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Objectives: We sought to evaluate the frequency and clinical characteristics of pruritic dermatoses in pregnancy and to assess a rationalized classification. Methods: Data of 505 pregnant patients seen at two university- based dermatologic hospitals (1994- 2004) were retrospectively studied. Results: Diagnoses included eczema in pregnancy (49.7% ), polymorphic eruption of pregnancy (PEP) (21.6% ), pemphigoid gestationis (PG) (4.2% ), intrahepatic cholestasis of pregnancy (ICP) (3% ), prurigo of pregnancy (0.8% ), pruritic folliculitis of pregnancy (0.2% ), and miscellaneous dermatoses (20.6% ). Eczema in pregnancy, prurigo of pregnancy, and pruritic folliculitis of pregnancy showed considerable overlap and were summarized as atopic eruption of pregnancy (AEP). While PEP, PG, and ICP presented in late pregnancy, AEP started significantly earlier. Primi gravidae and multiple gestations were characteristic for PEP, abdominal involvement for PEP and PG, and a history of affected pregnancies for ICP. Limitations: This was a retrospective study. Conclusion: We propose classifying the dermatoses of pregnancy as PG, PEP, AEP, and ICP. Stereotypic immunofluorescence and laboratory findings are diagnostic of PG and ICP, whereas distinct clinical characteristics facilitate discrimination between PEP andAEP.
Objectives: We sought to evaluate the frequency and clinical characteristics of pruritic dermatoses in pregnancy and to assess a rationalized classification. Methods: Data of 505 pregnant patients seen at two university-based dermatologic hospitals (1994- 2004) were retrospectively studied. Results: Diagnoses Included were eczema in pregnancy (49.7%), polymorphic eruption of pregnancy (PEP) (21.6%), pemphigoid gestationis (PG) (4.2%), intrahepatic cholestasis of pregnancy , prurigo of pregnancy, and pruritic folliculitis of pregnancy showed considerable overlap and were summarized as atopic eruption of pregnancy (AEP). While PEP, PG , and ICP presented in late pregnancy, AEP started significantly earlier. Primi gravidae and multiple gestations were characteristic for PEP, abdominal involvement for PEP and PG, and a history of affected pregnancie s for ICP. Limitations: This was a retrospective study. Conclusion: We propose classifying the dermatoses of pregnancy as PG, PEP, AEP, and ICP. Stereotypic immunofluorescence and laboratory findings are diagnostic of PG and ICP, PEP andAEP.