Hepatic Inborn Errors Of Metabolism

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Hepatic Inborn Errors Of Metabolism

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Title: Hepatic Inborn Errors Of Metabolism

1
Hepatic Inborn Errors Of Metabolism

Dr.Mona El Raziky
M.D. Pediatric Hepatology
Nasser Institute For Research Treatment

2
When To Suspect Metabolic Liver Disease?

jaundice,
hepatomegaly,
splenomegaly,
hepatic failure,
hypoglycemia,
organic acidemia,
hyperammonemia,
hypoprothrombinemia,
recurrent vomiting,

failure to thrive or short stature,
dysmorphic features,
developmental delay hypotonia,
neuromuscular deterioration,
seizures,
unusual odors,
rickets,
or cataracts.

3
When To Suspect Metabolic Liver Disease?

Clinical and laboratory examination can be
complemented by analysis of tissue obtained by
liver biopsy.
This analysis may confirm the suspicion or alert
the clinician to new possibilities and allow
enzyme assay and qualitative and quantitative
assay of stored material. This information will
have important genetic implications.

4
Differential Diagnosis of Neonatal Cholestasis

Metabolic
Disorders of amino acid metabolism
Tyrosinemia
Disorders of lipid metabolism
Wolman's disease
Nicmann-Pick disease (type C)
Gaucher's disease
Disorders of carbohydrate metabolism
Galactosemia
Fructosemia
Glycogenosis IV
Disorders of bile acid biosynthesis (reductase,
isomerase)

5
Differential Diagnosis of Neonatal Cholestasis

Other metabolic defects
Alpha1 -antitrypsin deficiency
Cystic fibrosis
Idiopathic hypopituitarism
Hypothyroidism
Zellweger (cerebrohepatorenal) syndrome
Neonatal iron storage disease
Indian childhood cirrhoris
infantile copper overload
Familial erythrophagocytic
Lymphohistiocytosis
Arginase deficiency
Mitochrondrial DNA depletion

6
Metabolic Liver Disease

Most patients with metabolic liver disease
present in infancy with either
Cholestasis (alpha1 -antitrypsin deficiency,
Niemann-Pick disease, cystic fibrosis),
Acute liver failure (mitochondrial
disorders,neonatal hemochromatosis,
galactosemia),
Multisystem disease (glycogen storage disease).

7
Causes of Conjugated Hyperbilirubinemia in Older
Children

Viral Infections
Hepatitis viruses A, B, C, D, E
Epstein-Barr virus
Cytomegalovirus
Herpes simplex
Metabolic Liver Disease
Wilson disease
Alpha-1-antitrypsin deficiency
Cystic fibrosis
Biliary Tract Disorders
Cholelithiasis
Cholecystitis
Choledochal cyst
Sclerosing cholangitis

Autoimmune Liver Disease
Type 1 (anti-smoooth muscle antibody)
Type 2 (anti-liver-kidney-microsomal antibody)
Hepatotoxins
Drugs Acetaminophen
Anticonvulsants
Anesthetics
Antituberculous agents
Chemotherapeutic agents
Antibiotics
Oral contraceptives
Other Alcohol, insecticides, organophosphates
Vascular Causes
Budd-Chiari syndrome
Veno-occlusive disease

8
Tyrosinemia

Recessive inherited metabolic liver and kidney
disease
Deficiency of fumarylacetoacetate hydrolase (FAH)
.
Accumulation of the reactive metabolites
fumarylacetoacetate and maleylacetoacetate and
their reduced derivatives succinylacetoacetate
and succinylacetone
Succinylacetone is a potent inhibitor of
porphobilinogen synthase.

9
Tyrosine degradation pathway indicating the
level of metabolic block in tyrosinemia type I by
loss of fumarylacetoacetate hydrolase (FAH) and
the site of inhibition induced by
2-(2-nitro-4-trifluoromethylbenzoyl)-1,3-cycloheax
anedione (NTBC)
10
Tyrosinemia

The clinical spectrum of the disorder
Acute liver failure in infancy.
Slowly progressive liver cirrhosis complicated by
a high incidence of childhood hepatocellular
carcinoma (HCC),
hypophosphatemic rickets caused by kidney tubular
dysfunction,
porphyrialike neurologic crisis.

