Erythropoietic protoporphyria (or commonly called EPP) is a form of porphyria, which varies in severity and can be very painful. It arises from a deficiency in the enzyme ferrochelatase, leading to abnormally high levels of protoporphyrin in the red blood cells (erythrocytes), plasma, skin, and liver.[2] The severity varies significantly from individual to individual.
Erythropoietic protoporphyria | |
---|---|
Other names | EPP[1] |
Chronic skin lesions of EPP | |
Specialty | Endocrinology, dermatology |
Risk factors | pain and irritation |
A clinically similar form of porphyria, known as X-Linked dominant protoporphyria, was identified in 2008.[3]
Presentation
editEPP usually presents in childhood with the most common mode of presentation as acute photosensitivity of the skin. It affects areas exposed to the sun and tends to be intractable. A few minutes of exposure to the sun induces pruritus, erythema, swelling and pain.[4] Longer periods of exposure may induce second degree burns. After repetitive exposure, patients may present with lichenification, hypopigmentation, hyperpigmentation and scarring of the skin.[5][6]
EPP usually first presents in childhood, and most often affects the face and the upper surfaces of the arms, hands, and feet and the exposed surfaces of the legs. Most patients, if the EPP is not as severe, manifest symptoms with onset of puberty when the male and female hormone levels elevate during sexual development and maintenance. More severe EPP can manifest in infancy. EPP can be triggered through exposure to sun even though the patient is behind glass. Even the UV emissions from arc welding with the use of full protective mask have been known to trigger EPP. EPP can also manifest between the ages of 3 and 6.[citation needed]
Prolonged exposure to the sun can lead to edema of the hands, face, and feet, rarely with blistering and petechiae. Skin thickening can sometimes occur over time.[citation needed]
People with EPP are also at increased risk to develop gallstones.[7] One study has noted that EPP patients suffer from vitamin D deficiency.[8]
Liver failure
editProtoporphyrin accumulates to toxic levels in the liver in 5–20% of EPP patients, leading to liver failure. The spectrum of hepatobiliary disease associated with EPP is wide. It includes cholelithiasis, mild parenchymal liver disease, progressive hepatocellular disease and end-stage liver disease.[5]
A lack of diagnostic markers for liver failure makes it difficult to predict which patients may experience liver failure, and the mechanism of liver failure is poorly understood. A retrospective European study identified 31 EPP patients receiving a liver transplant between 1983 and 2008, with phototoxic reactions in 25% of patients who were unprotected by surgical light filters. The same study noted a 69% recurrence of the disease in the grafted organ. Five UK liver transplants for EPP have been identified between 1987 and 2009. Frequent liver testing is recommended in EPP patients where no effective therapy has been identified to manage liver failure to date.[9]
Pregnancy
editEPP photosensitivity symptoms are reported to lessen in some female patients during pregnancy and menstruation, although this phenomenon is not consistent, and the mechanism is not understood.[10] This brings evidence that the pathology of the disorder may be mediated partially by the sex hormones.
