【 摘 要 】

Background

Pemphigus is a rare group of life-threatening mucocutaneous autoimmune blistering diseases. Frequently, oral lesions precede the cutaneous ones. This study aimed to describe clinical and histological features of oral pemphigus lesions in patients aged 18 years and above, attending outpatient’s facility of Khartoum Teaching Hospital - Dermatology Clinic, Sudan. In addition, the study aimed to assess the diagnostic significance of routine histolopathology along with immunohistochemical (IHC) examination of formalin-fixed, paraffin-embedded biopsy specimens in patients with oral pemphigus.

Methods

A cross-sectional hospital-based study was conducted from October 2008 to January 2009. A total of 588 patients with confirmed disease diagnosis completed an oral examination and a personal interview. Clinical evaluations supported with histopathology were the methods of diagnosis. IHC was used to confirm the diagnosis. Location, size, and pain of oral lesions were used to measure the oral disease activity.

Results

Twenty-one patients were diagnosed with pemphigus vulgaris (PV), 19 of them (mean age: 43.0; range: 20–72 yrs) presented with oral manifestations. Pemphigus foliaceus was diagnosed in one patient. In PV, female: male ratio was 1.1:1.0. Buccal mucosa was the most commonly affected site. Exclusive oral lesions were detected in 14.2% (3/21). In patients who experienced both skin and oral lesion during their life time, 50.0% (9/18) had oral mucosa as the initial site of involvement, 33.3% (6/18) had skin as the primary site, and simultaneous involvement of both skin and oral mucosa was reported by 5.5% (1/18). Two patients did not provide information regarding the initial site of involvement. Oral lesion activity score was higher in those who reported to live outside Khartoum state, were outdoor workers, had lower education and belonged to Central and Western tribes compared with their counterparts. Histologically, all tissues except one had suprabasal cleft and acantholytic cells. IHC revealed IgG and C3 intercellularly in the epithelium.

Conclusions

PV was the predominating subtype of pemphigus in this study. The majority of patients with PV presented with oral lesions. Clinical and histological pictures of oral PV are in good agreement with the literature. IHC confirmed all diagnoses of PV.

【 授权许可】

   
2013 Suliman et al.; licensee BioMed Central Ltd.

【 预 览 】

附件列表

Files	Size	Format	View
20150218021012897.pdf	1802KB	PDF	download
Figure 4.	141KB	Image	download
Figure 3.	140KB	Image	download
Figure 2.	249KB	Image	download
Figure 1.	48KB	Image	download