11
Tyrosinemia (Diagnosis)

neonatal liver disease
coagulopathy
severe metabolic disturbances
Serum amino acid patterns may exhibit high levels
of tyrosine, phenylalanine, proline, and
methionine. High levels of alpha-fetoprotein are
characteristic of tyrosinemia.
In the untreated patient, urinary succinylacetone
excretion, the pathognomonic sign of tyrosinemia
type I, is highly variable ranging from barely
detectable (i.e., lt 1 mmol/mol creatinine) to
more than 1000 mmol/mol creatinine.

12
Tyrosinemia (Treatment )

Was confined to treatment with a
diet restricted in tyrosine and phenylalanine.
Although dietary treatment may relieve acute
symptoms and resolve the kidney disease, the
prognosis remained poor.
Liver transplantation became widely accepted as
the only successful treatment
At this time, a new principle for treatment of
tyrosinemia type I based on inhibition of
tyrosine degradation at the level of
4-hydroxyphenylpyruvate dioxygenase was reported.

13
Tyrosinemia (Treatment )

Since then, the number of patients treated by the
inhibitor 2-(2-nitro-4-trifluoromethylbenzoyl)-1,3
-cyclohexanedione (NTBC) has steadily increased,
and NTBC treatment has become a first-line
treatment of tyrosinemia type I.
The urinary succinylacetone level is a very
sensitive marker for the efficiency of NTBC
treatment normalization of plasma level takes 2
to 3 months after the start of treatment.
NTBC treatment has greatly improved the survival
of patients with acute tyrosinemia and has
reduced the need for liver transplantation during
early childhood.

14
Urea Cycle Disorders

Deficiency of any of the five enzymes in the urea
cycle results in the accumulation of ammonia and
leads to encephalopathy.
Episodes of encephalopathy and associated
systems are unpredictable and, if untreated, are
lethal or produce devastating neurologic sequelae
in long-term survivors.
Although these disorders do not produce liver
disease, the consequences of hyperammonemia
resemble those seen in patients with hepatic
failure or in a transient interference with the
urea cycle, as seen in some forms of organic
acidemias.
Investigate for hyperammonemia in any infant or
child with altered mental status

15
The urea cycle Asterisk N-acetyl glutamate
synthetase 1 carbamyl phosphate synthetase 2
ornithine transcarbamylase 3
argininosuccinate synthetase 4
argininosuccinate lyase 5 arginase
16

17
Urea Cycle Disorders (Diagnosis)

Cultured skin fibroblasts may be desirable if
prenatal diagnosis is considered in future
pregnancies.
Carbamyl phosphate synthetase I and ornithine
transcarbamylase (OTC) are not expressed in
cultured fibroblasts.
The enzymatic diagnosis of CPSD and OTCD requires
liver biopsy.
Biopsy should be done when establishing the
diagnosis of the first case in a family.

18
Evaluation of hyperammonemia in the neonate
THANtransient hyperammonemia of the newborn PC
pyruvate carboxylase PDH pyruvate
dehydrogenase FAO fatty acid oxidation CPSD
carbamyl phosphate synthetase deficiency OTCD
ornithine transcarbamylase deficiency ASA
argininosuccinic acid.
19
Urea Cycle Disorders(Treatment)

Once hyperammonemia is demonstrated in an infant,
protein-containing feedings should be
discontinued immediately,
appropriate supportive care, (mechanical
ventilation)
Maximal calories should be provided in the form
of intravenous glucose and lipids in an effort to
reduce catabolism.
Plans should be immediately made to initiate
hemodialysis in infants who are encephalopathic
and have plasma ammonia levels over 10 times the
upper limit of normal.

20
Urea Cycle Disorders(Treatment)

Maintenance therapy
dietary protein restrictionsupplementation with
citrulline or arginine the use of drugs
The primary drug now used( provides an alternate
pathway for waste nitrogen excretion) for
maintenance therapy in patients with urea cycle
disorders is sodium phenylbutyrate (Buphenyl).
The drug is typically administered four times a
day in a dose of 0.4 to 0.6 g/kg/day. It is
supplied as a powder, which can be mixed with
food or formula, or as a tablet.

