight in Kilograms / (Height in Meters x Height in Meters)
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BMI = [Weight in Kilograms / (Height in Centimeters x Height in Centimeters)] x 10,000
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H.
How do we evaluate the need for supplemental daily enteral feeding via a gastrostomy?
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1. General. Infants and young children may have anatomical, neurological, or developmental disorders
that interfere with their ability to feed by mouth, resulting in inadequate caloric
intake to meet their growth needs. These disorders frequently result in the medical
necessity to supplement caloric intake and to bypass the anatomical feeding route
of mouth-throat- esophagus into the stomach.
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2. Children who have not attained age 3 and who require supplemental daily enteral
nutrition via a feeding gastrostomy meet 105.10 regardless of the medical reason for
the gastrostomy. Thereafter, we evaluate growth impairment under 100.02, malnutrition
under 105.08, or other medical or developmental disorder(s) (including the disorder(s)
that necessitated gastrostomy placement) under the appropriate listing(s).
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I.
How do we evaluate esophageal stricture or stenosis?
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Esophageal stricture or stenosis (narrowing) from congenital atresia (absence or abnormal
closure of a tubular body organ) or destructive esophagitis may result in malnutrition
or the need for gastrostomy placement, which we evaluate under 105.08 or 105.10. Esophageal
stricture or stenosis may also result in complications such as pneumonias due to frequent
aspiration, or difficulty in maintaining nutritional status short of listing-level
severity. While none of these complications may be of such severity that they would
meet the criteria of another listing, the combination of impairments may medically
equal the severity of a listing or functionally equal the listings.
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J.
What do we mean by the phrase ‘‘consider under a disability for 1 year’’?
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We use the phrase “consider under a disability for 1 year” following a specific event
in 105.02, 105.05A, and 105.09 to explain how long your impairment can meet the requirements
of those particular listings. This phrase does not refer to the date on which your
disability began, only to the date on which we must reevaluate whether your impairment
continues to meet a listing or is otherwise disabling. For example, if you have received
a liver transplant, you may have become disabled before the transplant because of
chronic liver disease. Therefore, we do not restrict our determination of the onset
of disability to the date of the specified event. We will establish an onset date
earlier than the date of the specified event if the evidence in your case record supports
such a finding.
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K.
How do we evaluate impairments that do not meet one of the digestive disorder listings?
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1. These listings are only examples of common digestive disorders that we consider
severe enough to result in marked and severe functional limitations. If your impairment(s)
does not meet the criteria of any of these listings, we must also consider whether
you have an impairment(s) that satisfies the criteria of a listing in another body
system. For example:
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a. If you have hepatitis B or C and you are depressed, we will evaluate your impairment
under 112.04.
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b. If you have multiple congenital abnormalities, we will evaluate your impairment(s)
under the criteria in the listings for impairments that affect multiple body systems
(110.00) or the criteria of listings in other affected body systems.
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c. If you have digestive disorders that interfere with intake, digestion, or absorption
of nutrition, and result in a reduction in your rate of growth, and your impairment
does not satisfy the criteria in the malnutrition listing (105.08), we will evaluate
your impairment under the growth impairment listings (100.00).
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2. If you have a severe medically determinable impairment(s) that does not meet a
listing, we will determine whether your impairment(s) medically equals a listing.
(See §416.926.) If your impairment(s) does not meet or medically equal a listing,
you may or may not have an impairment(s) that functionally equals the listings. (See
§416.926a.) When we decide whether you continue to be disabled, we use the rules in
§416.994a.
-
-
105.01 Category of Impairments, Digestive System
-
-
105.02 Gastrointestinal hemorrhaging from any cause, requiring blood transfusion (with or without hospitalization) of at least 10 cc of blood/kg of body weight, and
occurring at least three times during a consecutive 6-month period. The transfusions
must be at least 30 days apart within the 6-month period. Consider under a disability
for 1 year following the last documented transfusion; thereafter, evaluate the residual
impairment(s).
