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Autosomal Recessive Polycystic Kidney Disease

NORD is very grateful to Peter C. Harris, PhD, Professor Biochemistry/Molecular Biology and Medicine, Division of Nephrology and Hypertension, Mayo Clinic , for assistance in the preparation of this report.

Synonyms of Autosomal Recessive Polycystic Kidney Disease

  • polycystic kidney disease, infantile

Disorder Subdivisions

  • No subdivisions found.

General Discussion

Autosomal recessive polycystic kidney disease (ARPKD) is a rare genetic disorder characterized by the formation of fluid-filled sacs (cysts) in the kidneys. Most affected infants have enlarged kidneys during the newborn (neonatal) period and some cases may be fatal at this time. ARPKD is not simply a kidney disease and additional organ systems of the body may also be affected, especially the liver. High blood pressure (hypertension), excessive thirst, frequent urination and feeding difficulties may also occur. Some affected children may also have distinctive facial features and incomplete development of the lungs (pulmonary hypoplasia) causing breathing (respiratory) difficulties. The severity of the disorder and the specific symptoms that occur can vary greatly from one person to another. Some affected children eventually develop end-stage renal disease sometime during the first decade of life. In some cases, symptoms do not develop until adolescence or even adulthood. ARPKD is caused by mutations of the PKHD1 gene.


The severity and progression of ARPKD can vary greatly from one person to another, even among members of the same family. In severe cases, ARPKD can cause life-threatening complications during infancy. In other cases, affected individuals may not develop symptoms until later during childhood or adolescence. Some children may need a kidney (renal) transplant early in childhood; others may not need a transplant until early adulthood, or not at all. In rare cases, individuals may not develop symptoms until young adulthood. Generally, individuals who develop ARPKD later in life have milder kidney disease, but more severe liver disease.

Most of the medical literature on ARPKD, especially those written before the identification of the ARPKD disease gene, disproportionately focused on the most severe cases. Therefore, much of the literature may give the incorrect impression that ARPKD is a uniformly fatal or debilitating disease. Researchers now know that ARPKD cases can range from mild to severe. Consequently, it is important to note that affected individuals will not have all of the symptoms discussed below. Affected individuals should talk to their physician and medical team about their specific case, associated symptoms and overall prognosis.

The characteristic finding of ARPKD is the development of fluid-filled sacs (cysts) in the kidneys. All affected individuals develop cysts in the kidneys, but the number, size, progression and severity of cyst development varies greatly from one person to another. In most cases, renal cysts grow and multiply in utero causing abnormal enlargement of the kidneys. Enlarged kidneys may be apparent at birth or during the newborn period. In these infants, the kidneys are firm and can be felt (palpated) in both flanks. Additional symptoms associated with cystic kidneys include high blood pressure (hypertension) and flank pain. High blood pressure is common in children with ARPKD and can be widespread, severe and difficult to manage.

In severe cases of ARPKD, affected infants may face life-threatening complications shortly after birth, especially breathing (respiratory) insufficiency or failure. Breathing difficulties usually occur due to deficient levels of amniotic fluid (oligohydramnios) during pregnancy. Massively enlarged kidneys, which prevent the proper development of the lungs, may also contribute to respiratory insufficiency or failure. Although some children do not survive the newborn period (approximately 30 percent by most estimates), the majority of children are viable.

Children who survive beyond the newborn period usually develop worsening kidney function, although the kidneys may reduce in size. Most children do not develop chronic renal insufficiency until late childhood, adolescence or young adulthood. Renal insufficiency refers to the impaired ability of the kidneys to perform their basic functions. The kidneys are two bean-shaped organs located under the ribcage. The kidneys have several functions including filtering and excreting waste products from the blood and body, creating certain hormones, and helping maintain the balance of certain chemicals in the body such as potassium, sodium, chloride calcium and other electrolytes. Damage to the kidneys in ARPKD may be slowly progressive and can cause a variety of symptoms including weakness and fatigue, changes in appetite, puffiness or swelling, back pain, poor digestion, excessive thirst and frequent urination. Eventually, many children progress to end-stage renal disease.

