Dubin–Johnson syndrome

Classification	ICD-10: E80.6; ICD-9-CM: 277.4; OMIM: 237500; MeSH: D007566; DiseasesDB: 3982;
External resources	MedlinePlus: 000242; eMedicine: med/588; Orphanet: 234;

Dubin–Johnson syndrome is a rare, autosomal recessive, benign disorder that causes an isolated increase of conjugated bilirubin in the serum. Classically, the condition causes a black liver due to the deposition of a pigment similar to melanin.^[1] This condition is associated with a defect in the ability of hepatocytes to secrete conjugated bilirubin into the bile, and is similar to Rotor syndrome. It is usually asymptomatic, but may be diagnosed in early infancy based on laboratory tests. No treatment is usually needed.^[1]

Pathophysiology[edit | edit source]

The conjugated hyperbilirubinemia is a result of defective endogenous and exogenous transfer of anionic conjugates from hepatocytes into bile.^[2] Impaired biliary excretion of bilirubin glucuronides is due to a mutation in the canalicular multiple drug-resistance protein 2 (MRP2). A darkly pigmented liver is due to polymerized epinephrine metabolites, not bilirubin.^[3]

Dubin–Johnson syndrome has an autosomal recessive pattern of inheritance.

Dubin–Johnson syndrome is due to a defect in the multiple drug resistance protein 2 gene (ABCC2), located on chromosome 10.^[1] It is an autosomal recessive disease and is likely due to a loss of function mutation, since the mutation affects the cytoplasmic/binding domain.

Diagnosis[edit | edit source]

A hallmark of Dubin–Johnson syndrome is the unusual ratio between the byproducts of heme biosynthesis:

Unaffected subjects have a coproporphyrin III to coproporphyrin I ratio around 3–4:1.
In patients with Dubin–Johnson syndrome, this ratio is inverted, with coproporphyrin I being 3–4 times higher than coproporphyrin III. Analysis of urine porphyrins shows a normal level of coproporphyrin, but the I isomer accounts for 80% of the total (normally 25%).

For the first two days of life, healthy neonates have ratios of urinary coproporphyrin similar to those seen in patients with Dubin–Johnson syndrome; by 10 days of life, however, these levels convert to the normal adult ratio.^[4]

In post mortem autopsy, the liver will have a dark pink or black appearance due to pigment accumulation.

Plentiful canalicular multiple drug-resistant protein causes bilirubin transfer to bile canaliculi. An isoform of this protein is localized to the apical hepatocyte membrane, allowing transport of glucuronide and glutathione conjugates back into the blood. High levels of gamma-glutamyl transferase (GGT) help in diagnosing pathologies involving biliary obstruction.^{[citation needed]}

Differentiation from Rotor syndrome[edit | edit source]

Dubin–Johnson syndrome is similar to Rotor syndrome, but can be differentiated by:

	Rotor syndrome	Dubin–Johnson syndrome
Appearance of liver	normal histology and appearance	liver has black pigmentation
Gallbladder visualization	gallbladder can be visualized by oral cholecystogram	gallbladder cannot be visualized
Total urine coproporphyrin content	high with <70% being isomer 1	normal with >80% being isomer 1 (normal urine contains more of isomer 3 than isomer 1)

A test of MRP2 activity can also be done to differentiate between Dubin–Johnson syndrome and Rotor syndrome. The clearance of bromsulphthalein is used to determine this, the test for which is called bromsulphthalein clearance test. 100 units of BSP is injected intravenously and then the clearance. In case of Dubin–Johnson syndrome, clearance of bromsulphthalein will be within 90 minutes, while in case of Rotor syndrome, the clearance is slow, i.e., it takes more than 90 minutes for clearance.^{[citation needed]}

Treatment[edit | edit source]

Dubin–Johnson syndrome is a benign condition and no treatment is required. However, it is important to recognize the condition so as not to confuse it with other hepatobiliary disorders associated with conjugated hyperbilirubinemia that require treatment or have a different prognosis.^[5]

