136 results on '"Anna Sysa-Jędrzejowska"'
Search Results
2. Systemic sclerosis – diagnostic and therapeutic recommendations of the Polish Dermatological Society. Part 2: treatment
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Dorota Krasowska, Lidia Rudnicka, Aleksandra Dańczak-Pazdrowska, Grażyna Chodorowska, Anna Woźniacka, Anna Lis-Święty, Joanna Czuwara, Joanna Maj, Sławomir Majewski, Anna Sysa-Jędrzejowska, and Anna Wojas-Pelc
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methotrexate ,alprostadil ,sildenafil ,mycophenolate mofetil ,cyclophosphamide ,scleroderma ,guidelines ,Medicine ,Dermatology ,RL1-803 - Abstract
Systemic sclerosis is an immune-mediated disease characterized by a chronic progressive course. The complex and diverse clinical features seen in patients require case-by-case approach and cooperation of multiple specialists both at the stage of diagnosis and treatment. Critical factors in systemic sclerosis include early diagnosis, assessment of internal organ involvement, identification of patients at potential risk of organ complications, assessment of disease dynamics and activity, and implementation of optimal therapy. Treatment decisions should be made individually for each patient after careful consideration of such aspects as the severity of skin lesions, duration and activity of the disease, manifestations and possible internal organ involvement. On account of potential organ dysfunctions, patients require a multidisciplinary therapeutic approach and coordinated treatment by experienced specialists or in specialist medical centres. Part 2 presents current guidelines for the treatment of systemic sclerosis.
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- 2017
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3. Systemic sclerosis – diagnostic and therapeutic recommendations of the Polish Dermatological Society. Part 1: diagnosis and monitoring
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Dorota Krasowska, Lidia Rudnicka, Aleksandra Dańczak-Pazdrowska, Grażyna Chodorowska, Anna Woźniacka, Anna Lis-Święty, Joanna Czuwara, Joanna Maj, Sławomir Majewski, Anna Sysa-Jędrzejowska, and Anna Wojas-Pelc
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systemic sclerosis ,guidelines ,diagnostics ,monitoring ,Medicine ,Dermatology ,RL1-803 - Abstract
Systemic sclerosis is an immune-mediated disease characterized by a chronic and progressive course. It often leads to multiorgan failure and patient disability, and contributes to significant reduction in the quality of life. Systemic sclerosis affects the skin, subcutaneous tissue, muscles, osteoarticular system and internal organs. The complexity and diversity of clinical presentations require an individual approach and multidisciplinary collaboration both at the stage of diagnosis and treatment. Critical factors in systemic sclerosis include early diagnosis, assessment of internal organ involvement, identification of patients at potential risk of organ complications, assessment of disease dynamics and activity, and implementation of optimal therapy. Part 1 presents current recommendations for the diagnostics and monitoring of patients with systemic sclerosis. Attention is given to classification criteria, clinical forms of systemic sclerosis, assessment of skin thickness and systemic sclerosis microangiopathy, significance of antinuclear antibodies, diagnosis of interstitial lung disease and pulmonary arterial hypertension, renal crisis and cardiac abnormalities, and evaluation of the gastrointestinal tract and osteoarticular and muscular systems.
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- 2017
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4. Vitiligo and autoimmune diseases
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Magdalena Kutwin, Anna Sysa-Jędrzejowska, and Anna Woźniacka
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autoimmune diseases ,vitiligo ,Hashimoto’s disease ,autoimmune polyendocrine syndromes ,Medicine ,Dermatology ,RL1-803 - Abstract
Vitiligo is a quite frequently occurring skin disease. Although it does not cause any pain or internal organ damage, it constitutes a significant cosmetic problem having a significant impact on quality of life. A number of factors can influence the disease pathogenesis, including the genetic background, environmental factors and stress. Studies performed in recent years indicate the role of immunological phenomena in the development of vitiligo, as is confirmed by co-occurrence with other autoimmune diseases such as thyroid disease, rheumatoid arthritis, psoriasis, diabetes and many autoimmune polyendocrine syndromes. In the manuscript the clinical presentation, course of the disease and prognostic symptoms are also presented. Understanding the causes of skin depigmentation may allow for the development of effective therapeutic methods, and the knowledge of coexistence with other autoimmune diseases will help with the early diagnostic process.