【 图 表 】

【 参考文献 】

• [1]Neville BW: Dermatologic Diseases. In Oral & maxillofacial pathology. 3rd edition. St. Louis: Saunders Elsevier; 2009:765-771.
• [2]Scully C, Paes De Almeida O, Porter SR, Gilkes JJ: Pemphigus vulgaris: the manifestations and long-term management of 55 patients with oral lesions. Br J Dermatol 1999, 140(1):84-89.
• [3]Cirillo N, Cozzani E, Carrozzo M, Grando S: Urban legends: pemphigus vulgaris. Oral Dis 2012, 18(5):442-458.
• [4]Sagi L, Baum S, Agmon-Levin N, Sherer Y, Katz BS, Barzilai O, Ram M, Bizzaro N, SanMarco M, Trau H, et al.: Autoimmune bullous diseases the spectrum of infectious agent antibodies and review of the literature. Autoimmunity reviews 2011, 10(9):527-535.
• [5]Ruocco V, Ruocco E: Pemphigus and environmental factors. Gital Dermatol Venereol 2003, 138:299-309.
• [6]Bastuji-Garin S, Turki H, Mokhtar I, Nouira R, Fazaa B, Jomaa B, Zahaf A, Osman AB, Souissi R, Hemon D, et al.: Possible relation of Tunisian pemphigus with traditional cosmetics: a multicenter case–control study. Am J Epidemiol 2002, 155(3):249-256.
• [7]Valikhani M, Kavusi S, Chams-Davatchi C, Daneshpazhooh M, Barzegari M, Ghiasi M, Abedini R: Pemphigus and associated environmental factors: a case–control study. Clin Exp Dermatol 2007, 32(3):256-260.
• [8]Sullivan TP, Elgart GW, Kirsner RS: Pemphigus and smoking. Int J Dermatol 2002, 41(8):528-530.
• [9]Nousari HC, Anhalt GJ: Pemphigus and bullous pemphigoid. Lancet 1999, 354(9179):667-672.
• [10]Weedon D, Strutton G, Rubin AI, Weedon D: The vesiculobullous reaction pattern. In Weedon’s skin pathology. 3rd edition. [Edinburgh]: Churchill Livingstone/Elsevier; 2010:151-152.
• [11]Tsankov N, Vassileva S, Kamarashev J, Kazandjieva J, Kuzeva V: Epidemiology of pemphigus in Sofia, Bulgaria. A 16-year retrospective study (1980–1995). Int J Dermatol 2000, 39(2):104-108.
• [12]Bozdag K, Bilgin I: Epidemiology of pemphigus in the western region of Turkey: retrospective analysis of 87 patients. Cutan Ocul Toxicol 2012, 31(4):280-285.
• [13]Bastuji-Garin S, Souissi R, Blum L, Turki H, Nouira R, Jomaa B, Zahaf A, Ben Osman A, Mokhtar I, Fazaa B, et al.: Comparative epidemiology of pemphigus in Tunisia and France. Incidence of foliaceus pemphigus in young Tunisian women. Ann Dermatol Venereol 1996, 123(5):337-342.
• [14]Alsaleh QA, Nanda A, Al-Baghli NM, Dvorak R: Pemphigus in Kuwait. Int J Dermatol 1999, 38(5):351-356.
• [15]Seo PG, Choi WW, Chung JH: Pemphigus in Korea: clinical manifestations and treatment protocol. J Dermatol 2003, 30(11):782-788.
• [16]Scully C, Challacombe SJ: Pemphigus vulgaris: update on etiopathogenesis, oral manifestations, and management. Crit Rev Oral Biol Med 2002, 13(5):397-408.
• [17]Scully C, Felix DH: Oral medicine–update for the dental practitioner. Mouth ulcers of more serious connotation. Br Dent J 2005, 199(6):339-343.
• [18]Hietanen J, Salo OP: Pemphigus: an epidemiological study of patients treated in Finnish hospitals between 1969 and 1978. Acta Derm Venereol 1982, 62(6):491-496.
• [19]Simon DG, Krutchkoff D, Kaslow RA, Zarbo R: Pemphigus in Hartford County, Connecticut, from 1972 to 1977. Arch Dermatol 1980, 116(9):1035-1037.
• [20]Pisanti S, Sharav Y, Kaufman E, Posner LN: Pemphigus vulgaris: incidence in Jews of different ethnic groups, according to age, sex, and initial lesion. Oral Surg Oral Med Oral Pathol 1974, 38(3):382-387.