-
-
-
-
-
-
105.05 Chronic liver disease, with:
-
A. Hemorrhaging from esophageal, gastric, or ectopic varices or from portal hypertensive
gastropathy, demonstrated by endoscopy, x-ray, or other appropriate medically acceptable
imaging, resulting in hemodynamic instability as defined in 105.00D5, and requiring
hospitalization for transfusion of at least 10 cc of blood/kg of body weight. Consider
under a disability for 1 year following the last documented transfusion; thereafter,
evaluate the residual impairment(s).
-
-
-
-
B. Ascites or hydrothorax not attributable to other causes, despite continuing treatment
as prescribed, present on at least two evaluations at least 60 days apart within a
consecutive 6-month period. Each evaluation must be documented by:
-
1. Paracentesis or thoracentesis; or
-
2. Appropriate medically acceptable imaging or physical examination and one of the
following:
-
a. Serum albumin of 3.0 g/dL or less; or
-
b. International Normalized Ratio (INR) of at least 1.5.
-
-
-
-
C. Spontaneous bacterial peritonitis with peritoneal fluid containing an absolute neutrophil
count of at least 250 cells/mm3.
-
-
-
-
D. Hepatorenal syndrome as described in 105.00D8, with one of the following:
-
1. Serum creatinine elevation of at least 2 mg/dL; or
-
2. Oliguria with 24-hour urine output less than 1 mL/kg/hr; or
-
3. Sodium retention with urine sodium less than 10 mEq per liter.
-
-
-
-
E. Hepatopulmonary syndrome as described in 105.00D9, with:
-
1. Arterial oxygenation (PaO2,) on room air of:
-
a. 60 mm Hg or less, at test sites less than 3000 feet above sea level, or
-
b. 55 mm Hg or less, at test sites from 3000 to 6000 feet, or
-
c. 50 mm Hg or less, at test sites above 6000 feet; or
-
2. Documentation of intrapulmonary arteriovenous shunting by contrast-enhanced echocardiography
or macroaggregated albumin lung perfusion scan.
-
-
-
-
F. Hepatic encephalopathy as described in 105.00D10, with 1 and either 2 or 3:
-
1. Documentation of abnormal behavior, cognitive dysfunction, changes in mental status,
or altered state of consciousness (for example, confusion, delirium, stupor, or coma),
present on at least two evaluations at least 60 days apart within a consecutive 6-month
period; and
-
2. History of transjugular intrahepatic portosystemic shunt (TIPS) or any surgical
portosystemic shunt; or
-
3. One of the following occurring on at least two evaluations at least 60 days apart
within the same consecutive 6-month period as in F1:
-
a. Asterixis or other fluctuating physical neurological abnormalities; or
-
b. Electroencephalogram (EEG) demonstrating triphasic slow wave activity; or
-
c. Serum albumin of 3.0 g/dL or less; or
-
d. International Normalized Ratio (INR) of 1.5 or greater.
-
-
-
-
G. End Stage Liver Disease, with:
-
1. For children 12 years of age or older, SSA CLD scores of 22 or greater calculated
as described in 105.00D11a. Consider under a disability from at least the date of
the first score.
-
2. For children who have not attained age 12, SSA CLD-P scores of 11 or greater calculated
as described in 105.00D11b. Consider under a disability from at least the date of
the first score.
-
-
-
-
H. Extrahepatic biliary atresia as diagnosed on liver biopsy or intraoperative cholangiogram.
Consider under a disability for 1 year following the diagnosis; thereafter, evaluate
the residual liver function.
-
-
105.06 Inflammatory bowel disease (IBD) documented by endoscopy, biopsy, appropriate medically acceptable imaging, or operative
findings with:
-
-
A. Obstruction of stenotic areas (not adhesions) in the small intestine or colon with
proximal dilatation, confirmed by appropriate medically acceptable imaging or in surgery,
requiring hospitalization for intestinal decompression or for surgery, and occurring
on at least two occasions at least 60 days apart within a consecutive 6-month period;
-
-
-
-
B. Two of the following despite continuing treatment as prescribed and occurring within
the same consecutive 6-month period:
-
1. Anemia with hemoglobin less than 10.0 g/dL, present on at least two evaluations
at least 60 days apart; or
-
2. Serum albumin of 3.0 g/dL or less, present on at least two evaluations at least
60 days apart; or
-
3. Clinically documented tender abdominal mass palpable on physical examination with
abdominal pain or cramping that is not completely controlled by prescribed narcotic
medication, present on at least two evaluations at least 60 days apart; or
-
4. Perineal disease with a draining abscess or fistula, with pain that is not completely
controlled by prescribed narcotic medication, present on at least two evaluations
at least 60 days apart; or
-
5. Need for supplemental daily enteral nutrition via a gastrostomy or daily parenteral
nutrition via a central venous catheter. (See 105.10 for children who have not attained
age 3.)