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- 2016
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5. Does inflammation play a role in development of necrobiosis lipoidica?
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Iwona Słowik-Kwiatkowska, Aleksandra Lesiak, Anna Woźniacka, Anna Sysa-Jędrzejowska, and Joanna Narbutt
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necrobiosis lipoidica ,TNF-α ,angiogenesis ,inflammation ,Medicine ,Dermatology ,RL1-803 - Abstract
Introduction. Necrobiosis lipoidica (NL) is a granulomatous skin disease of still only partially known pathogenesis. Microangiopathy is considered as one of the most important processes in NL, and vascular endothelial growth factor (VEGF) and endothelin-1 are strongly involved in it. Recent studies have demonstrated the beneficial therapeutic effect of tumor necrosis factor α (TNF-α) inhibitors in treatment of recalcitrant cases of NL, which is due to the important role of TNF-α in development of inflammation and granulomas in the course of NL. Objective. To assess the serum levels of VEGF, endothelin-1 and TNF-α in NL patients. Material and methods . The study group consisted of 17 patients with NL (mean age 48.22 ±15.99 years), 37 patients with diabetes mellitus (mean age 52.11 ±17.41 years) and 23 healthy volunteers (mean age 44.13 ±9.33 years) as a control group. Serum concentrations of TNF-α, VEGF and endothelin-1 were assessed in all patients with the ELISA test. Results. The TNF-α concentration was statistically lower in the controls when compared to the NL patients and diabetic patients (p 0.05 for all comparisons). Endothelin-1 serum values were under the tested values in most cases; however, statistically more frequently these values were found in the controls than in the NL group (p < 0.05). Conclusions. The results of our study suggest that inflammation with enhanced synthesis of TNF-α in NL patients is the primary pathological effect, followed by local impairment of angiogenesis.
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- 2014
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6. Zaburzenia psychiczne w toczniu rumieniowatym układowym
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Anna Bogaczewicz, Tomasz Sobów, Jarosław Bogaczewicz, Jakub Ząbek, Przemysław Bieńkowski, Jan Kowalski, Ewa Robak, Anna Sysa-Jędrzejowska, and Anna Woźniacka
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toczeń rumieniowaty układowy ,toczeń neuropsychiatryczny ,zaburzenia psychiczne ,zaburzenia nastroju ,zaburzenia poznawcze ,Medicine - Abstract
Toczeń rumieniowaty układowy (systemic lupus erythematosus, SLE) jest chorobą tkanki łącznej, rozwijającą się na podłożu autoimmunizacji. Objawy kliniczne SLE są związane z występowaniem nie tylko wykwitów skórnych, ale również dolegliwości ze strony narządów wewnętrznych, a także zaburzeń hematologicznych oraz o charakterze neuropsychiatrycznym. Patogeneza NPSLE (neuropsychiatric systemic lupus erythematosus) jest złożona, próbuje się ją wyjaśniać wytwarzaniem autoprzeciwciał oraz odkładaniem się kompleksów immunologicznych, czego następstwem jest cytotoksyczne uszkodzenie neuronów, jak również nieprawidłową ekspresją mediatorów zapalnych i napływem komórek zapalnych, zaburzeniami naczyniowymi i skłonnością do zakrzepów. Całkowita częstość występowania NPSLE jest szacowana na 56,3% pacjentów z SLE. Najczęściej występującymi zaburzeniami psychicznymi u chorych na toczeń rumieniowaty są zaburzenia nastroju, lękowe, poznawcze oraz świadomości. Istotnym aspektem są także polekowe zaburzenia psychiczne. W podejściu terapeutycznym wobec pacjentów z NPSLE o nieznacznej aktywności choroby i/lub nieznacznym stopniu zmian narządowych stosuje się glikokortykosteroidy w niskich dawkach oraz – w zależności od potrzeb – leki przeciwlękowe, przeciwdepresyjne, niekiedy kwas walproinowy, karbamazepinę, lamotryginę i preparaty przeciwpsychotyczne. W profilaktyce przeciwzakrzepowej u chorych z grupy ryzyka stosuje się kwas acetylosalicylowy.