Genetics
editMost cases of EPP are results of inborn errors of metabolism[2] but the metabolic defect in some patients may be acquired.[11] Mutation of the gene that encodes for ferrochelatase in the long arm of chromosome 18 is found in majority of the cases. Ferrochelatase (FECH) catalyzes the insertion of ferrous iron into the protoporphyrin IX ring to form heme. EPP exhibits both recessive and dominant patterns of inheritance and a high degree of allelic heterogeneity with incomplete penetrance. Most heterozygotes are asymptomatic. Symptoms do not occur unless FECH activity is less than 30% of normal, but such low levels are not present in a majority of patients.[12]
Pathophysiology
editCells which synthesize heme are predominantly erythroblasts/reticulocytes in the bone marrow (80%) and hepatocytes (20%). Deficiency of FECH results in increased release of protoporphyrin, which binds to albumin in plasma and subsequently undergoes hepatic extraction. Normally, most protoporphyrin in hepatocytes is secreted into bile; the remainder undergoes transformation into heme. Some protoporphyrin in bile is returned to the liver as a consequence of the enterohepatic circulation; the remaining protoporphyrin in the intestine undergoes fecal excretion. Protoporphyrin is insoluble and hence unavailable for renal excretion. In EPP, subnormal biotransformation of protoporphyrin into heme results in accumulation of protoporphyrin in hepatocytes.[13]
Since FECH deficiency is associated with increased concentrations of protoporphyrin in erythrocytes, plasma, skin and liver, retention of protoporphyrin in skin predisposes to acute photosensitivity. As a result of absorption of ultraviolet and visible light (peak sensitivity at 400 nm, with lesser peaks between 500–625 nm[14]) by protoporphyrin in plasma and erythrocytes when blood circulates through the dermal vessels, free radicals are formed, erythrocytes become unstable and injury to the skin is induced.[5]
A significant increase in the hepatobiliary excretion of protoporphyrin can damage the liver through both cholestatic phenomena and oxidative stress[13]—predisposing to hepatobiliary disease of varying degrees of severity.[15][16]
Diagnosis
editEPP is generally suspected by the presence of acute photosensitivity of the skin and can be confirmed by detection of a plasmatic fluorescence peak at 634 nm. It is also useful to find increased levels of protoporphyrin in feces and the demonstration of an excess of free protoporphyrin in erythrocytes.[17]
Screening for FECH mutation on one allele or aminolevulinic acid synthase 2 gain-of-function mutation in selected family members may be useful, especially in genetic counseling.
Liver biopsy confirms hepatic disease in EPP by the presence of protoporphyrin deposits in the hepatocytes that can be observed as a brown pigment within the biliary canaliculi and the portal macrophages. Macroscopically, the cirrhotic liver can have a black color due to protoporphyrin deposits. Using polarized light the characteristic Maltese cross shape of birefringent crystalline pigment deposits is found. The examination of liver tissue under a Wood’s lamp reveals a red fluorescence due to protoporphyrin. Liver biopsy is not helpful for estimation of prognosis of liver disease.[15]
Treatment
editThere is no cure for this disorder; however, symptoms can usually be managed by limiting exposure to daytime sun and some types of artificial lighting. Most types of artificial lighting emit light in the problematic wavelengths, with fluorescent lighting being the worst offender. Color temperature can be a good indicator of what light is most detrimental, as the higher the color temperature, the more violet light (380–450 nm) is emitted. Incandescent and LED lighting in the soft white range (2700–3000 K) produce the least problematic light. Additionally, selecting lower wattage bulbs can reduce the overall output of light.
Since the photosensitivity results from light in the visible spectrum, most sunscreens are of little use (with the exception of non-nano zinc oxide which provides uniform protection between 290–400 nm and some protection up to 700 nm[18]). Sun protective clothing can also be very helpful, although clothing with UPF values are only rated based on their UV protection (up to 400 nm) and not on their protection from the visible spectrum. Some sun protective clothing manufacturers use zinc oxide in their fabrics, such as Coolibar's ZnO Suntect line, which will offer protection from visible light.[19]
Window films which block UV and visible light up to 450 nm can provide relief from symptoms if applied to the patient's automobile and home windows.
Blue blocking screen protectors can help provide relief from symptoms caused by televisions, phones, tablets and computer screens.
EPP is considered one of the least severe of the porphyrias. Unless there is liver failure, it is not a life-threatening disease.
Approved therapies
editAfamelanotide, developed by Australian-based Clinuvel Pharmaceuticals, was approved in Europe in December 2014 and in the United States in October 2019 for treatment or prevention of phototoxicity in adults with EPP.[20][21]
Off-label therapies
editSeveral drugs are used off label by patients with EPP:
- Ursodeoxycholic acid is a bile acid that is administered to promote biliary secretion of protoporphyrin. Results of its use in EPP are controversial. However, it is known to alter the composition of bile, to protect hepatocytes from the cytotoxic effect of hydrophobic bile acids, and to stimulate biliary secretion by several distinct mechanisms.[22][23]
- Hematin appears to reduce excess protoporphyrin production in the bone marrow. It has been administered to patients with EPP (3–4 mg/kg iv) who develop a crisis after liver transplantation.[24]
- Plasmapheresis can also decrease the levels of protoporphyrin in plasma, however its use in treating acute episodes is controversial.[25]
- Cholestyramine is an orally administered resin which reduces circulating levels of protoporphyrin by binding to protoporphyrin in the intestine and, hence, interrupting the enterohepatic circulation. It is usually used in combination with other treatment approaches.[26]
- Activated carbon, like cholestyramine, binds to protoporphyrin in the intestine and prevents its absorption. It is cheap and readily available. It seems to be effective in reducing circulating protoporphyrin levels.[27]
Bone marrow transplantation, liver transplantation, acetylcysteine, extracorporeal albumin dialysis, parenteral iron and transfusion of erythrocytes are alternative plans for treatment of EEP.