21
Urea Cycle Disorders(Treatment)

Liver transplantation for
Severe neonatal OTC and CPS deficiency.
Liver failure and cirrhosis in ASL deficiency.
Failed medical-pharmacologic treatment.
Pretransplant care by
aggressively managing intercurrent
hyperammonemia,
vaccinations and prophylaxis are given against
infectious
appropriate caloric intake
Gene replacement

22
Niemann-Pick Disease Type C

Caused by decreased sphingomyelinase, resulting
in accumulation of sphingomyelin and cholesterol
in the reticuloendothelial system of many organs,
including the liver.
Sixty-five percent of these children will present
with prolonged cholestasis and hepatosplenomegaly
in infancy.
All of these children will develop neurologic
complications, with a mean age of onset at 5
years.
Most children die in early adolescence from
respiratory rather than hepatic complications.
Characterized histologically by lipid-laden foam
cells and stored sphingomyelin in macrophages.

23
Gaucher's Disease

Autosomal recessive disorder,
Deficiency of glucosyl-ceramide beta-glucosidase
is present throughout the phagocyte-mononuclear
system.
Hepatosplenomegaly and respiratory, neurologic,
and bone disease complicate the clinical course.
Therapy includes enzyme replacement and bone
marrow or liver transplantation

24
Glycogen Storage Disease

Hepatomegaly growth failure hypoglycemia,
the typical presenting signs (type 1 is the
most prevalent type)
Type 4 (brancher enzyme deficiency), a rare
disorder, presents with signs of hepatocellular
dysfunction and liver failure during the first 2
years of life.
The diagnosis of glycogen storage disease is
based on demonstrating the respective enzyme
deficiency
All deficiencies are inherited in an autosomal
recessive pattern except for phosphorylase kinase
deficiency (type 9), which follows an X-linked
pattern.

25
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26
Glycogen Storage Disease

Type 1
Is the most common.
Deficiency of hepatic glucose 6-phosphatase
impairs both conversion of glycogen to glucose
and the formation of glucose from lactate and
amino acids (gluconeogenesis).
Affected persons develop profound hypoglycemia
after short fasting periods, with associated
lactic acidemia, hyperuricemia, hypophosphatemia,
and hyperlipidemia.
Treatment, aimed at preventing fasting
hypoglycemia, includes a high-starch diet, often
with nocturnal cornstarch infusions, and
continuous nasogastric feedings

27
Hereditary Fructose Intolerance

An autosomal recessive disorder.
The disorder results from absence or reduction
of fructose-1-phosphate aldolase beta in liver,
kidneys, and small intestine.
Clinical presentation varies from
severe vomiting, failure to thrive,
hepatomegaly, and coagulopathy to acute liver
failure with jaundice, encephalopathy, and renal
failure
Treatment is dietary elimination of fructose.

28
Galactosemia

Deficiency of the intracellular enzyme galactose
1-phosphate uridyltransferase usually presents
within the first few days of life,
with protracted vomiting shortly after the onset
of lactose feeding.
If untreated, accumulation of galactose
1-phosphate and galactitol occurs in several
organ systems, and infants will succumb to
hepatic failure.
Early treatment consists of removing all sources
of lactose from the diet and will prevent
complications.

29
Neonatal Hemochromatosis

Acute liver failure is uncommon in the newborn
period neonatal hemochromatosis is the most
common cause.
Iron accumulation commences in utero, either as a
consequence of a primary disorder of
fetoplacental iron handling or as a secondary
manifestation of fetal liver disease.
The diagnosis is established by MR imaging and by
demonstrating iron accumulation in biopsy tissue
obtained from the minor salivary gland on the
lower lip.

30
Neonatal Hemochromatosis

Medical management initially involves supportive
therapy for acute liver failure.
Treatment with a combination of antioxidants that
combines N-acetylcysteine, vitamin E, selenium,
prostaglandin E1 , and desferrioxamine should be
started as soon as the diagnosis has been
established. Liver transplantation is usually
required, and, if successful, is curative.