Prognosis[edit | edit source]

Prognosis is good, and treatment of this syndrome is usually unnecessary. Most patients are asymptomatic and have normal lifespans.^[2] Some neonates present with cholestasis.^[2] Hormonal contraceptives and pregnancy may lead to overt jaundice and icterus (yellowing of the eyes and skin).^{[citation needed]}

History[edit | edit source]

Dubin–Johnson syndrome was first described in 1954 by two men — Dr. Frank Johnson, a military physician and researcher at the Veterans Administration and Armed Forces Institute of Pathology in Washington, DC, and Dr. Isadore Dubin, a Canadian pathologist then working alongside him.^[6] Dr. Johnson had studied medicine at Howard University College of Medicine and faced substantial discrimination in his medical career, on account of being an African-American, and was even turned away from active duty during the Battle of the Bulge, despite being a first lieutenant and trained physician.^[7] Later, during his internship, he was required to sleep in a tuberculosis sanitarium, as the hospital did not allow African-American physicians to live in the same residencies as white physicians, and he was prevented from rotating on several services, including general surgery.^[7] These experiences, coupled with his inherent interest in chemistry, compelled him to pursue pathology, where he ultimately met Dr. Dubin and described this syndrome for the first time.^{[citation needed]}

References[edit | edit source]

↑ ^1.0 ^1.1 ^1.2
↑ ^2.0 ^2.1 ^2.2 Suzanne M Carter, MS Dubin–Johnson Syndrome at eMedicine
↑
↑
↑ Up-to-date: "Inherited disorders associated with conjugated hyperbilirubinemia"
↑
↑ ^7.0 ^7.1 Kennedy, Charles Stuart (1992). Dr. Frank B. Johnson Oral History Interview. Armed Forces Institute of Pathology Oral History Program. Archived by the Internet Archive, retrieved March 24, 2016.

External links[edit | edit source]

Dubin-Johnson syndrome at ght.nlm.nig.gov
Dubin-Johnson syndrome at Medline Plus encyclopedia
Dubin–Johnson syndrome at NIH's Office of Rare Diseases

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[strassburg2010-1] 1.0 ^1.1 ^1.2

[Carter-2] 2.0 ^2.1 ^2.2 Suzanne M Carter, MS Dubin–Johnson Syndrome at eMedicine

[3] ↑

[4] ↑

[5] Up-to-date: "Inherited disorders associated with conjugated hyperbilirubinemia"

[dubin1954-6] ↑

[johnson_interview-7] 7.0 ^7.1 Kennedy, Charles Stuart (1992). Dr. Frank B. Johnson Oral History Interview. Armed Forces Institute of Pathology Oral History Program. Archived by the Internet Archive, retrieved March 24, 2016.

[1]

[2]

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[5]

[6]

[7]

v t e Genetic disorder, membrane: ABC-transporter disorders
ABCA	ABCA1 (Tangier disease) ABCA3 (Surfactant metabolism dysfunction 3) ABCA4 (Stargardt disease 1, Retinitis pigmentosa 19) ABCA12 (Harlequin-type ichthyosis, Lamellar ichthyosis 2)
ABCB	ABCB4 (Progressive familial intrahepatic cholestasis 3) ABCB7 (ASAT) ABCB11 (Progressive familial intrahepatic cholestasis 2)
ABCC	ABCC2 (Dubin–Johnson syndrome) ABCC6 (Pseudoxanthoma elasticum) ABCC7 (Cystic fibrosis) ABCC8 (HHF1, TNDM2) ABCC9 (Dilated cardiomyopathy 1O)
ABCD	ABCD1 (Adrenoleukodystrophy, Adrenomyeloneuropathy)
ABCG	ABCG5 (Sitosterolemia) ABCG8 (Gallbladder disease 4, Sitosterolemia)
see also ABC transporters