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- 2013
7. Współistnienie linijnej IgA dermatozy pęcherzowej z atopowym zapaleniem skóry. Trudności diagnostyczne. Opis przypadku
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Marcin Zakrzewski, Aleksandra Lesiak, Joanna Pietrzyk, Anna Sysa-Jędrzejowska, and Joanna Narbutt
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linijna IgA dermatoza pęcherzowa ,atopowe zapalenie skóry ,terapia ,Medicine ,Dermatology ,RL1-803 - Abstract
Wprowadzenie: Linijna IgA dermatoza pęcherzowa (ang. linear IgAbullous dermatosis – LABD) jest przewlekłą autoimmunologiczną chorobąpęcherzową skóry, która niezwykle rzadko współistnieje z innymischorzeniami. Cel pracy: Przedstawienie wyjątkowo rzadkiego współistnienia LABDz atopowym zapaleniem skóry (AZS). Opis przypadku: Kobieta, lat 28, zgłosiła się do poradni dermatologicznejz powodu rozsianych na skórze całego ciała, układających sięobrączkowato zmian pęcherzowych na rumieniowym podłożu oraznadżerek w obrębie błon śluzowych jamy ustnej. Poza tym na skórzetwarzy, nadgarstków oraz w zgięciach łokciowych stwierdzano zmianytypowe dla AZS. Pacjentka od wczesnego dzieciństwa choruje naAZS, idiopatyczną nadpłytkowość oraz obecnie na bezobjawowewrzodziejące zapalenie jelita grubego. U matki kobiety rozpoznanostwardnienie rozsiane. W badaniu immunofluorescencyjnym bezpośrednimwycinka skóry wykazano obecność linijnych złogów IgA nagranicy skórno-naskórkowej, za pomocą badania immunofluorescencyjnegopośredniego nie stwierdzono obecności przeciwciał reagującychz błoną podstawną, a metodą ELISA przeciwciał anty-NC16A. Napodstawie obrazu klinicznego oraz wykonanych badań rozpoznanoLABD, co dodatkowo potwierdzono badaniem wycinka skóry metodąmikroskopii konfokalnej. Ze względu na nadpłytkowość pacjentkabyła konsultowana hematologicznie i miała wykonaną biopsję szpiku.Rozpoznano u niej nadpłytkowość idiopatyczną. Pomimo zaburzeńhematologicznych podjęto leczenie prednizonem w dawkach zmniejszającychsię (od 40 mg/dobę) oraz enoksaparyną. Podczas terapiiobserwowano systematyczną poprawę kliniczną, pęcherze wchłonęłysię, pozostawiając pozapalne przebarwienia. Przy redukcji dawki prednizonuobserwowano stopniowe pogarszanie się zmian skórnych typowychdla AZS, zwłaszcza w obrębie twarzy i kończyn górnych. Z tegowzględu włączono leczenie cyklosporyną A. Wnioski: Przypadek przedstawiono ze względu na niezmiernie rzadkiewspółistnienie LABD z AZS oraz trudności terapeutyczne wynikająceze współwystępowania innych chorób.