-
-
105.07 Short bowel syndrome (SBS), due to surgical resection of more than one-half of the small intestine, with dependence
on daily parenteral nutrition via a central venous catheter (see 105.00F).
-
-
105.08 Growth Failure due to any digestive disorder (see 105.00G), documented by A and B:
-
-
A. Chronic nutritional deficiency present on at least two evaluations at least 60 days
apart within a consecutive 12-month period documented by one of the following:
-
1. Anemia with hemoglobin less than 10.0 g/dL; or
-
2. Serum albumin of 3.0 g/dL or less
-
-
-
-
B. Growth failure as required in 1 or 2:
-
1. For children from birth to attainment of age 2, three weight-for-length measurements that are:
-
a. Within a 12-month period; and
-
b. At least 60 days apart; and
-
c. Less than the third percentile on Table I or Table II; or
-
Table I – Males Birth to Attainment of Age 2
-
Third Percentile Values for Weight-for Length
-
Length
(Centimeters)
|
Weight
(kilograms)
|
|
45.0
|
1.597
|
|
45.5
|
1.703
|
|
46.5
|
1.919
|
|
47.5
|
2.139
|
|
48.5
|
2.364
|
|
49.5
|
2.592
|
|
50.5
|
2.824
|
|
51.5
|
3.058
|
|
52.5
|
3.294
|
|
53.5
|
3.532
|
|
54.5
|
3.771
|
|
55.5
|
4.010
|
|
56.5
|
4.250
|
|
57.5
|
4.489
|
|
58.5
|
4.728
|
|
59.5
|
4.966
|
|
60.5
|
5.203
|
|
61.5
|
5.438
|
|
62.5
|
5.671
|
|
63.5
|
5.903
|
|
64.5
|
6.132
|
|
65.5
|
6.359
|
|
66.5
|
6.584
|
|
67.5
|
6.807
|
|
68.5
|
7.027
|
|
69.5
|
7.245
|
|
70.5
|
7.461
|
|
71.5
|
7.674
|
|
72.5
|
7.885
|
|
73.5
|
8.094
|
|
74.5
|
8.301
|
|
75.5
|
8.507
|
|
76.5
|
8.710
|
|
77.5
|
8.913
|
|
78.5
|
9.113
|
|
79.5
|
9.313
|
|
80.5
|
9.512
|
|
81.5
|
9.710
|
|
82.5
|
9.907
|
|
83.5
|
10.104
|
|
84.5
|
10.301
|
|
85.5
|
10.499
|
|
86.5
|
10.696
|
|
87.5
|
10.895
|
|
88.5
|
11.095
|
|
89.5
|
11.296
|
|
90.5
|
11.498
|
|
91.5
|
11.703
|
|
92.5
|
11.910
|
|
93.5
|
12.119
|
|
94.5
|
12.331
|
|
95.5
|
12.546
|
|
96.5
|
12.764
|
|
97.5
|
12.987
|
|
98.5
|
13.213
|
|
99.5
|
13.443
|
|
100.5
|
13.678
|
|
101.5
|
13.918
|
|
102.5
|
14.163
|
|
103.5
|
14.413
|
|
-
-
Table II – Females Birth to Attainment of Age 2
-
Third Percentile Values for Weight-for-Length
-
Length (centimeters)
|
Weight (kilograms)
|
|
45.0
|
1.613
|
|
45.5
|
1.724
|
|
46.5
|
1.946
|
|
47.5
|
2.171
|
|
48.5
|
2.397
|
|
49.5
|
2.624
|
|
50.5
|
2.852
|
|
51.5
|
3.081
|
|
52.5
|
3.310
|
|
53.5
|
3.538
|
|
54.5
|
3.767
|
|
55.5
|
3.994
|
|
56.5
|
4.220
|
|
57.5
|
4.445
|
|
58.5
|
4.669
|
|
59.5
|
4.892
|
|
60.5
|
5.113
|
|
61.5
|
5.333
|
|
62.5