31
Disorders of Mitochondrial Energy Metabolism

Primary mitochondrial hepatopathies
Inherited defects in structure or function of the
hepatocellular mitochondria.
Maternally inherited mutations or deletions of
the mitochondrial genome or
Putative nuclear gene mutations encoding
electron transport proteins cause defective
electron transport, oxidative stress, impaired
oxidative phosphorylation, and other metabolic
derangements.

32
Disorders of Mitochondrial Energy Metabolism

Primary mitochondrial hepatopathies
These defects in turn lead to hepatic failure or
chronic dysfunction.
Abnormalities of the electron transport chain
result in cellular ATP deficiency and the
generation of toxic free radicals.
In a patient with liver failure, isolated
deficiencies of the electron-chain enzymes and
mitochondrial DNA depletion syndromes must be
considered

33
Disorders of Mitochondrial Energy Metabolism

Secondary mitochondrial hepatopathies
The mitochondria are major targets during liver
injury caused by
metal overload, drugs, toxins, alcohol,oxidants.
The current treatment of these disorders is
empiric, involving agents that may improve the
oxidation-reduction status of mitochondria,
promote electron flow, or act as mitochondrial
antioxidants.
Liver transplantation can be considered in the
absence of systemic involvement.

34
Inborn Errors of Bile Acid Synthesis

Defects early in the biosynthetic pathway produce
profound neonatal cholestasis
severe liver dysfunction
subacute hepatic failure.
The GGTP values are low
AP and aminotransferase levels are usually
elevated.
Diagnosis is reached by qualitative assessment
of bile acids in serum and urine.
Early diagnosis permits therapy with exogenously
administered bile acids, often with dramatic
results.
Liver transplantation, when required, is
curative.

35
Inborn Errors of Bile Acid Synthesis(Types)

Primary Defects (Enzymopathies)
Defective transformation of steroid nucleus
Delta -3-oxosteroid-5beta reductase deficiency
3 beta-hydroxy Delta -C27 steroid
dehydrogenase/isomerase deficiency
24,25-dihydroxy cholanoic cleavage enzyme
deficiency (25-hydroxylase pathway)
7-dehydrocholesterol 7-reductase deficiency (the
Smith-Lemli-Opitz syndrome)
Deficiency of 7alpha-hydroxylation
2. Defective degradation or transformation of
cholesterol side chain
cerebrotendinous xanthomatosis (cholesterol
27-hydroxylase)
defective amidation?

36
Inborn Errors of Bile Acid Synthesis(Types)

Secondary Defects (caused by organelle damage)
Peroxisomal disorders
Generalized hepatic synthetic dysfunction

37
Inborn Errors of Bile Acid Synthesis

The mechanism of cholestasis is thought to be
either
(1) underproduction of normal trophic or
choleretic primary bile acids that are essential
for the promotion and secretion of bile,
(2) overproduction of potentially hepatotoxic
primitive bile acid metabolites.
Patients affected by these disorders have
previously been considered to have idiopathic
disease (e.g., idiopathic neonatal hepatitis or
intrahepatic cholestasis).

38
Inborn Errors of Bile Acid Synthesis

Diagnosis
Fast atom bombardment-mass spectrometry (FAB-MS)
and gas chromatography-mass spectrometry (GC-MS),
have allowed specific delineation of disorders of
bile acid synthesis and subsegmentation of those
broader categories.
The bile acid profiles of urine, serum, and bile
in these patients are characterized by the
predominance of atypical bile acids retaining the
structure of the steroid nucleus characteristic
of the substrates for the inactive or deficient
enzyme.

39
Inborn Errors of Bile Acid SynthesisZellweger's
Syndrome (cerebrohepatorenal)

Profound psychomotor retardation,
hypotonia, characteristic facies,
cortical cysts of the kidneys,
and intrahepatic cholestasis.
Hepatomegaly with jaundice in the first 2 to 3
weeks of life.
There is absence of hepatic peroxisomes.
Biochemical features reflecting absent
peroxisomal function include excessive urinary
excretion of all precursors of primary bile
acids that have not undergone side-chain
oxidation.
Increased concentrations of C27 bile acid
intermediates are present in serum and bile.
Hepatic histologic features cholestasis, lobular
disarray, and focal liver cell necrosis, often
with paucity of intrahepatic ducts.