In severe cases of ARPKD, affected infants have extremely enlarged kidneys and decreased urine production at birth. Decreased urine production in utero contributes to a deficiency of amniotic fluid (oligohydramnios), the fluid that surrounds a developing fetus. In addition to protecting and cushioning a fetus, amniotic fluid contains growth factors and other substances that are vital to fetal development. Low amniotic fluid levels can impair lung development and, consequently, some affected infants may have underdeveloped lungs (pulmonary hypoplasia). These infants can experience severe, life-threatening breathing (respiratory) complications during the newborn period. Infants with oligohydramnios may also develop distinctive facial features including deep-set eyes, a flattened nose, a small jaw (micrognathia), and abnormal, low-set ears. The physical findings associated with oligohydramnios are sometimes referred to as Potter’s sequence.

In addition to the kidneys, the liver is also commonly affected in children with ARPKD. The liver performs many functions in the body including converting food into energy and nutrients, storing vitamins, and filtering toxins from the body. Children with ARPKD develop a liver condition known as congenital hepatic fibrosis, in which excess fiber-like connective tissue spreads throughout the liver. Although all children have congenital hepatic fibrosis, not all children develop liver dysfunction. Liver abnormalities that can occur in ARPKD include enlargement of the liver (hepatomegaly), inflammation and infection of the tubes (bile ducts) that carry bile from the liver to the gallbladder and intestines (cholangitis), and high blood pressure of the main vein of the liver (portal hypertension).

Portal hypertension can cause increased pressure and swelling (distention) of veins (varices) of the esophagus, the stomach and intestines. These veins can rupture and potentially cause life-threatening gastrointestinal bleeding (variceal bleeding). Affected children may experience progressive liver dysfunction and scarring (cirrhosis) and ultimately liver failure.

Children with ARPKD may also experience feeding difficulties due to poor kidney function or from compression of the stomach by enlarged kidneys, liver and/or spleen. Feeding difficulties and chronic renal failure may contribute to poor growth in affected individuals. Some children may be prone to urinary tract infections and have problems with water and salt balance.

Some children with ARPKD may also experience enlargement of the spleen (splenomegaly). Splenomegaly can potentially result in low levels of red blood cells (anemia), platelets (thrombocytopenia) and white blood cells (leukopenia). Anemia can cause fatigue, pale skin, irregular heartbeat, and shortness of breath. Thrombocytopenia can result in easy bruising, prolonged bleeding from cuts, spontaneous nosebleeds, and superficial bleeding in the skin (petechiae). Leukopenia decreases the body’s ability to fight infection and disease.


ARPKD is caused by mutations of the PKHD1 gene, which is inherited as an autosomal recessive trait. Genetic diseases are determined by the combination of genes for a particular trait that are on the chromosomes received from the father and the mother.

Recessive genetic disorders occur when an individual inherits the same abnormal gene for the same trait from each parent. If an individual receives one normal gene and one gene for the disease, the person will be a carrier for the disease, but usually will not show symptoms. The risk for two carrier parents to both pass the defective gene and, therefore, have an affected child is 25 percent with each pregnancy. The risk to have a child who is a carrier like the parents is 50 percent with each pregnancy. The chance for a child to receive normal genes from both parents and be genetically normal for that particular trait is 25 percent. The risk is the same for males and females.

Investigators have determined that most typical cases of ARPKD are caused by mutation to a single gene, specifically the PKHD1 gene. The PKHD1 gene is located on the long arm (q) of chromosome 6 (6q21.1). PKHD1 is a large gene and many different mutations to this gene cause ARPKD.

Investigators have determined that the PKHD1 gene contains instructions for creating (encoding) a protein known as fibrocystin (or polyductin). If patients have two mutations that result in no protein being generated, the result is usually lethal. However, in the majority of patients at least one copy of the gene generates some protein and these cases are usually viable. The exact role and function of this protein in the body is unknown.