|
5.552
|
|
63.5
|
5.769
|
|
64.5
|
5.985
|
|
65.5
|
6.200
|
|
66.5
|
6.413
|
|
67.5
|
6.625
|
|
68.5
|
6.836
|
|
69.5
|
7.046
|
|
70.5
|
7.254
|
|
71.5
|
7.461
|
|
72.5
|
7.667
|
|
73.5
|
7.871
|
|
74.5
|
8.075
|
|
75.5
|
8.277
|
|
76.5
|
8.479
|
|
77.5
|
8.679
|
|
78.5
|
8.879
|
|
79.5
|
9.078
|
|
80.5
|
9.277
|
|
81.5
|
9.476
|
|
82.5
|
9.674
|
|
83.5
|
9.872
|
|
84.5
|
10.071
|
|
85.5
|
10.270
|
|
86.5
|
10.469
|
|
87.5
|
10.670
|
|
88.5
|
10.871
|
|
89.5
|
11.074
|
|
90.5
|
11.278
|
|
91.5
|
11.484
|
|
92.5
|
11.691
|
|
93.5
|
11.901
|
|
94.5
|
12.112
|
|
95.5
|
12.326
|
|
96.5
|
12.541
|
|
97.5
|
12.760
|
|
98.5
|
12.981
|
|
99.5
|
13.205
|
|
100.5
|
13.431
|
|
101.5
|
13.661
|
|
102.5
|
13.895
|
|
103.5
|
14.132
|
|
-
-
2. For children age 2 to attainment of age 18, three (BMI)-for-age measurements that are:
-
a.
Within a consecutive 12-month period; and
-
b.
At least 60 days apart; and
-
c.
Less than the third percentile on Table III or Table IV
Table III – Males Age 2 to Attainment of Age 18
-
Third Percentile Values for BMI-for-Age
Age (yrs. and mos.)
|
BMI
|
|
2.0 to 2.1
|
14.5
|
|
2.2 to 2.4
|
14.4
|
|
2.5 to 2.7
|
14.3
|
|
2.8 to 2.11
|
14.2
|
|
3.0 to 3.2
|
14.1
|
|
3.3 to 3.6
|
14.0
|
|
3.7 to 3.11
|
13.9
|
|
4.0 to 4.5
|
13.8
|
|
4.6 to 5.0
|
13.7
|
|
5.1 to 6.0
|
13.6
|
|
6.1 to 7.6
|
13.5
|
|
7.7 to 8.6
|
13.6
|
|
8.7 to 9.1
|
13.7
|
|
9.2 to 9.6
|
13.8
|
|
9.7 to 9.11
|
13.9
|
|
10.0 to 10.3
|
14.0
|
|
10.4 to 10.7
|
14.1
|
|
10.8 to 10.10
|
14.2
|
|
10.11 to 11.2
|
14.3
|
|
11.3 to 11.5
|
14.4
|
|
11.6 to 11.8
|
14.5
|
|
11.9 to 11.11
|
14.6
|
|
12.0 to 12.1
|
14.7
|
|
12.2 to 12.4
|
14.8
|
|
12.5 to 12.7
|
14.9
|
|
12.8 to 12.9
|
15.0
|
|
12.10 to 13.0
|
15.1
|
|
13.1 to 13.2
|
15.2
|
|
13.3 to 13.4
|
15.3
|
|
13.5 to 13.7
|
15.4
|
|
13.8 to 13.9
|
15.5
|
|
13.10 to 13.11
|
15.6
|
|
14.0 to 14.1
|
15.7
|
|
14.2 to 14.4
|
15.8
|
|
14.5 to 14.6
|
15.9
|
|
14.7 to 14.8
|
16.0
|
|
14.9 to 14.10
|
16.1
|
|
14.11 to 15.0
|
16.2
|
|
15.1 to 15.3
|
16.3
|
|
15.4 to 15.5
|
16.4
|
|
15.6 to 15.7
|
16.5
|
|
15.8 to 15.9
|
16.6
|
|
15.10 to 15.11
|
16.7
|
|
16.0 to 16.1
|
16.8
|
|
16.2 to 16.3
|
16.9
|
|
16.4 to 16.5
|
17.0
|
|
16.6 to 16.8
|
17.1
|
|
16.9 to 16.10
|
17.2
|
|
16.11 to 17.0
|
17.3
|
|
17.1 to 17.2
|
17.4
|
|
17.3 to 17.5
|
17.5
|
|
17.6 to 17.7
|
17.6
|
|
17.8 to 17.9
|
17.7
|
|
17.10 to 17.11
|
17.8
|
|
-
Table IV – Females Age 2 to Attainment of Age 18
-
Third Percentile Values for BMI-for-Age
Age
(yrs. and mos.)