• [21]Uzun S, Durdu M, Akman A, Gunasti S, Uslular C, Memisoglu HR, Alpsoy E: Pemphigus in the Mediterranean region of Turkey: a study of 148 cases. Int J Dermatol 2006, 45(5):523-528.
• [22]Mahe A, Flageul B, Cisse I, Keita S, Bobin P: Pemphigus in Mali: a study of 30 cases. Br J Dermatol 1996, 134(1):114-119.
• [23]Shafi M, Khatri ML, Mashina M, Ben-Ghazeil M: Pemphigus: a clinical study of 109 cases from Tripoli, Libya. Indian J Dermatol Venereol Leprol 1994, 60(3):140-143.
• [24]Aboobaker J, Morar N, Ramdial PK, Hammond MG: Pemphigus in South Africa. Int J Dermatol 2001, 40(2):115-119.
• [25]Moy R, Jordon RE: Immunopathology in pemphigus. Clin Dermatol 1983, 1(2):72-81.
• [26]Zhang X, Hyjek E, Soltani K, Petronic-Rosic V, Shea CR: Immunohistochemistry for Immunoglobulin G4 on Paraffin Sections for the Diagnosis of Pemphigus. Arch Pathol Lab Med 2012, 136(11):1402-1407.
• [27]Kordofani YM, Shah IM, El-Agraa B, Shalayel MH: Pemphigus in Khartoum Skin Teaching Hospital. Sudan Medical Monitor 2008, 3(2):58-60.
• [28]Suliman NM, Astrom AN, Ali RW, Salman H, Johannessen AC: Oral mucosal lesions in skin diseased patients attending a dermatologic clinic: a cross-sectional study in Sudan. BMC Oral Health 2011, 11(1):24. BioMed Central Full Text
• [29]Annual Health Statistical Report-2007. http://www.fmoh.gov.sd/indexAr.php?id=16 webcite
• [30]Lwanga SK, Lemeshow S: Sample size determination in health studies: a practical manual. Geneva: World Health Organization; 1991.
• [31]Kramer IR, Pindborg JJ, Bezroukov V, Infirri JS: Guide to epidemiology and diagnosis of oral mucosal diseases and conditions. World Health Organization. Community Dent Oral Epidemiol 1980, 8(1):1-26.
• [32]Axell T, Pindborg JJ, Smith CJ, van der Waal I: Oral white lesions with special reference to precancerous and tobacco- related lesions: conclusions of an international symposium held in Uppsala, Sweden, May 18–21 1994. International Collaborative Group on Oral White Lesions. J Oral Pathol Med 1996, 25(2):49-54.
• [33]Axell T: A prevalence study of oral mucosal lesions in an adult Swedish population. Odontol Revy Suppl 1976, 36:1-103.
• [34]Saraswat A, Bhushan K, India C: A new grading system for oral pemphigus. Int J Dermatol 2003, 42(5):413-414.
• [35]Agarwal M, Walia R, Kochhar AM, Chander R: Pemphigus Area and Activity Score (PAAS)–a novel clinical scoring method for monitoring of pemphigus vulgaris patients. Int J Dermatol 1998, 37(2):158-160.
• [36]Weedon D, Strutton G, Rubin AI: The vesiculobullous reaction pattern. In Weedon’s Skin Pathology. 3rd edition. [Edinburgh]: Churchill Livingstone/Elsevier; 2010:135-138.
• [37]Brenner S, Tur E, Shapiro J, Ruocco V, D’Avino M, Ruocco E, Tsankov N, Vassileva S, Drenovska K, Brezoev P, et al.: Pemphigus vulgaris: environmental factors. Occupational, behavioral, medical, and qualitative food frequency questionnaire. Int J Dermatol 2001, 40(9):562-569.
• [38]Ramirez-Amador VA, Esquivel-Pedraza L, Orozco-Topete R: Frequency of oral conditions in a dermatology clinic. Int J Dermatol 2000, 39(7):501-505.
• [39]Esmaili N, Chams-Davatchi C, Valikhani M, Daneshpazhooh M, Balighi K, Hallaji Z, Barzegari M, Akhyani M, Ghodsi ZS, Mrotazavi H, et al.: Pemphigus vulgaris in Iran: a clinical study of 140 cases. Int J Dermatol 2007, 46(11):1166-1170.