Investigators have determined that the ARPKD protein may be involved in the proper development or function of cilia, a hair-like structure found on most cells in the body. Cilia are classified as motile or immotile. Motile cilia have specific mechanical functions such as to move or propel mucus over the cell in the respiratory tract, while immotile (primary) cilia were believed to play a sensory or mechano-sensory role. Immotile cilia are active structures required for normal health and development that are involved in sensing the environment outside of the cell and sending related signals into the cell. The exact relationship between the ARPKD protein and the cilia and their ultimate roles in proper kidney function and health is not fully understood. More research is necessary to determine the complex, underlying mechanisms that ultimately cause ARPKD.

The symptoms of ARPKD result from the development and continued enlargement of cysts in the kidneys and other organ systems of the body. Cysts within the kidneys form within nephrons, which are small tubules that serve as the basic filtering units of the kidneys and help to remove waste from the blood. Cysts form at the tips or ends of the nephrons, a section known as the collecting tubules. Specifically, a cyst is a widened (dilated) collecting tubule that has swollen or ballooned. Because of the numerous cysts that form, the kidneys become enlarged and normal nephrons are destroyed, eventually eliminating kidney function. In a normal kidney, the nephrons and collecting tubules help to regulate the amount of water and acid in the body.

The liver symptoms of ARPKD result from the improper development of the network of bile ducts found within the liver. Bile ducts may be widened (dilated) and duplicated and surrounding tissue may become inflamed, ultimately causing scarring in the affected area. This scarring process is known as congenital hepatic fibrosis. All children with ARPKD have congenital hepatic fibrosis, but not all children develop clinically evident liver disease.

Affected Populations

ARPKD affects males and females in equal numbers. The incidence of ARPKD is estimated to occur in approximately 1 in 20,000 individuals in the general population. Because some cases may go undiagnosed, it is difficult to determine the true frequency of ARPKD is the general population. Although most cases are diagnosed in utero or at birth, mild cases may not become apparent until adolescence or adulthood. ARPKD can affect individuals of any ethnic group.

Related Disorders

Symptoms of the following disorders can be similar to those of ARPKD. Comparisons may be useful for a differential diagnosis.

Autosomal dominant polycystic kidney disease (ADPKD) is a genetic disorder characterized by the formation of cysts within the kidneys. Since ADPKD is a dominant disease, in most cases affected individuals have a family history of PKD, unlike ARPKD. Symptoms caused by cyst formation in the kidneys include high blood pressure (hypertension), pain on the sides of the body between the last rib and the hip (flank pain), blood in the urine (hematuria) and progressively poor function of the kidneys (kidney insufficiency). In at least 50 percent of cases, ADPKD eventually progresses to end stage renal disease, requiring renal replacement therapy, either dialysis or renal transplantation. ADPKD is not simply a kidney disorder and other organ systems of the body can potentially be affected (multisystem disorder) by the development of cysts and other disease. The specific symptoms present in each person depend upon the specific organ systems involved. The liver, pancreas, a membrane covering the spinal cord and brain (arachnoid membrane), and the glands of the male reproductive tract that produce fluid that is part of semen (seminal vesicles) may develop cysts. Abnormalities affecting the heart and blood vessels (cardiovascular system) may also occur in individuals with ADPKD. ADPKD usually does not become apparent until the fourth or fifth decade and was once known as “adult” polycystic kidney disease. However, it has been reported in children and infants. ADPKD is caused by mutations of one of two genes that create certain proteins essential for the proper health of the kidneys and other parts of the body. Rarely, atypical mutations to the ADPKD genes can manifest with an ARPKD-like phenotype. (For more information on this disorder, choose “ADPKD” as your search term in the Rare Disease Database.)