|
BMI
|
|
2.0 to 2.2
|
14.1
|
|
2.3 to 2.6
|
14.0
|
|
2.7 to 2.10
|
13.9
|
|
2.11 to 3.2
|
13.8
|
|
3.3 to 3.6
|
13.7
|
|
3.7 to 3.11
|
13.6
|
|
4.0 to 4.4
|
13.5
|
|
4.5 to 4.11
|
13.4
|
|
5.0 to 5.9
|
13.3
|
|
5.10 to 7.6
|
13.2
|
|
7.7 to 8.4
|
13.3
|
|
805 to 8.10
|
13.4
|
|
8.11 to 9.3
|
13.5
|
|
9.4 to 9.8
|
13.6
|
|
9.9 to 10.0
|
13.7
|
|
10.1 to 10.4
|
13.8
|
|
10.5 to 10.7
|
13.9
|
|
10.8 to 10.10
|
14.0
|
|
10.11 to 11.2
|
14.1
|
|
11.3 to 11.5
|
14.2
|
|
11.6 to 11.7
|
14.3
|
|
11.8 to 11.10
|
14.4
|
|
11.11 to 12.1
|
14.5
|
|
12.2 to 12.4
|
14.6
|
|
12.5 to 12.6
|
14.7
|
|
12.7 to 12.9
|
14.8
|
|
12.10 to 12.11
|
14.9
|
|
13.0 to 13.2
|
15.0
|
|
13.3 to 13.4
|
15.1
|
|
13.5 to 13.7
|
15.2
|
|
13.8 to 13.9
|
15.3
|
|
13.10 to 14.0
|
15.4
|
|
14.1 to 14.2
|
15.5
|
|
14.3 to 14.5
|
15.6
|
|
14.6 to 14.7
|
15.7
|
|
14.8 to 14.9
|
15.8
|
|
14.10 to 15.0
|
15.9
|
|
15.1 to 15.2
|
16.0
|
|
15.3 to 15.5
|
16.1
|
|
15.6 to 15.7
|
16.2
|
|
15.8 to 15.10
|
16.3
|
|
15.11 to 16.0
|
16.4
|
|
16.1 to 16.3
|
16.5
|
|
16.4 to 16.6
|
16.6
|
|
16.7 to 16.9
|
16.7
|
|
16.10 to 17.0
|
16.8
|
|
17.1 to 17.3
|
16.9
|
|
17.4 to 17.7
|
17.0
|
|
17.8 to 17.11
|
17.1
|
|
-
105.09 Liver transplantation. Consider under a disability for 1 year following the date of transplantation; thereafter,
evaluate the residual impairment(s) (see 105.00D13 and 105.00J).
-
105.10 Need for supplemental daily enteral feeding via a gastrostomy due to any cause, for children who have not attained age 3; thereafter, evaluate
the residual impairment(s) (see 105.00H).
-