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- 2011
8. Zastosowanie leków biologicznych w nietypowych postaciach łuszczycy – opis przypadków
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Michał Rogowski-Tylman, Aleksandra Lesiak, Anna Sysa-Jędrzejowska, Anna Brucka-Stemkowska, Dorota Sobolewska, and Joanna Narbutt
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łuszczyca ,inhibitory TNF-α ,ustekinumab ,Medicine ,Dermatology ,RL1-803 - Abstract
Wprowadzenie: Łuszczyca jest ciężką, przewlekłą chorobą, w przebieguktórej występują liczne zaburzenia immunologiczne. Wprowadzeniedo lecznictwa dermatologicznego terapii biologicznej stało się przełomemze względu na jej bardzo dużą skuteczność i bezpieczeństwow opornych na leczenie przypadkach łuszczycy zwyczajnej oraz łuszczycowegozapalenia stawów. Często jednak nietypowe postacie łuszczycy,takie jak: uogólniona łuszczyca krostkowa, łuszczyca odwrócona,łuszczyca skóry owłosionej głowy, łuszczyca ograniczona do rąki stóp, sprawiają istotne problemy terapeutyczne. Mimo braku rejestracjileków biologicznych do leczenia powyższych odmian łuszczycy,w piśmiennictwie spotyka się opisy zastosowania tych preparatóww nietypowych postaciach psoriasis. Cel pracy: Przedstawienie 3 przypadków klinicznych zastosowanialeków biologicznych we wskazaniach pozarejestracyjnych – w nietypowychpostaciach łuszczycy. Opis przypadków: Przypadek 1. dotyczy 24-letniej kobiety z łuszczycąograniczoną do dłoni i stóp opornej na leczenie etanerceptem, adalimumabemi ustekinumambem, przypadek 2. – 54-letniej kobietyz uogólnioną łuszczycą krostkową leczonej skutecznie infliksymabemoraz przypadek 3. – 27-letniego mężczyzny z oporną na leczenie łuszczycązwyczajną o nietypowej lokalizacji, u którego poprawę klinicznąuzyskano po zastosowaniu adalimumabu. Wnioski: Przedstawione przypadki oraz dane z piśmiennictwa wskazują,że leki biologiczne mogą być stosowane alternatywnie w terapiinietypowych postaci łuszczycy.
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- 2011
9. Wpływ niskich nierumieniotwórczych dawek promieniowania ultrafioletowego B na ekspresję reduktazy metylenotetrahydrofolianowej w skórze
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Anna Sysa-Jędrzejowska, Michał Rogowski-Tylman, Rafał Pawliczak, Karolina Wódz-Naskiewicz, Aleksandra Lesiak, and Joanna Narbutt
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promieniowanie ultrafioletowe ,ekspresja MTHFR ,fotoprotekcja ,Medicine ,Dermatology ,RL1-803 - Abstract
Wprowadzenie: Promieniowanie ultrafioletowe (ultraviolet radiation –UVR) jest jednym z głównych czynników zaangażowanych w procesfo to kancerogenzy. Powszechnie uznany jest fakt niszczenia folianówprzez ekspozycję na promieniowanie UVA, jednakże do chwili obecnejnie został do końca wyjaśniony wpływ promieniowania UVB na stężenietych związków. Dane z piśmiennictwa sugerują, że foliany, a zwłaszczaich metabolit 5-metylenotetrahydrofolian, jest niezbędny w procesach na -praw czych zmian w DNA zachodzących pod wpływem UVR. Reduktazametylenotetrahydrofolianowa (methylenetetrahydrofolate reductase – MTHFR)jest enzymem odgrywającym istotną rolę w metabolizmie folianów. Cel pracy: Ocena wpływu promieniowania UVB na ekspresję MTHFRw skórze. Materiał i metodyka: Badaniem objęto cztery grupy zdrowych wolontariuszy.Pierwszą grupę stanowiły osoby naświetlane nierumieniotwórczymidawkami UVB przez 10 kolejnych dni (10 × 0,7 MED – całeciało). Grupę drugą stanowili wolontariusze eksponowani równieżprzez 10 kolejnych dni na nierumieniotwórcze dawki UVB, a następnienaświetlani aplikowaną miejscowo (10 × 10 cm, skóra pośladka)wysoką dawką 3 MED UVB. Kolejną grupę ochotników poddawanoekspozycji jedynie na pojedynczą, miejscowo aplikowaną dawkę3 MED. Grupę kontrolną stanowiły osoby nienaświetlane. U wszystkichwolontariuszy pobierano biopsje ze skóry pośladka, w którychoceniano ekspresję MTHFR przy zastosowaniu metody Western blot. Wyniki: Ekspresja MTHFR była istotnie wyższa w grupie naświetlanejprzez 10 kolejnych dni nierumieniotwórczymi dawkami UVBw porównaniu z ekspresją tego białka u wolontariuszy eksponowanychprzewlekłe przez 10 kolejnych dni na nierumieniotwórcze dawkiUVB, a następnie naświetlanych w obrębie skóry pośladka dawką3 MED (p < 0,05). Wnioski: Wzrost ekspresji MTHFR występujący pod wpływem niskichprzewlekłych dawek UVB może być dowodem na fotoprotekcyjne właściwościfolianów.