A variety of different disorders may have cystic kidneys as a feature. These disorders may sometimes be referred to as syndromic forms of polycystic kidney. These disorders usually have additional neurological, digital, eye and/or other symptoms and physical findings that distinguish them from ARPKD. These disorders include Bardet-Biedl syndrome, Meckel syndrome, Joubert syndrome, Senior-Loken syndrome, nephronophthisis, and oral-facial-digital syndrome. (For more information on these disorders, choose the specific disorder name as your search term in the Rare Disease Database.)

Standard Therapies

ARPKD may be suspected before birth based upon clinical findings (e.g., palpable flank mass, underdeveloped lungs, oligohydramnios, and hypertension). Radiologic imaging including sonograms, ultrasound and magnetic resonance imaging (MRI) can be used to aid in obtaining a diagnosis of ARPKD. In addition to detecting kidney abnormalities, various radiologic imaging techniques can also be used to identify non-obstructive widening (dilatation) of the intraheptic ducts within the liver.

A prenatal ultrasound may reveal enlarged kidneys (as early 18 weeks after conception in some cases). An ultrasound may also reveal innumerable small cysts that are actually dilated collecting tubules. True renal cysts may also be present. An ultrasound, however, may fail to detect kidney enlargement or oligohydramnios.

Genetic testing for mutations in the PKHD1 genes is available at several different laboratories (see GeneTests website: /). Genetic testing may be employed for prenatal or preimplantation genetic diagnostics for some at-risk families who have had at least one pregnancy diagnosed with ARPKD.

The treatment of ARPKD is directed toward the specific symptoms that are apparent in each individual. Specific treatments are aimed at preserving kidney and liver function. In infancy many children with respiratory difficulties may require mechanical ventilation to assist breathing. Medications such as nitric oxide can help provide oxygen to (oxygenate) the lungs.

In severe cases, newborns who experience decreased urine production (oliguria) or no passage of urine (anuria) may require peritoneal dialysis during the first few days of life.

Medications can be used to control and manage high blood pressure, specifically angiotensin-converting enzyme (ACE) inhibitors. In some cases, high blood pressure can be resistant to therapy (refractory) and severe enough to require more than one medication. Antibiotics may be used to treat urinary tract infections or cholangitis.

Some children may require nutritional supplements including vitamin D, iron, bicarbonate and citrate. Adequate fluid and salt supplementation may also be necessary. Because of feeding difficulties and growth delays, some children may require the insertion of a tube through a small surgical opening in the stomach (gastrostomy) or a tube through the nose, down the esophagus and into the stomach (nasogastric tube). These tubes are used to directly provide essential nutrients. In severe cases, growth hormone therapy may be necessary.

Individuals with end-stage renal disease, in which the kidneys no longer function, require dialysis or kidney transplant. Dialysis is a procedure in which a machine is used to perform some of the functions of the kidney – filtering waste products from the bloodstream, helping to control blood pressure and helping to maintain proper levels of essential chemicals such as potassium. End-stage renal disease is not reversible so individuals will require lifelong dialysis treatment or a kidney transplant. The rate of progression of kidney dysfunction to end-stage renal disease can vary greatly from one person to another. Some individuals require a kidney transplant in childhood, others may not require a transplant until adulthood, or not at all.

Progressive portal hypertension may require treatment with a portacaval shunt, in which a connection is made between the portal vein and the inferior vena cava, the main vein that drains blood from the lower two-thirds of the body. A portacaval shunt is designed to relieve high blood pressure of the portal vein.

Variceal bleeding is a medical emergency and requires immediate treatment. Variceal bleeding may be treated by sclerotherapy, a procedure in which a solution such as sodium chloride is injected into an affected blood vessel. The solution irritates the blood vessel eventually causing it to scar and the blood to clot. A small percentage of individuals with ARPKD may eventually require liver transplantation.

Erythropoietin may be used to stimulate the bone marrow to produce red blood cells in some children with ARPKD who experience anemia. Surgical removal of the spleen (splenectomy) has been used in some cases to treat severe splenomegaly.