40
Inborn Errors of Bile Acid Synthesis(Treatment)

Bile acid therapy
when cholic and chenodeoxycholic acid (100 mg
each per day) were given orally, a significant
improvement in biochemical and histological
aspects occurs.

41
DEFECTIVE BILE ACID TRANSPORT IN INHERITED
CHOLESTATIC DISEASES

Byler's Disease (Progressive Familial
Intrahepatic Cholestasis)
Byler's disease is a relatively discrete form of
PFIC characterized by unrelenting progressive
intrahepatic cholestasis
The clinical findings in PFIC-1--pruritus, fat
malabsorption, and low gamma-GTP The coarsely
granular bile found in canaliculi on transmission
electron microscopy in PFIC-1 is also suggestive
of a defect in bile acid transport at the
canalicular membrane. levels--resemble those seen
in 3beta-HSD deficiency.

42
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43
METABOLIC DISEASE IN OLDER CHILDREN

Hepatomegaly
Glycogen storage disease
Hereditary fructose intolerance
Acute liver failure
Wilson's disease
Alper's disease
Valproate toxicity

Chronic liver disease
(with or without portal hypertension)
Alpha1 -antitrypsin deficiency
Cystic fibrosis
Tyrosinemia type 1
Wilson's disease
Gaucher's disease

44
Wilson's Disease

Autosomal recessive disorder of hepatic copper
metabolism
The Wilson's gene has been located on chromosome
13 and encodes a copper-binding,
membrane-spanning protein with ATPase that
regulates metal transport proteins.
Patients usually present with liver disease
during adolescence however,
clinical onset may be detected as early as 3
years of age.
Features in childhood include hepatic dysfunction
(40), psychiatric symptoms (35), and renal,
hematologic, and endocrinologic symptoms. Chronic
liver inflammation (often confused with
autoimmune, chronic-active hepatitis), cirrhosis,
and fulminant hepatic failure are well-described
complications. The characteristic Kayser-Fleisher
rings (present in all patients with
neuropsychiatric symptoms) are not usually
detected before age 7 years

45
Wilson's Disease (Pathology)

Acute hepatitis submassive or massive necrosis,
chronic active hepatitis, and macronodular
cirrhosis.
Liver cells are ballooned and fatty change is
usual.
In some patients, Mallory's bodies simulating
acute alcoholic hepatitis are observed. The
disease may also resemble histologically chronic
active hepatitis analogous to chronic viral
hepatitis.
Cirrhosis usually takes two or three decades to
occur.
Copper chelation therapy with penicillamine
usually retards or reverses liver disease
progression.

46
Wilson's Disease

Diagnosis
is established by detecting low levels of serum
copper (lt 20 mug/dl) and low serum ceruloplasmin,
an increased level of copper in the urine (gt 100
mug/24 h), and an elevated hepatic copper level
(gt 250 mug of copper/1 g of liver (dry weight).
Treatment
Pharmacologic treatment includes D-penicillamine,
triethylene tetramine dihydrochloride (tientene
generally used in D-penicillamine-intolerant
patients), and oral zinc.
Liver transplantation has been successful in
patients with fulminant hepatitis or advanced
cirrhosis.

47
Alper's Syndrome

Rare disorder that usually presents with sudden
onset of
intractable seizures between the ages of 1 and 3
years.
This hepatic disease presents as jaundice,
hepatomegaly, and coagulopathy, with rapidly
progressive liver failure.
The condition is uniformly fatal, and liver
transplantation is contraindicated because
neurologic deterioration progresses after
transplantation

48
HEREDITARY HEMOCHROMATOSIS (HHC)

A common inherited disorder of iron metabolism .
This disorder described in 1886 as bronze
diabetes is an
autosomal recessive
continuous and inappropriate increase in the
duodenal absorption of ingested iron.
The genetic defect is on chromosome 6 and the HHC
gene has been recently cloned.
The gene defect now can be tested.
In HHC there is evidence in the liver of
increased lipid peroxidation possibly the direct
effect of the oxidizing potential of ferrous iron
generating active oxygen species and free
radicals. The target organs that are damaged in
iron overload, are the liver, heart, pancreas,
and endocrine organs.