• [40]Ishii N, Maeyama Y, Karashima T, Nakama T, Kusuhara M, Yasumoto S, Hashimoto T: A clinical study of patients with pemphigus vulgaris and pemphigus foliaceous: an 11-year retrospective study (1996–2006). Clin Exp Dermatol 2008, 33(5):641-643.
• [41]Tallab T, Joharji H, Bahamdan K, Karkashan E, Mourad M, Ibrahim K: The incidence of pemphigus in the southern region of Saudi Arabia. Int J Dermatol 2001, 40(9):570-572.
• [42]Camacho-Alonso F, Lopez-Jornet P, Bermejo-Fenoll A: Pemphigus vulgaris. A presentation of 14 cases and review of the literature. Med Oral Patol Oral Cir Bucal 2005, 10(4):282-288.
• [43]Budimir J, Mihic LL, Situm M, Bulat V, Persic S, Tomljanovic-Veselski M: Oral lesions in patients with pemphigus vulgaris and bullous pemphigoid. Acta Clin Croat 2008, 47(1):13-18.
• [44]Michailidou EZ, Belazi MA, Markopoulos AK, Tsatsos MI, Mourellou ON, Antoniades DZ: Epidemiologic survey of pemphigus vulgaris with oral manifestations in northern Greece: retrospective study of 129 patients. Int J Dermatol 2007, 46(4):356-361.
• [45]Nanda A, Dvorak R, Al-Saeed K, Al-Sabah H, Alsaleh QA: Spectrum of autoimmune bullous diseases in Kuwait. Int J Dermatol 2004, 43(12):876-881.
• [46]Zaraa I, Kerkeni N, Ishak F, Zribi H, El Euch D, Mokni M, Osman AB: Spectrum of autoimmune blistering dermatoses in Tunisia: an 11-year study and a review of the literature. Int J Dermatol 2011, 50(8):939-944.
• [47]Alcaide-Martin AJ, Gallardo-Perez MA, Castillo-Munoz R, Mendiola Fernandez MV, Herrera-Ceballos E: Epidemiologic study of 20 cases of pemphigus at Hospital Clinico Universitario Virgen de la Victoria de Malaga, Spain. Actas Dermosifiliogr 2010, 101(6):524-533.
• [48]Chighizola C, Meroni PL: The role of environmental estrogens and autoimmunity. Autoimmunity reviews 2012, 11(6–7):A493-A501.
• [49]Whitacre CC: Sex differences in autoimmune disease. Nat Immunol 2001, 2(9):777-780.
• [50]Kulthanan K, Chularojanamontri L, Tuchinda P, Sirikudta W, Pinkaew S: Clinical features and course of pemphigus in Thai patients. Asian Pac J Allergy Immunol 2011, 29(2):161-168.
• [51]Baican A, Baican C, Chiriac G, Chiriac MT, Macovei V, Zillikens D, Ciuce D, Sitaru C: Pemphigus vulgaris is the most common autoimmune bullous disease in Northwestern Romania. Int J Dermatol 2010, 49(7):768-774.
• [52]Bertram F, Brocker EB, Zillikens D, Schmidt E: Prospective analysis of the incidence of autoimmune bullous disorders in Lower Franconia, Germany. J Dtsch Dermatol Ges 2009, 7(5):434-440.
• [53]Davenport S, Chen SY, Miller AS: Pemphigus vulgaris: clinicopathologic review of 33 cases in the oral cavity. Int J Periodontics Restorative Dent 2001, 21(1):85-90.
• [54]Salmanpour R, Shahkar H, Namazi MR, Rahman-Shenas MR: Epidemiology of pemphigus in south-western Iran: a 10-year retrospective study (1991–2000). Int J Dermatol 2006, 45(2):103-105.
• [55]Pobutsky A, Bradbury E, Wong Tomiyasu D: Chronic Disease Disparities Report 2011: Social Determinants. Honolulu: Hawaii State Department of Health, Chronic Disease Management and Control Branch; 2011.
• [56]Ruocco V, Pisani M: Induced pemphigus. Arch Dermatol Res 1982, 274(1–2):123-140.
• [57]Wohl Y, Brenner S: Pemphigus in Israel–an epidemiologic analysis of cases in search of risk factors. Isr Med Assoc J 2003, 5(6):410-412.