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- 2011
10. Retrospektywna analiza obrazu klinicznego u chorych z pierwotnymi chłoniakami skóry
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Joanna Narbutt, Anna Sysa-Jędrzejowska, Dorota Sobolewska, and Aleksandra Lesiak
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pierwotne chłoniaki skóry ,ziarniniak grzybiasty ,zespół Sezary’ego ,erytrodermia ,Medicine ,Dermatology ,RL1-803 - Abstract
Wprowadzenie. Wśród pierwotnych chłoniaków skóry dominująpostaci wywodzące się z limfocytów T. Najczęściej występującą jednostkąchorobową jest ziarniniak grzybiasty. Pierwsze zmiany skórne sączęsto nieswoiste i sprawiają niekiedy istotne problemy diagnostyczne. Cel pracy: Dokonanie retrospektywnej analizy pacjentów leczonychz powodu pierwotnych chłoniaków skóry w Klinice Dermatologiii Wenerologii Uniwersytetu Medycznego w Łodzi w latach 1985–2005. Materiał i metodyka: Materiał stanowiło 64 pacjentów (43 mężczyzn,21 kobiet) w średnim wieku 60 lat. Badanie oparto na analizie historiichorób, ze szczególnym uwzględnieniem rozpoznania wstępnego,badania podmiotowego, przedmiotowego (charakter i lokalizacjazmian skórnych), badań laboratoryjnych oraz badania histopatologicznegowycinków skóry. Wyniki: Badana grupa obejmowała 60 przypadków ziarniniaka grzybiastegoi 4 przypadki zespołu Sezary’ego. Na podstawie przeprowadzonejanalizy wykazano, że u 70% chorych z rozpoznaniem ziarniniakagrzybiastego wstępna diagnoza obejmowała inne jednostkichorobowe, w tym wyprysk i łuszczycę. Najczęściej zgłaszaną dolegliwościąbył świąd skóry, zmiany chorobowe zazwyczaj były rozsiane,lokalizowały się głównie na kończynach górnych i dolnych. Wnioski: W większości przypadków pierwotnych chłoniaków skórypoczątkowe objawy choroby były mało charakterystyczne i stanowiłyproblem diagnostyczny.
- Published
- 2011
11. Ekspresja receptora dla witaminy D oraz reduktazy metylenotetrahydrofolianowej w rakach podstawnokomórkowych
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Adam Włodarkiewicz, Joanna Narbutt, Michał Sobjanek, Michał Rogowski-Tylman, Anna Sysa-Jędrzejowska, Rafał Pawliczak, Aleksandra Lesiak, and Karolina Wódz-Naśkiewicz
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rak podstawnokomórkowy ,ekspresja VDR i MTHFR ,kancerogeneza ,Medicine ,Dermatology ,RL1-803 - Abstract
Wprowadzenie: Dane z literatury wskazują na udział receptora dlawitaminy D (ang. vitamin D receptor – VDR) w rozwoju nowotwo równarządów wewnętrznych oraz raków skóry. W pojedynczychpracach analizowano rolę reduktazy metylenotetrahydrofolianowej(ang. methylenetetrahydrofolate reductase – MTHFR), której nieprawidłowaaktywność związana jest z indukcją kancerogenezy. Cel pracy: Ocena stężenia 25(OH)D oraz parathormonu w surowicyu pacjentów z rakiem podstawnokomórkowym (ang. basal cell carcinoma– BCC), a także analiza ekspresji VDR i MTHFR w bioptatach zezmian skórnych typu BCC. Materiał i metodyka: Badaniem objęto grupę 79 chorych z BCC oraz46 wolontariuszy stanowiących grupę kontrolną. U wszystkich badanychoznaczano stężenie witaminy D i parathormonu w surowicy,natomiast u 44 pacjentów z BCC oraz 30 wolontariuszy pobieranobiopsje skóry celem oznaczenia ekspresji VDR i MTHFR. Wyniki: Stężenie 25(OH)D było statystycznie istotnie wyższe w grupiekontrolnej niż u chorych na BCC (p = 0,0026), podczas gdy stężenieparathormonu w surowicy pacjentów z BCC było istotnie wyższew porównaniu z grupą kontrolną (p < 0,0001). U chorych na BCCwykazano istotnie wyższą ekspresję VDR niż w grupie kontrolnej(p < 0,001). Taką samą zależność obserwowano w odniesieniu do ekspresjiMTHFR, która była istotnie wyższa w bioptatach skóry pobranychze zmian typu BCC w porównaniu z grupą kontrolną (p < 0,01). Wnioski: Na podstawie wyników badań własnych nie można jednoznacznieokreślić roli VDR i MTHFR w rozwoju raków podstawnokomórkowychskóry, jakkolwiek wiele argumentów przemawia za ichistotnym udziałem w procesie kancerogenezy. Stąd też uzasadnionejest prowadzenie dalszych, kompleksowych i wieloośrodkowychbadań celem poznania złożonej etiopatogenezy BCC.
