Plantar keratoderma: a manifestation of tyrosinemia type II (Richner-Hanhart Syndrome)
2005; King Faisal Specialist Hospital and Research Centre; Volume: 25; Issue: 5 Linguagem: Inglês
10.5144/0256-4947.2005.422
ISSN0975-4466
AutoresJihad T Al-Ratrout, Mohammed Al-Muzian, Mona Al-Nazer, Naseem A. Ansari,
Tópico(s)Biomedical Research and Pathophysiology
ResumoCase ReportPlantar keratoderma: a manifestation of tyrosinemia type II (Richner-Hanhart Syndrome) Jihad T. Al-Ratrout, Mohammed Al-Muzian, Mona Al-Nazer, and Naseem A. Ansari Jihad T. Al-Ratrout Qatif Central Hospital, Department of Dermatology, Qatif, Saudi Arabia , Mohammed Al-Muzian Qatif Central Hospital, Department of Dermatology, Qatif, Saudi Arabia , Mona Al-Nazer Qatif Central Hospital, Department of Pathology, Qatif, Saudi Arabia , and Naseem A. Ansari Qatif Central Hospital, Arabian Gulf University, College of Medicine & Medical Sciences, Department of Pathology, Bahrain Published Online:6 Oct 2005https://doi.org/10.5144/0256-4947.2005.422SectionsPDF ToolsAdd to favoritesDownload citationTrack citations ShareShare onFacebookTwitterLinked InRedditEmail AboutIntroductionTyrosinemia type II (Richner-Hanhart syndrome) is a distinctive clinical syndrome involving the eye, skin and central nervous system. It is caused by a deficiency of hepatic tyrosine amino-transferase, resulting in elevated plasma tyrosine concentrations and elevated levels of abnormal metabolites of tyrosine in the urine. We describe the case of a middle-aged Saudi male with painful plantar keratoderma since the age of 16 years. He had certain eye signs and moderate mental retardation. To the authors' knowledge the patient described represents only the eighth case of tyrosinemia type II from Saudi Arabia. Furthermore, there have been fewer than 100 such cases reported worldwide.CaseA 38-year-old man was seen in the dermatology clinic at Qatif Central Hospital, Qatif, Saudi Arabia, for evaluation of painful keratinous plantar lesions associated with increased sweating. The cutaneous lesion first manifested at the age of 16 and were never associated with ocular symptoms such as photophobia, redness or tearing. The lesions resolved in the winter and reappeared with increased severity in the summer. There was no exacerbation of the lesions with certain foods. The lesions usually started as bullae and erosions, progressing to crusted painful keratoderma. The degree of pain was so severe that he resorted to walking on tiptoe.The patient was born to a consanguineous marriage, but there was no other similar history in the family. Treatment with keratolytic ointment and a diet free of fish, chicken and meat—to which he did not strictly adhere—minimally improved his condition. General examination revealed mild mental retardation with an IQ of 68. Skin examination showed symmetrical patchy, hyperkeratotic and foul smelling yellow plaques on the weight-bearing areas (Figure 1). Light pressure over his calluses elicited intense pain. His hands were clear of lesions apart from a single small yellowish hyperkeratotic plaque on the left palm at the metacarpophalangeal joint (Figure 2). This was the most recently developed lesion.Figure 1 Symmetrical patchy, hyperkeratotic yellow plaques on the weight-bearing areas of both feet. The lesions were exquisitely painful such that the patient resorted to walking on tiptoe.Download FigureFigure 2 A single small yellowish hyperkeratotic plaque on the left palm at the fourth metacarpophalangeal joint (arrow).Download FigureOphthalmological examination found trachoma scarring with mild post-trachoma degeneration. The cornea showed a mild diffuse haze with superior and inferior accentuation. The left cornea showed an old round superficial stromal opacity. There was no corneal neovascularisation. Incidentally, despite a variety of ocular signs at examination, at no time did the patient complain of eye symptoms.Laboratory studies found serum tyrosine of 1430 μmol/L (normal 51-91 μmol/L) and excessive excretion of urinary tyrosine and its metabolites, p-hydroxyphenyl-pyruvic acid (PHPPA), p-hydroxyphenyl lactic acid (PHPLA), and p-hydroxyphenyl acetic acid (PHPAA). Results of a complete blood cell count with differential cell count, urinalysis, blood chemistry panel and liver function tests were within normal limits. A skin biopsy