• [58]Hashimoto T, Ogawa MM, Konohana A, Nishikawa T: Detection of pemphigus vulgaris and pemphigus foliaceus antigens by immunoblot analysis using different antigen sources. J Invest Dermatol 1990, 94(3):327-331.
• [59]Kyriakis KP, Vareltzidis AG, Tosca AD: Environmental factors influencing the biologic behavior of patterns of pemphigus vulgaris: epidemiologic approach. Int J Dermatol 1995, 34(3):181-185.
• [60]Ali H, Ahmed Zakieldeen S, Sulaiman S: Climate Change and Health in Sudan. Capacity Strengthening in the least developed countries (LDCS) for adaptation to climate change (CLACC) International Institute for Enviroment and Development 2008.
• [61]Health System Profile Sudan. http://gis.emro.who.int/healthsystemobservatory/main/Forms/CountryInfo.aspx?Country=SUDAN webcite
• [62]Robati RM, Saeedi M, Alirezayee P: Pemphigus vulgaris and season: are they really related or not? J Eur Acad Dermatol Venereol 2011, 25(10):1235-1236.
• [63]Bastuji-Garin S, Souissi R, Blum L, Turki H, Nouira R, Jomaa B, Zahaf A, Ben Osman A, Mokhtar I, Fazaa B, et al.: Comparative epidemiology of pemphigus in Tunisia and France: unusual incidence of pemphigus foliaceus in young Tunisian women. J Invest Dermatol 1995, 104(2):302-305.
• [64]Meyer N, Misery L: Geoepidemiologic considerations of auto-immune pemphigus. Autoimmun Rev 2010, 9(5):A379-A382.
• [65]Fridkis-Hareli M: Distribution Of Jewish And Non-Jewish Haplotypes Among Pemphigus Vulgaris Patients Worldwide. Internet J Dermatol 2007, 6(1): .
• [66]Ruocco V, Peluso G, Pisani M: Pemphigus vulgaris in only one of two monozygotic twins. J Am Acad Dermatol 1985, 12(3):587-589.
• [67]Yamamoto T, Ikeda K, Sasaoka S, Yamasaki O, Fujimoto W, Aoyama Y, Iwatsuki K: Human leukocyte antigen genotypes and antibody profiles associated with familial pemphigus in Japanese. J Dermatol 2011, 38(7):711-716.
• [68]Danaei G, Ding EL, Mozaffarian D, Taylor B, Rehm J, Murray CJ, Ezzati M: The preventable causes of death in the United States: comparative risk assessment of dietary, lifestyle, and metabolic risk factors. PLoS Med 2009, 6(4):e1000058.
• [69]Mehta JN, Martin AG: A case of pemphigus vulgaris improved by cigarette smoking. Arch Dermatol 2000, 136(1):15-17.
• [70]Axell T, Henricsson V: Association between recurrent aphthous ulcers and tobacco habits. Scand J Dent Res 1985, 93(3):239-242.
• [71]Pullan RD, Rhodes J, Ganesh S, Mani V, Morris JS, Williams GT, Newcombe RG, Russell MA, Feyerabend C, Thomas GA, et al.: Transdermal nicotine for active ulcerative colitis. N Engl J Med 1994, 330(12):811-815.
• [72]Grando SA, Horton RM, Pereira EF, Diethelm-Okita BM, George PM, Albuquerque EX, Conti-Fine BM: A nicotinic acetylcholine receptor regulating cell adhesion and motility is expressed in human keratinocytes. J Invest Dermatol 1995, 105(6):774-781.
• [73]Zia S, Ndoye A, Lee TX, Webber RJ, Grando SA: Receptor-mediated inhibition of keratinocyte migration by nicotine involves modulations of calcium influx and intracellular concentration. J Pharmacol Exp Ther 2000, 293(3):973-981.
• [74]Metelitsa AI, Lauzon GJ: Tobacco and the skin. Clin Dermatol 2010, 28(4):384-390.
• [75]Sorensen LT, Karlsmark T, Gottrup F: Abstinence from smoking reduces incisional wound infection: a randomized controlled trial. Ann Surg 2003, 238(1):1-5.
• [76]Meliska CJ, Stunkard ME, Gilbert DG, Jensen RA, Martinko JM: Immune function in cigarette smokers who quit smoking for 31 days. J Allergy Clin Immunol 1995, 95(4):901-910.