Over-the-counter drug
editSome over-the-counter drugs may help:
- Proferrin is an oral heme supplement which may work similarly to Hematin.
- B. subtilis (a gram-positive soil probiotic) produces ferrochelatase,[28] which may be able to convert some of the protoporphyrin in the intestine into heme.
- Beta carotene, though a recent meta analysis of carotene treatment has called its effectiveness into question.[29]
Experimental therapies
editBitopertin has been undergoing trials in Australia since 2022 with some success in allowing participants to spend more time in full sunlight without ill effects. [30]
Home remedies
editAlthough erythropoietic protoporphyria symptoms may be temporarily suppressed with cold temperatures, patients have found that this method may extend, or even intensify pain and discomfort. However, home treatments that increase blood flow to the affected areas, such as immersion in warm water with quick drying or warm dry compresses, may increase the rate of pain relief. This has been noted as particularly effective in the hands, forearms, and face, as areas of decreased blood flow may be exposed to the accumulation of protoporphyrins for an extended period. [31]
Epidemiology
editCase reports suggest that EPP is prevalent globally. The prevalence has been estimated somewhere between 1 in 75,000 and 1 in 200,000[32] however it has been noted that the prevalence of EPP may be increasing due to a better understanding of the disease and improved diagnosis.[33] An estimated 5,000–10,000 individuals worldwide have EPP.[medical citation needed] EPP is considered the most common form of porphyria in children.[34] The prevalence in Sweden has been published as 1:180,000.[35]
History
editErythropoietic protoporphyria was first described in 1953 by Kosenow and Treibs[36] and completed in 1960 by Magnus et al. at the St John's Institute of Dermatology in London.[37]
See also
editReferences
edit- ^ "Autosomal erythropoietic protoporphyria". Orphanet. Retrieved 17 April 2019.
- ^ a b Casanova-González MJ, Trapero-Marugán M, Jones EA, Moreno-Otero R (September 2010). "Liver disease and erythropoietic protoporphyria: a concise review". World Journal of Gastroenterology. 16 (36): 4526–4531. doi:10.3748/wjg.v16.i36.4526. PMC 2945483. PMID 20857522.
- ^ Seager MJ, Whatley SD, Anstey AV, Millard TP (January 2014). "X-linked dominant protoporphyria: a new porphyria". Clinical and Experimental Dermatology. 39 (1): 35–37. doi:10.1111/ced.12202. PMID 24131146. S2CID 1971165.
- ^ Wensink D, Langendonk JG, Overbey JR, Balwani M, Van Broekhoven EJ, Wagenmakers MA, et al. (September 2021). "Erythropoietic protoporphyria: time to prodrome, the warning signal to exit sun exposure without pain-a patient-reported outcome efficacy measure". Genetics in Medicine. 23 (9): 1616–1623. doi:10.1038/s41436-021-01176-z. PMID 33941881. S2CID 233719987.
- ^ a b c Tsuboi H, Yonemoto K, Katsuoka K (November 2007). "Erythropoietic protoporphyria with eye complications". The Journal of Dermatology. 34 (11): 790–794. doi:10.1111/j.1346-8138.2007.00386.x. PMID 17973823. S2CID 23093030.
- ^ Poh-Fitzpatrick MB (June 1986). "Molecular and cellular mechanisms of porphyrin photosensitization". Photo-Dermatology. 3 (3): 148–157. PMID 3529055.