specimen of the plaque from the callosity of the foot showed hyperkeratosis, hypergranulosis and acanthosis. There were no other specific features. A diagnosis of tyrosinemia type II was made based on the high serum and urinary tyrosine levels and the clinical features.DiscussionTyrosinemia type II (also known as oculocutaneous tyrosinemia and Richner-Hanhart syndrome) is a rare distinctive disorder with autosomal recessive inheritance, characterized by skin and eye lesions, and occasionally mental retardation.1 Approximately half of the hitherto reported cases are of Italian descent; fewer than ten cases have been reported from the Arabian peninsula.2-4 It is distinct from the more severe hepatorenal tyrosinemia (tyrosinemia type I) and from benign transient tyrosinemia of the new-born.Richner-Hanhart syndrome was first described by Richner, a Swiss ophthalmologist, in 1938,5 and later by Hanhart, a Swiss geneticist, in 1947.6 However, it was not until the early 1970s that the association with tyrosine metabolism was made.1,7,8 The disease is caused by a deficiency of the hepatic enzyme tyrosine aminotransferase (TAT), which leads to increased levels of tyrosine in the blood and urine. The TAT gene is located on the long arm of chromosome 16, the exact locus being 16q22-24.9,10 The TAT gene has been cloned, and up to twelve different mutations have been identified.11,12The typical oculocutaneous neurologic triad is not always present. Tyrosinemia type II with features confined to the skin has been reported previously.13,14 The typical dermatologic findings are painful, well-demarcated hyperkeratosis on the palms and soles, although the palms can be unaffected.15,16 On the palms the distribution usually involves the fingertips, and the thenar and hypothenar eminences, while the lesions on the soles are on the weight-bearing areas. It is uncertain how high the level of tyrosine in the serum must be to induce the clinical manifestations, and why it should be confined to the palmoplanter locations, especially weight-bearing areas. The lesions, which may begin as bullae and erosions that progress to crusted, hyperkeratotic plaques, are often associated with hyperhydrosis.17 Age at onset of skin lesions can range from the first week of life to the second decade.13,15,16,18,19 Ocular manifestations can develop as early as the first day of life and alternatively may present for the first time as late as the fourth decade. Early signs are photophobia, pain, tearing and redness, while late signs include corneal clouding and central or paracentral opacities, superficial or deep dendritic ulceration, corneal neovascularization, and corneal scars.16,18,20,21 Mental retardation of varying degrees is not a constant feature.16,19,20,22The light microscopic features of the cutaneous lesions are not specific. The usual findings are hyperkeratosis, acanthosis, parakeratosis, a faint parakeratotic column in the acrosyringium and multinucleated keratinocytes.13 Ultrastructural examination of the skin usually shows increases in tonofibrils and keratohyaline, aggregation of the keratin intermediate filaments, multinucleated keratinocytes, and minute tyrosine crystals in keratinocytes and Merkel cells. Deposition of tyrosine crystals in the epidermal keratinocytes (and corneal epithelium) is the triggering event in the pathogenesis of skin and eye lesions. In the skin, tyrosine in the keratinocyte cytoplasm leads to crystal formation with subsequent cell injury and rupture followed by fusion of two or more keratinocytes. Tyrosine induces excessive noncovalent cross-linking of keratin, causing abnormal tonofilament aggregation.Management of tyrosinemia type II is largely by dietary restriction to food low in tyrosine and phenylalanine, which reverses ocular and cutaneous abnormalities. Early diagnosis and immediate initiation of diet therapy may prevent the occurrence of other symptoms.17 Mental retardation can be avoided if treatment is started in the early stage of the disease. 24,25 Systemic retinoid may inhibit disulfide and nondisulfide cross-linking of keratin and decrease tonofilaments. A combined therapy with diet and etretinate would be advisable for those patients who do not follow a strict diet. For those who have no ocular or central nervous system abnormalities, retinoids have been reported to control the skin lesion.16,18,24ARTICLE REFERENCES:1. Goldsmith LA, Kang E, Bienfang DC, et al. "Tyrosinemia with plantar and palmar keratosis and keratitis" . J Pediatr. 