• [77]Heymann AD, Chodick G, Kramer E, Green M, Shalev V: Pemphigus variant associated with penicillin use: a case-cohort study of 363 patients from Israel. Arch Dermatol 2007, 143(6):704-707.
• [78]Lee A, Thomson J: Drug-induced skin reactions. 2006.
• [79]Shamim T, Varghese VI, Shameena PM, Sudha S: Pemphigus vulgaris in oral cavity: clinical analysis of 71 cases. Med Oral Patol Oral Cir Bucal 2008, 13(10):E622-E626.
• [80]Chams-Davatchi C, Valikhani M, Daneshpazhooh M, Esmaili N, Balighi K, Hallaji Z, Barzegari M, Akhiani M, Ghodsi Z, Mortazavi H, et al.: Pemphigus: analysis of 1209 cases. Int J Dermatol 2005, 44(6):470-476.
• [81]Camisa C, Rindler JM: Diseases of the oral mucous membranes. Curr Probl Dermatol 1996, 8(2):43-96.
• [82]Arisawa EA, Almeida JD, Carvalho YR, Cabral LA: Clinicopathological analysis of oral mucous autoimmune disease: a 27-year study. Med Oral Patol Oral Cir Bucal 2008, 13(2):E94-E97.
• [83]Scully C, Mignogna M: Oral mucosal disease: pemphigus. Br J Oral Maxillofac Surg 2008, 46(4):272-277.
• [84]Robinson JC, Lozada-Nur F, Frieden I: Oral pemphigus vulgaris: a review of the literature and a report on the management of 12 cases. Oral Surg Oral Med Oral Pathol Oral Radiol Endod 1997, 84(4):349-355.
• [85]Iamaroon A, Boonyawong P, Klanrit P, Prasongtunskul S, Thongprasom K: Characterization of oral pemphigus vulgaris in Thai patients. J Oral Sci 2006, 48(1):43-46.
• [86]Mignogna MD, Lo Muzio L, Bucci E: Clinical features of gingival pemphigus vulgaris. J Clin Periodontol 2001, 28(5):489-493.
• [87]Shklar G, Cataldo E: Histopathology and cytology of oral lesions of pemphigus. Arch Dermatol 1970, 101(6):635-641.
• [88]Nishifuji K, Amagai M, Kuwana M, Iwasaki T, Nishikawa T: Detection of antigen-specific B cells in patients with pemphigus vulgaris by enzyme-linked immunospot assay: requirement of T cell collaboration for autoantibody production. J Invest Dermatol 2000, 114(1):88-94.
• [89]Hertl M, Riechers R: Analysis of the T cells that are potentially involved in autoantibody production in pemphigus vulgaris. J Dermatol 1999, 26(11):748-752.
• [90]Coscia-Porrazzi L, Maiello FM, Ruocco V, Pisani M: Cytodiagnosis of oral pemphigus vulgaris. Acta Cytol 1985, 29(5):746-749.
• [91]Shamim T, Varghese VI, Shameena PM, Sudha S: Candida smear-an adjunct for diagnosis of acantholytic cells in oral pemphigus vulgaris. J Coll Physicians Surg Pak 2008, 18(6):392.
• [92]Rinaggio J, Crossland DM, Zeid MY: A determination of the range of oral conditions submitted for microscopic and direct immunofluorescence analysis. J Periodontol 2007, 78(10):1904-1910.
• [93]Sirois D, Leigh JE, Sollecito TP: Oral pemphigus vulgaris preceding cutaneous lesions: recognition and diagnosis. J Am Dent Assoc 2000, 131(8):1156-1160.
• [94]Awadelkarim KD, Mohamedani AA, Barberis M: Role of pathology in sub-Saharan Africa: an example from Sudan. Pathol Lab Med Int 2010, 2:49-57.
• [95]Mera SL, Young EW, Bradfield JW: Direct immunofluorescence of skin using formalin-fixed paraffin-embedded sections. J Clin Pathol 1980, 33(4):365-369.
• [96]Handlers JP, Melrose RJ, Abrams AM, Taylor CR: Immunoperoxidase technique in diagnosis of oral pemphigus vulgaris: an alternative method to immunofluorescence. Oral Surg Oral Med Oral Pathol 1982, 54(2):207-212.