Genetic counseling may be of benefit for affected individuals and their families. Other treatment is symptomatic and supportive.

Investigational Therapies

Information on current clinical trials is posted on the Internet at All studies receiving U.S. government funding, and some supported by private industry, are posted on this government web site.

For information about clinical trials being conducted at the NIH Clinical Center in Bethesda, MD, contact the NIH Patient Recruitment Office:

Toll-free: (800) 411-1222
TTY: (866) 411-1010

For information about clinical trials sponsored by private sources, in the main, contact:

Contact for additional information about autosomal recessive polycystic kidney disease:

Peter C. Harris, PhD
Professor Biochemistry/Molecular Biology and Medicine
Division of Nephrology and Hypertension
Mayo Clinic
200 First Street
Rochester, MN 55905
Tel: 507-266-0541 or 507-255-3774
Fax: 507-266-9315

Autosomal Recessive Polycystic Kidney Disease Resources

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Kher KK, Schnaper HW, Makker SP, eds. Clinical Pediatric Neurology. 2nd ed. Informa UK Ltd. London, UK; 2007:261-274.

Meyers KEC. Autosomal-Recessive Polycystic Kidney Disease. NORD Guide to Rare Disorders. Lippincott Williams & Wilkins. Philadelphia, PA. 2003:697.

Rimoin D, Connor JM, Pyeritz RP, Korf BR. Eds. Emory and Rimoin’s Principles and Practice of Medical Genetics. 4th ed. Churchill Livingstone. New York, NY; 2002:1693-1707.

Welling LW, Grantham JJ. Cystic and Developmental Diseases of the Kidney. In: Brenner BM, Rector Jr FC. Eds. The Kidney. 4th ed. Philadelphia: W.B. Saunders Company;1991:1657-1694.

Harris PC, Torres VE. Polycystic kidney disease. Ann Rev Med. 2009;60:321-337.

Ibraghinov-Beskrovnaya O, Bukanov N. Polycystic kidney disease: from molecular discoveries to targeted therapeutic strategies. Cell Mol Life Sci. 2008;65:605-619.

Rossetti S, Harris PC. Genotype-phenotype correlations in autosomal dominant and autosomal recessive polycystic kidney disease. J Am Soc Nephrol. 2007;18:1374-1380.

Guary-Woodford LM. Renal cystic diseases: diverse phenotypes converge on the cilium/centrosome complex. Pedistr Nephrol. 2006;21:1369-1376.

Adeva M, El-Youssef M, Rossetti S, et al. Clinical and molecular characterization defines a broadened spectrum of autosomal recessive polycystic kidney disease (ARPKD). Medicine (Baltimore). 2005;85:1-21.

Guay-Woodford LM, Desmond RA. Autosomal recessive polycystic kidney disease: the clinical experience in North America. Pediatrics. 2003;111:1072-1080.

Bergmann C, Senderek J, Windelen E, et al. Clinical consequences of PKHD1 mutations in 164 patients with autosomal-recessive polycystic kidney disease (ARPKD). Kidney Intl. 2005;67:829-848.

Bergmann C, Senderek J, Kupper F, et al. PKHD1 mutations in autosomal recessive polycystic kidney disease (ARPKD). Hum Mutat. 2004;23:453-463.

MacRae Dell K, Avner ED. Updated 07/14/2009. Polycystic Kidney Disease, Autosomal Recessive. In: GeneReviews at GeneTests: Medical Genetics Information Resource (database online). Copyright, University of Washington, Seattle. 1997-2003. Available at

Niaudet P. Autosomal recessive polycystic kidney disease. Orphanet encyclopedia, March 2004. Available at: Accessed May 20, 2010.

McKusick VA., ed. Online Mendelian Inheritance in Man (OMIM). Baltimore. MD: The Johns Hopkins University; Entry No:263200; Last Update:04/29/2008. Available at: Accessed May 20, 2010.

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Report last updated: 2011/04/13 00:00:00 GMT+0

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