49
In the balanced state, 1 to 2 mg of iron enters
and leaves the body each day. Dietary iron is
absorbed by duodenal enterocytes. It circulates
in plasma bound to transferrin. Most of the iron
in the body is incorporated into hemoglobin in
erythroid precursors and mature red cells.
Approximately 10 to 15 percent is present in
muscle fibers (in myoglobin) and other tissues
(in enzymes and cytochromes). Iron is stored in
parenchymal cells of the liver and
reticuloendothelial macrophages. These
macrophages provide most of the usable iron by
degrading hemoglobin in senescent erythrocytes
and reloading ferric iron onto transferrin for
delivery to cells.
50
HEREDITARY HEMOCHROMATOSIS (HHC) Clinical
Manifestations

Variable age of presentation.
Most patients present with liver disease after
the fourth decade of life.
eight to one male to female ratio explainable
because of iron loss in females from menstruation
and childbearing.
In later years, the heart muscle may be affected
resulting in cardiomyopathy.
Other non-hepatic organs affected are the joints
with chondrocalcinosis typically in the
interphalangeal joints and metacarpophalangeal
joints as well as the knees to the back of the
neck.
The common endocrine organs which exhibit
dysfunction are the pituitary gland, and the
pancreas resulting into testicular atrophy,
infertility, and diabetes mellitus.
Most patients show increase pigment in the skin
mainly due to melanin although in 50 of patients
increases in iron deposits in the basal cells of
the epidermis and sweat glands are noted

51
HEREDITARY HEMOCHROMATOSIS (HHC) Clinical
Manifestations

LIVER
This is organ that is most effected. The liver
damage as evidenced by cell necrosis and
increased amino transferase enzymes is not usual.
Rather, the liver has increased hepatocyte and
later biliary epithelial and Kupffer cell iron
which after three or four decades is associated
with fibrosis and later cirrhosis. The risk of
primary liver cancer increases at this point.
Thus an early diagnosis of this condition which
is treatable is mandatory.
When patients are frankly cirrhotic, many show
also evidence of diabetes and increased
pigmentation hence the term, bronze diabetes.

52
HEREDITARY HEMOCHROMATOSIS (HHC) Clinical
Manifestations

LIVER
Classically, when no other causes of liver injury
co-exists such as alcohol or hepatitis, when
liver stores of iron exceed 20 g, cirrhosis may
ensue.
Normal hepatic iron concentration is usually less
than 1000 micrograms per gram/dry weight which
relates to about 2 g of iron stores.
Patients with cirrhosis have an excess of 22,000
micrograms/dry weight equivalent to 20 g of
liver iron stores.

53
HEREDITARY HEMOCHROMATOSIS (HHC)

Diagnosis
to measure serum iron, iron binding capacity in
the ferritin in the blood.
If these are at the high level of normal,
patients should be followed up.
If there is an annual increase of serum
ferritin approximating 50 micrograms per liter
per year, the patient should have a liver biopsy.
Liver biopsy yields important information.
Prussian blue staining of liver hemosiderin
correlates with iron stores.
In the absence of infection or acute disease, if
the serum iron is less than 60 saturated,
cirrhosis is very unlikely.
When hemochromatosis is anticipated, the liver
should be biopsied and a portion should be sent
in a metal-free container for an absolute iron
measurement.

54
HEREDITARY HEMOCHROMATOSIS (HHC)

Management
Iron should be removed by phlebotomy.
One unit of blood (500ml) removes to about 250 mg
of iron.
In contrast, chelation therapy with deferoxamine
which is expensive and inconvenient is capable of
removing 60 mg iron a day.
Because this is a autosomal recessive disease,
family screening is recommended. All siblings,
parents, and children over the age of ten should
be screened with the serum iron, TIBC and
ferritin.
Saturation greater than 50 with an increasing
serum ferritin is an indication for liver biopsy.