- Published
- 2010
12. Brak związku polimorfizmu –590 C/T genu IL-4 oraz –1082 A/G genu IL-10 z rozwojem atopowego zapalenia skóry
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Anna Sysa-Jędrzejowska, Piotr Kuna, Iwona Stelmach, Karolina Przybyłowska, Aleksandra Lesiak, Marcin Zakrzewski, and Joanna Narbutt
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atopowe zapalenie skóry ,polimorfizm –590 C/T genu IL-4 ,polimorfizm –1082 A/G genu IL-10 ,patogeneza ,Medicine ,Dermatology ,RL1-803 - Abstract
Wprowadzenie: Atopowe zapalenie skóry (AZS) jest przewlekłą,zapalną dermatozą, często współistniejącą z innymi chorobami atopowymi,takimi jak astma, alergiczny nieżyt nosa bądź spojówek. Wśródwielu czynników etiopatogenetycznych podłoże genetyczne, obejmującepolimorfizmy i mutacje w genach kodujących białka zaangażowanew prawidłową budowę bariery naskórkowej oraz odpowiedź immunologiczną,jest przedmiotem wielu prac badawczych. W patogenezieAZS szczególną rolę przypisuje się cytokinom Th2-zależnym, w tyminterleukinom 4 i 10 (IL-4 i IL-10). Cel pracy: Ocena polimorfizmów regionu promotorowego –590 C/Tgenu IL-4 oraz 1082 A/G genu IL-10 u pacjentów z AZS zamieszkującychteren województwa łódzkiego. Materiał i metodyka: Grupę badawczą stanowiło 163 chorych na AZS,u których rozpoznanie choroby ustalono na podstawie kryteriów Hanifinai Rajki, natomiast grupę kontrolną 204 zdrowych wolontariuszy.Nasilenie procesu chorobowego u wszystkich chorych oceniono przyużyciu skali Rajki i Langelanda. Analizę wariantów polimorficznychw regionie promotorowym genów IL-4 i IL-10 przeprowadzono metodąRFLP-PCR z wykorzystaniem enzymów restrykcyjnych do wykrywaniazmian w sekwencji DNA. Wyniki: Nie wykazano istotnych statystycznie różnic w rozkładziegenotypów polimorfizmów –590 C/T dla IL-4 oraz –1082 A/G genuIL-10 między grupą pacjentów a grupą kontrolną (p > 0,05 dla wszystkichporównań). W badanych polimorfizmach genów kodujących IL-4i IL-10 rozkład genotypów nie różnił się statystycznie istotnie w grupiepacjentów mających łagodny przebieg AZS od chorych z AZS o umiarkowanymi ciężkim przebiegu. Nie stwierdzono (p > 0,05) równieżzwiązku między badanymi polimorfizmami genów IL-4 i IL-10 a wczesnymzachorowaniem na astmę. Wnioski: Brak pozytywnej korelacji między obecnością polimorfizmówgenów IL-4 oraz IL-10 a rozwojem AZS w badanej grupie chorychmoże świadczyć o odmienności genetycznej badanej populacji,a także o dużej różnorodności czynników genetycznych zaangażowanychw patogenezę tego schorzenia, zależnie od pochodzenia chorych.