1973; 83:798-805. Google Scholar2. Rehak A, Selim MM, Yadav J. "Richner-Hanhart syndrome (tyrosinaemia-II). Report of four cases without ocular involvement" . Br J Dermatol. 1981; 104:469-475. Google Scholar3. Al-Hemidan AI, Al-Hazzaa SA. "Richner-Hanhart syndrome (tyrosinemia type II). Case report and literature review" . Ophthalmic Genet. 1995; 16:21-26. Google Scholar4. Al-Essa M, Rashed M, Ozand T. "Tyrosinemia type II: Report of the first four cases in Saudi Arabia" . Ann Saudi Med. 1998; 18:466-468. Google Scholar5. Richner H. "Hornhautaffektion bei keratoderma palmar et plantare hereditariu" . Klin Monastsbl bigenheilkd. 1938; 100:580-588. Google Scholar6. Hanhart E. "Neue sonderformen von keratosis palmoplantaris, u.a. eine regelmabig-dominant misystmatisierten lipomen, ferner 2 eihfach -rezessive mit schwachsinn und Z.T. Horautver and erungen des auges (ektodermal syndrom)" . Dermatologica. 1947; 94:286-308. Google Scholar7. Buist NRM, Kennaway NG, Burns RP. "Eye and skin lesons in tyrosinemia" . Lancet. 1973; 1:620-621. Google Scholar8. Zaleski WA, Hill A, Kushniruk W, et al. "Skin lesions in tyrosinosis: response to dietary treatment" . Br J Dermatol. 1973; 88:335-840. Google Scholar9. Natt E, Kao FT, Rettenmeier R, et al. "Assignment of the human tyrosine aminotransferase gene to chromosome 16" . Hum Genet. 1986; 72:225-228. Google Scholar10. Barton DE, Yang-Feng TL, Francke U. "The human tyrosine aminotransferase gene mapped to the long arm of chromosome 16 (region 16q22-24) by somatic cell hybrid analysis and in situ hybridization" . Hum Genet. 1986; 72(3):221-224. Google Scholar11. Natt E, Kida K, Odievre M, et al. "Point mutations in the tyrosine aminotransferase gene in tyrosinemia type II" . Proc Natl Acad Sci. 1992; 89:9297-9301. Google Scholar12. Huhn R, Stoermer H, Klingele B, et al. "Novel and recurrent tyrosine aminotransferase gene mutations in tyrosinemia type II" . Hum Genet. 1998; 102(3):305-313. Google Scholar13. Shimizu N, Ito M, Ito K, et al. "Richner -Hanhart's syndrome. Electron microscopic study of the skin lesion" . Arch Dermatol. 1990; 126:1342-1346. Google Scholar14. Lestringant GG. "Tyrosinemia type II with incomplete Richner- Hanhart's syndrome" . Int J Dermatol. 1988; 27:43-44. Google Scholar15. Acosta FJ. "Painful plantar callouses and mental retardation" . Arch Dermatol. 1994; 130:507. Google Scholar16. Rabinowitz LG, Williams LR, Anderson CE, et al. "Painful keratoderma and photophobia: hallmarks of tyrosinemia type II" . J Pediatr. 1995; 126:266-269. Google Scholar17. Fraser NG, MacDonald J, Griffiths WA, et al. "Tyrosinemia type II (Richner-Hanhart syndrome): report of two cases treated with etretinate" . Clin Exp Dermatol. 1987; 12:440-443. Google Scholar18. Tallab TM. "Richner-Hanhart syndrome: importance of early diagnosis and early intervention" . J Am Acad Dermatol. 1996; 35:857-9. Google Scholar19. Colditz PB, Yu JS, Billson FA, et al. "Tyrosinemia II" . Med J Aust. 1984; 141:244-245. Google Scholar20. Balato N, Cusano F, Lembo G, et al. "Tyrosinemia type II in two cases previously reported as Richner-Hanhart syndrome" . Dermatologica. 1986; 173:66-74. Google Scholar21. Goldsmith LA, Reed J. "Tyrosine-induced eye and skin lesions. A treatable genetic disease" . JAMA. 1976; 236:382-384. Google Scholar22. Danks DM, Callan NJ. "Palmoplantar keratoderma with normal intelligence in tyrosinaemia II" . Australas J Dermatol. 1988; 29:107-109. Google Scholar23. Heidemann DG, Dunn SP, Bawle EV, et al. "Early diagnosis of tyrosinemia type II" . Am J Ophthalmol. 1989; 107:559-560. Google Scholar24. Farage IT. "Dietetic therapy of Richnar-Hanhart syndrome" . J R Soc Med. 1993; 86:495. Google Scholar Previous article Next article FiguresReferencesRelatedDetails Volume 25, Issue 5September-October 2005 Metrics History Accepted1 June 2004Published online6 October 2005 AcknowledgementsWe gratefully acknowledge the keen assistance of Dr. Randa Al-Ratrout who diligently extracted relevant clinical data from the case files.InformationCopyright © 2005, Annals of Saudi MedicineThis work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License.PDF download
Referência(s)