- ^ Bonkovsky HL, Rudnick SR (December 2020). "Erythropoietic Protoporphyria and X-Linked Protoporphyria - Hormonal and Metabolic Disorders". Merck Manuals Consumer Version. Merck Sharp & Dohme Corp. Retrieved 11 January 2021.
- ^ Spelt JM, de Rooij FW, Wilson JH, Zandbergen AA (December 2010). "Vitamin D deficiency in patients with erythropoietic protoporphyria". Journal of Inherited Metabolic Disease. 33 (Suppl 3): S1–S4. doi:10.1007/s10545-008-1037-0. PMID 24137761. S2CID 22847583.
- ^ "Erythropoietic Protoporphyria (EPP) and X-Linked Protoporphyria (XLP)". American Porphyria Foundation. Retrieved 2022-01-26.
- ^ Wahlin S, Marschall HU, Fischler B (June 2013). "Maternal and fetal outcome in Swedish women with erythropoietic protoporphyria". The British Journal of Dermatology. 168 (6): 1311–1315. doi:10.1111/bjd.12242. PMID 23738640. S2CID 37761662.
- ^ Blagojevic D, Schenk T, Haas O, Zierhofer B, Konnaris C, Trautinger F (July 2010). "Acquired erythropoietic protoporphyria" (PDF). Annals of Hematology. 89 (7): 743–744. doi:10.1007/s00277-009-0859-7. PMID 19902211. S2CID 36170513.
- ^ Kong XF, Ye J, Gao DY, Gong QM, Zhang DH, Lu ZM, et al. (February 2008). "Identification of a ferrochelatase mutation in a Chinese family with erythropoietic protoporphyria". Journal of Hepatology. 48 (2): 375–379. doi:10.1016/j.jhep.2007.09.013. PMID 18160121.
- ^ a b Holme SA, Worwood M, Anstey AV, Elder GH, Badminton MN (December 2007). "Erythropoiesis and iron metabolism in dominant erythropoietic protoporphyria". Blood. 110 (12): 4108–4110. doi:10.1182/blood-2007-04-088120. PMID 17804693.
- ^ Magnus IA (February 1968). "Photobiological aspects of porphyria". Proceedings of the Royal Society of Medicine. 61 (2): 196–198. doi:10.1177/003591576806100233. PMC 1902233. PMID 5688974.
- ^ a b Lecha M, Puy H, Deybach JC (September 2009). "Erythropoietic protoporphyria". Orphanet Journal of Rare Diseases. 4: 19. doi:10.1186/1750-1172-4-19. PMC 2747912. PMID 19744342.
- ^ Bruguera M, Herrero C (December 2005). "[Liver disease in erythropoietic protoporphyria]". Gastroenterologia y Hepatologia. 28 (10): 632–636. doi:10.1016/s0210-5705(05)71529-6. PMID 16373015.
- ^ Anstey AV, Hift RJ (July 2007). "Liver disease in erythropoietic protoporphyria: insights and implications for management". Gut. 56 (7): 1009–1018. doi:10.1136/gut.2006.097576. PMC 1994365. PMID 17360790.
- ^ "Zinc Oxide - Physical UVA+UVB sunscreen/sunblock agent". smartskincare.com. Retrieved 2019-04-02.
- ^ "Sun Protective Clothing". The Skin Cancer Foundation. Retrieved 2022-01-26.
- ^ "Scenesse (afamelanotide)". Union Register of medicinal products. European Commission. Retrieved 8 December 2020.
- ^ "FDA approves first treatment to increase pain-free light exposure in patients with a rare disorder". U.S. Food and Drug Administration (Press release). 8 October 2019. Archived from the original on 9 October 2019.
- ^ Pirlich M, Lochs H, Schmidt HH (December 2001). "Liver cirrhosis in erythropoietic protoporphyria: improvement of liver function with ursodeoxycholic acid". The American Journal of Gastroenterology. 96 (12): 3468–3469. doi:10.1111/j.1572-0241.2001.05363.x. PMID 11774991. S2CID 27973564.
- ^ Paumgartner G, Beuers U (September 2002). "Ursodeoxycholic acid in cholestatic liver disease: mechanisms of action and therapeutic use revisited". Hepatology. 36 (3): 525–531. doi:10.1053/jhep.2002.36088. PMID 12198643. S2CID 28282761.