- Published
- 2010
13. Nieswoiste zmiany skórne o charakterze naczyniowym w przebiegu tocznia rumieniowatego układowego
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Tomasz Hawro, Anna Sysa-Jędrzejowska, and Anna Woźniacka
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zapalenie naczyń ,pokrzywka naczyniowa ,sinica siateczkowata ,plamica wyczuwalna palpacyjnie ,owrzodzenie skóry ,Medicine ,Dermatology ,RL1-803 - Abstract
Wprowadzenie: Wykwity skórne w przebiegu tocznia rumieniowategomogą mieć charakter swoisty o charakterystycznym obrazie histopatologicznymlub nieswoisty, bez typowych cech w badaniu mikroskopowym.Wśród zmian skórnych nieswoistych najliczniejszą grupęstanowią zmiany o charakterze naczyniowym, do których zalicza się:owrzodzenia, sinicę siateczkowatą, pokrzywkę naczyniową, plamicęwyczuwalną palpacyjnie, zmiany wybroczynowe, rumienie w obrębiepowierzchni dłoniowych rąk oraz wałów paznokciowych i zmianymartwicze na opuszkach palców. Cel pracy: Określenie częstości występowania nieswoistych zmianskórnych o charakterze naczyniowym u chorych na SLE oraz ocena ichzwiązku z innymi parametrami klinicznymi. Materiał i metodyka: Badaną grupę stanowiło 63 chorych na SLE. Rozpoznanieustalono na podstawie aktualnie obowiązujących kryteriówAmerican College of Rheumatology. Wiek chorych zawierał się w przedzialeod 20 do 67 lat, średnia 41 lat. Aktywność procesu chorobowegooceniono przy użyciu skali aktywności tocznia układowego SystemicLupus Activity Measure (SLAM). Wyniki: Nieswoiste dla tocznia zmiany skórne o podłożu naczyniowymwystępowały u 77,78% chorych. Owrzodzenia obserwowanou 11,11%, sinicę siateczkowatą u 30,16%, pokrzywkę naczyniowąu 7,94%, zmiany rumieniowe na skórze kłębu i kłębika u 58,73%,rumień na opuszkach palców u 52,38%, rumień okołopaznokciowyu 33,33%, „objaw drzazgi” u 17,46%, zmiany plamicze o charakterzewybroczyn na kończynach u 30,16%, plamicę wyczuwalną palpacyjnieu 6,35% i zmiany martwicze na opuszkach palców u 9,5% badanych.Stwierdzono istotną zależność (p < 0,05) między aktywnością procesuchorobowego a obecnością: owrzodzeń, sinicy siateczkowatej,pokrzywki naczyniowej, wybroczyn podpaznokciowych, wybroczynna skórze kończyn i plamicy wyczuwalnej palpacyjnie. Wnioski: Związek między określonymi nieswoistymi dla toczniawykwitami o charakterze naczyniowym a aktywnością procesu chorobowegomoże wskazywać na ich wartość rokowniczą.
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- 2010
14. Autoprzeciwciała przeciwko kalcytriolowi w toczniu rumieniowatym układowym – doniesienie wstępne
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Jarosław Bogaczewicz, Anna Sysa-Jędrzejowska, Jakub Ząbek, Ewa Kontny, and Anna Woźniacka
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toczeń rumieniowaty układowy ,witamina D ,kalcytriol ,kalcydiol ,autoprzeciwciała ,Medicine ,Dermatology ,RL1-803 - Abstract
Wprowadzenie: U chorych na toczeń rumieniowaty układowy (ang.systemic lupus erythematosus – SLE) często stwierdza się niedobór witaminyD. Spośród możliwych przyczyn tego stanu rozpatruje się: objęcieprocesem chorobowym nerek, terapię z zastosowaniem kortykosteroidówlub leków przeciwmalarycznych, a także fotoprotekcję.Dotychczas nie w pełni poznany jest wpływ autoprzeciwciał skierowanychprzeciwko kalcytriolowi na stężenie kalcydiolu w surowicy. Cel pracy: Ocena częstości występowania autoprzeciwciał skierowanychprzeciwko kalcytriolowi w grupie chorych na SLE. Materiał i metodyka: Badaniem objęto grupę 37 chorych na SLE. Grupękontrolną stanowiło 30 zdrowych dawców krwi. Przeciwciała oznaczanometodą immunoenzymatyczną. Wyniki: Autoprzeciwciała skierowane przeciwko kalcytriolowiwykryto u 3 pacjentów (8,1%) z SLE. Nie stwierdzono istotnej statystycznieróżnicy w stężeniu kalcydiolu [25(OH)D3] między chorymi,u których obecne były przeciwciała skierowane przeciwko kalcytriolowi,a osobami bez tych przeciwciał. Wnioski: W surowicy chorych na SLE obserwuje się autoprzeciwciałaprzeciwko kalcytriolowi, jednak ich obecność wydaje się nie wpływaćna występowanie niedoboru witaminy D.