55
ALPHA-ONE ANTITRYPSIN (AAT) DEFICIENCY

Is a relatively common autosomal recessive
disorder,
It is the most common genetic cause of liver
disease in children
The most frequent genetic diagnosis for which
children undergo liver transplantation.
AAT synthesized in the endoplasmic reticulum of
the liver and comprises 80 - 90 of the serum
alpha-one globulin.
It is an inhibitor of trypsin and other
protease.
Deficiency results in unopposed action of these
enzymes.
The lungs are the main target with damage to the
alveoli resulting in emphysema. The liver
pathology ranges from acute liver damage, chronic
active hepatitis, or cirrhosis.

56
ALPHA-ONE ANTITRYPSIN (AAT) DEFICIENCY

The gene for AAT is on chromosome 14 and there
are about 75 different alleles at this locus.
M is the most common normal allele,
Z and S are the most frequent abnormal alleles.
Pi (protease inhibitor) MM is the normal state
with normal serum AAT levels.
Pi ZZ results in a low concentration of serum
AAT. Pi Null-Null (NN) gives zero levels. Both
predispose to emphysema. Pi SS and Pi MZ give
levels about half normal with no lung disease.
Liver disease tends to occur with mutations where
AAT accumulates in the hepatocytes, detectable as
PAS positive granules on special staining of
liver biopsy tissue.

57
ALPHA-ONE ANTITRYPSIN (AAT) DEFICIENCY

The disease in the liver can present as neonatal
cholestasis, acute hepatitis, fulminant hepatic
failure, or chronic active hepatitis and
cirrhosis.
The classic subtype for this is Pi ZZ and
therefore, liver disease is commonly associated
with lung disease.
Liver injury is caused by the toxic effect of the
mutant molecule alpha1 ATZ retained within the
endoplasmic reticulum (ER) rather than secreted
into the blood and body fluids.
Recent basic cell biologic studies have shown
that the ER quality control system is extremely
sophisticated It is not surprising, then, that
there are several different genetic and
biochemical mechanisms by which the quality
control system can be altered and an alpha1
AT-deficient host be rendered susceptible to
liver injury.

58
ALPHA-ONE ANTITRYPSIN (AAT) DEFICIENCY

Diagnosis
The diagnosis is suspected by reduced AAT levels
in the plasma and confirmed as liver biopsy.
Treatment
There is no specific treatment for the liver
lesion
Hepatic transplantation is required at the end
stage of liver disease.

59
CYSTIC FIBROSIS

An autosomal recessive pattern of inheritance
with a prevalence of one in 2,000 and a carrier
rate of 5.
Is the most common heritable disorder among white
populations,
Is the most common disorder in which the primary
defect affects cholangiocyte transport systems.
Is the cause of prolonged cholestasis in
approximately 1 of newborns with obstructive
jaundice.
The gene responsible is on chromosome 7 and has
been cloned.
The product is a transmembrane protein regulating
ion conductance.

60
CYSTIC FIBROSIS

prolonged cholestasis respiratory disease
or meconium ileus
Approximately 20 of patients develop liver
disease including fatty change, focal biliary
fibrosis, multi-lobular biliary cirrhosis due to
viscous bile resulting in extrahepatic portal
obstruction and secondary biliary cirrhosis.
The main target organ of this disorder is of the
pancreas where pancreatic insufficiency and
malabsorption, dominate clinically.
Viscous secretions in the lungs also can
predispose to chronic lung disease with
bronchiectasis.

61
CYSTIC FIBROSIS

Diagnosis
When CF is suspected, a sweat chloride
measurement greater than 50 mmol/L is diagnostic
and accurate after 4 weeks of age.
In younger infants, genetic analysis may be
useful.
The most common mutation occurs at position F508
on chromosome 7. Absence of this abnormality does
not rule out CF, however, because several other
genetic mutations have been identified.