- ^ Potter C, Tolaymat N, Bobo R, Sharp H, Rank J, Bloomer J (November 1996). "Hematin therapy in children with protoporphyric liver disease". Journal of Pediatric Gastroenterology and Nutrition. 23 (4): 402–407. doi:10.1097/00005176-199611000-00006. PMID 8956175.
- ^ Tung BY, Farrell FJ, McCashland TM, Gish RG, Bacon BR, Keeffe EB, Kowdley KV (September 1999). "Long-term follow-up after liver transplantation in patients with hepatic iron overload". Liver Transplantation and Surgery. 5 (5): 369–374. doi:10.1002/lt.500050503. PMID 10477837.
- ^ McCullough AJ, Barron D, Mullen KD, Petrelli M, Park MC, Mukhtar H, Bickers DR (January 1988). "Fecal protoporphyrin excretion in erythropoietic protoporphyria: effect of cholestyramine and bile acid feeding". Gas Naila troenterology. 94 (1): 177–181. doi:10.1016/0016-5085(88)90627-0. PMID 3335288.
- ^ Gorchein A, Foster GR (March 1999). "Liver failure in protoporphyria: long-term treatment with oral charcoal". Hepatology. 29 (3): 995–996. doi:10.1002/hep.510290314. PMID 10189233.
- ^ Hansson M, Hederstedt L (February 1994). "Purification and characterisation of a water-soluble ferrochelatase from Bacillus subtilis". European Journal of Biochemistry. 220 (1): 201–208. doi:10.1111/j.1432-1033.1994.tb18615.x. PMID 8119288.
- ^ Minder EI, Schneider-Yin X, Steurer J, Bachmann LM (February 2009). "A systematic review of treatment options for dermal photosensitivity in erythropoietic protoporphyria". Cellular and Molecular Biology. 55 (1): 84–97. PMID 19268006.
- ^ Ahmed jan, Marisa (13 December 2023). "Erythropoietic Protoporphyria". porphyrianews.com. BioNews Inc. Retrieved 28 May 2024.
- ^ Ahmed jan, Naila (16 December 2023). "Erythropoietic Protoporphyria". www.ncbi.nlm.nih.gov. StatPearls Publishing LLC. Retrieved 6 Jul 2024.
- ^ Arceci R, Hann IM, Smith OP (2006). Pediatric Hematology. Malden, Mass.: Blackwell Pub. ISBN 978-1-4051-3400-2.[page needed]
- ^ Elder G, Harper P, Badminton M, Sandberg S, Deybach JC (September 2013). "The incidence of inherited porphyrias in Europe". Journal of Inherited Metabolic Disease. 36 (5): 849–857. doi:10.1007/s10545-012-9544-4. PMID 23114748. S2CID 20442163.
- ^ Michaels BD, Del Rosso JQ, Mobini N, Michaels JR (July 2010). "Erythropoietic protoporphyria: a case report and literature review". The Journal of Clinical and Aesthetic Dermatology. 3 (7): 44–48. PMC 2921755. PMID 20725556.
- ^ Wahlin S, Floderus Y, Stål P, Harper P (March 2011). "Erythropoietic protoporphyria in Sweden: demographic, clinical, biochemical and genetic characteristics". Journal of Internal Medicine. 269 (3): 278–288. doi:10.1111/j.1365-2796.2010.02236.x. PMID 20412370.
- ^ Kosenow W, Treibs A (1953). "Lichtüberempfindlichkeit und Porphyrinämie". Zeitschrift für Kinderheilkunde. 73 (1): 82–92. doi:10.1007/BF00438257. PMID 13103364. S2CID 46459771.
- ^ Magnus IA, Jarrett A, Prankerd TA, Rimington C (August 1961). "Erythropoietic protoporphyria. A new porphyria syndrome with solar urticaria due to protoporphyrinaemia". Lancet. 2 (7200): 448–451. doi:10.1016/S0140-6736(61)92427-8. PMID 13765301.
External links
edit- Erythropoietic protoporphyria at NLM Genetics Home Reference