BNF for Children (BNFC) 2018-2019

7 Liver disorders and related

conditions

7.1 Biliary disorders

Cholestasis 01-May-2017

Description of condition

Cholestasis is an impairment of bile formation and/or bile

flow, which may clinically present with fatigue, pruritus,

dark urine, pale stools and, in its most overt form, jaundice

and signs of fat soluble vitamin deficiencies.

Treatment

gUrsodeoxycholic acid p. 65 [unlicensed] and

colestyramine p. 129 [unlicensed under 6 years] are used to

relieve cholestatic pruritus in children, even if evidence to

support their use is limited.

Colestyramine is an anion-exchange resin that is not

absorbed from the gastro-intestinal tract. It relieves pruritus

by forming an insoluble complex in the intestine with bile

acids and other compounds—the reduction of serum bile

acid levels reduces excess deposition in the dermal tissue

with a resultant decrease in pruritus.

Under specialist supervision, other drugs which may be

used as an alternative treatment forintractablecholestatic

pruritus include rifampicin p. 364 [unlicensed indication],

phenobarbital p. 216 [unlicensed indication] and opioid

antagonists [unlicensed indication]. However, they should be

used with caution and under expert guidance as these

children usually have severe liver disease—careful

monitoring is required.l

Inborn errors of primary bile acid

synthesis 27-Apr-2018

Description of condition

Inborn errors of primary bile acid synthesis are a group of

diseases in which the liver does not produce enough primary

bile acids due to enzyme deficiencies. These acids are the

main components of the bile, and include cholic acid and

chenodeoxycholic acid.

Treatment

Cholic acid p. 65 is licensed for the treatment of inborn

errors of primary bile acid synthesis due to an inborn

deficiency of two specific liver enzymes. It acts by replacing

some of the missing bile acids, therefore relieving the

symptoms of the disease.

Chenodeoxycholic acid below is licensed for the treatment

of inborn errors of primary bile acid synthesis due to a

deficiency of one specific enzyme in the bile acid synthesis

pathway when presenting as cerebrotendinous

xanthomatosis.

Ursodeoxycholic acid p. 65 [unlicensed indication] has

been used to treat inborn errors in primary bile acid

synthesis, but there is an absence of evidence to recommend

its use.

Primary biliary cholangitis 30-May-2017

Description of condition

Primary biliary cholangitis (or primary biliary cirrhosis) is a

chronic cholestatic disease which develops due to

progressive destruction of small and intermediate bile ducts

within the liver, subsequently evolving tofibrosis and

cirrhosis.

Treatment

gUrsodeoxycholic acid p. 65 is recommended for the

management of primary biliary cholangitis, including those

with asymptomatic disease. It slows disease progression, but

the effect on overall survival is uncertain.h

Smith-Lemli-Opitz syndrome 30-May-2017

Description of condition

Smith-Lemli-Opitz syndrome is an inborn error of

cholesterol synthesis. It is characterised by multiple

congenital anomalies, intellectual deficit, growth delay,

microcephaly, and behavioural problems. The disease is

present at birth, but may be detected in later childhood or

adulthood in mild forms. Hypoglycaemia due to adrenal

insufficiency can present as an acute manifestation.

Aims of treatment

There is currently no cure for Smith-Lemli-Opitz syndrome.

Management is aimed at symptom relief and alleviation of

functional disabilities.

Treatment

gChildren with Smith-Lemli-Opitz syndrome are treated

with dietary cholesterol supplementation, including high

cholesterol foods (such as egg yolks) or a suspension of

pharmaceutical grade cholesterol p. 66 (available from

Special-order manufacturers p. 1066 or specialist importing

companies) to help improve growth failure and

photosensitivity.lHowever, it is not clear who will benefit

most from cholesterol treatment or how long it should

continue.

gIn some cases bile acid supplements, such as

chenodeoxycholic acid below [unlicensed] and

ursodeoxycholic acid p. 65 [unlicensed indication] have been

also used for this condition, but their use is not generally

recommended.l

BILE ACIDS

Chenodeoxycholic acid 05-Apr-2018

lINDICATIONS AND DOSE

Cerebrotendinous xanthomatosis (specialist use only)

▶BY MOUTH

▶Child:Initially 5 mg/kg daily in 3 divided doses,

adjusted according to response; maximum 15 mg/kg

per day; maximum 1000 mg per day

Defective synthesis of bile acid (specialist use only)

▶BY MOUTH

▶Neonate:Initially 5 mg/kg 3 times a day, reduced to

2. 5 mg/kg 3 times a day.

▶Child:Initially 5 mg/kg 3 times a day, reduced to

2. 5 mg/kg 3 times a day

Smith-Lemli-Opitz syndrome (specialist use only)

▶BY MOUTH

▶Neonate: 7 mg/kg once daily, alternatively 7 mg/kg daily

in divided doses.

▶Child: 7 mg/kg once daily, alternatively 7 mg/kg daily in

divided doses

lUNLICENSED USENot licensed for defective synthesis of

bile acid. Not licensed for Smith-Lemli-Opitz syndrome.

lCONTRA-INDICATIONSNon-functioning gall bladder.

radio-opaque stones

64 Liver disorders and related conditions BNFC 2018 – 2019

Gastro-intestinal system

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