62
CYSTIC FIBROSIS

Treatment
CF-associated cholestasis has evolved
significantly with the wide availability of UDCA.
Improvement in both the clinical and biochemical
markers of cholestatic disease has been
demonstrated following UDCA treatment.
The long-term response to oral bile acid therapy
remains to be elucidated, however.
Liver transplantation may be required.
If any of the recipient bile duct is left
behind, liver disease may reoccur.

63
HEPATIC PORPHYRIAS

Heme is a ubiquitous pigment and in tissues it is
responsible for oxygen transport and metabolism.
The human porphyrias are a group of disorders
that reflect bone marrow or hepatic expression of
the inherited/acquired disorders of heme
biosynthesis.
Heme is made from simple precursors, glycine and
succinic acid, and following seven enzymatic
steps, protoporphyrin is formed, into which
enzymatic insertion of iron by ferrochelatase
results in the biosynthesis of heme

64
Biosynthesis Of Heme
65
HEPATIC PORPHYRIAS

There are seven porphyrias, each reflecting a
defect of enzymatic step in heme biosynthesis.
The classification of human porphyrias reflects
the organ of porphyrin overproduction .
Although uncommon, human porphyria is important
not only because photocutaneous manifestations
can be debilitating and disfiguring, but also
because individuals with mostly inherited hepatic
porphyrias, are prone to potentially lethal acute
attacks associated with progressive
polyneuropathy, acute abdomen, severe psychiatric
disturbance, and coma.

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HEPATIC PORPHYRIAS

Clinical Manifestations
If the metabolic lesion is distal to the
porphobilinogen (PBG) deaminase step,
photosensitizing porphyrins may accumulate in the
plasma and skin resulting
Photocutaneous lesions in sun exposed areas, i.e.
the face, the neck, and the extremities -
particularly the hands (in PCT, HCP, and VP).
In hepatic porphyrias, other than porphyria
cutanea tarda (PCT) ingestion of a
porphyrinogenic drug may result in an acute
attack in which abdominal pain, polyneuropathy,
or neurologic disturbances may dominate.
Bone marrow porphyria may result in
photomutilation

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Clinical Manifestations of Human Porphyrias
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Algorithm of therapeutic approach to an acute
porphyric attack
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Classification of Diseases for which OLT Has Been
Performed in Infants and Children

Obstructive biliary tract disease
Biliary atresia ( 50 of all transplant
candidates)
Sclerosing cholangitis
Metabolic disease ( 20 of all candidates)
alpha1 -Antitrypsin deficiency
Tyrosinemia
Glycogen storage diseases (GSD) type IV (and,
rarely, types I, III)
Wilson's disease
Neonatal iron storage disease
Miscellaneous (urea cycle defects)
Intrahepatic cholestasis ( 5 of all candidates)
Familial intrahepatic cholestasis (Byler's
disease)
Syndromic bile duct paucity (Alagille syndrome)
Nonsyndromic bile duct paucity
Idiopathic neonatal hepatitis

Acute and chronic hepatitis
Fulminant hepatic failure ( 10 of all
candidates)
Acute viral hepatitis (non-alphabet)
Toxin or drug induced
Chronic hepatitis/cirrhosis ( 5 of all
candidates)
Postviral
Autoimmune
Idiopathic
Tumors ( 1 of all candidates)
Hepatoblastoma
Hepatocellular carcinoma
Sarcoma
Hemangioendothelioma
Miscellaneous (1-2 of all candidates)
Cryptogenic cirrhosis
Congenital hepatic fibrosis
Caroli's disease
Cystic fibrosis
Cirrhosis resulting from prolonged total
parenteral nutrition (often combined with small
bowel transplantation)

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HEPATOCYTE TRANSPLANTATION(HTX)

Hepatocyte transplantation can correct a
metabolic defect by serving as the essential
vehicle for ex vivo gene therapy or
by providing the vital enzyme that is deficient
in patients with a liver-based inborn error of
metabolism.
Hepatocyte transplantation can also function as a
life-saving bridge by providing a cellular mass
temporarily sufficient carry out metabolic
function for patients with liver failure awaiting
liver transplantation.

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Potential Applications of Hepatic Gene Therapy