- Published
- 2010
15. Circulating TCR γδ Cells in the Patients with Systemic Lupus Erythematosus
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Ewa Robak, Jerzy Z. Błoński, Jacek Bartkowiak, Hanna Niewiadomska, Anna Sysa-Jędrzejowska, and Tadeusz Robak
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Pathology ,RB1-214 - Abstract
Systemic lupus erythematosus (SLE) is a disorder with a wide range of immunological abnormalities. The results of the studies undertaken in the last decade indicated that SLE pathogenesis was mainly connected with the breakdown of the activation control of B and T cells, generating humoral or cell-mediated responses against several self-antigens of affected cells. The last studies demonstrate that the role of γδ T lymphocytes in autoimmune diseases can be especially important. Flow cytometry techniques were used to investigate the number and percentage of TCR γδ T cells and their most frequent subtypes in peripheral blood of 32 patients with SLE and 16 healthy volunteers. We also correlated TCR γδ cells number with the level of T CD3+, T CD4+, T CD8+, and NK (CD16) cells (cytometric measurements) and SLE activity (on the basis of clinical investigations). Our studies were preliminary attempts to evaluate the role of that minor T cell subpopulation in SLE. Absolute numbers of cells expressing γδ TCR in most SLE blood specimens were significantly lower than in the control group (P
- Published
- 1999
- Full Text
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16. Expression of Selected Integrins and Selectins in Bullous Pemphigoid
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Elżbieta Waszczykowska, Anna Erkiert-Polguj, Ewa Joss-Wichman, Małgorzata Wągrowska-Danilewicz, Anna Sysa-Jędrzejowska, and Agnieszka Żebrowska
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Pathology ,RB1-214 - Published
- 2007
- Full Text
- View/download PDF
17. Dermatomyositis. Diagnostic and therapeutic recommendations of the Polish Dermatological Society
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Anna Woźniacka, Joanna Maj, Adam Reich, Lidia Rudnicka, Anna Lis-Święty, Anna Sysa-Jędrzejowska, Anna Wojas-Pelc, Joanna Narbutt, and Dorota Krasowska
- Subjects
medicine.medical_specialty ,dermatomyositis ,business.industry ,idiopathic inflammatory myopathies ,Dermatology ,Dermatomyositis ,medicine.disease ,treatment ,Idiopathic inflammatory myopathies ,autoimmune diseases of connective tissue ,RL1-803 ,medicine ,Medicine ,business - Abstract
Dermatomyositis is an autoimmune disease characterized by skin lesions and/or symptoms of myositis. In addition to the so-called classic dermatomyositis the following forms of dermatomyositis are distinguished based on the clinical presentation: pediatric, paraneoplastic, drug-induced and amyopathic. A number of disease-specific autoantibodies are identified in dermatomyositis (including anti-Mi2, anti-TIF1, anti-NXP2, anti-SAE or anti-MDA5), presence of which may be associated with a specific clinical phenotype. The diagnosis of the severity of muscle involvement is currently based mainly on physical examination, deviations in results of laboratory investigations, electromyographic examination and imaging examination, mainly with the use of magnetic resonance imaging. Systemic glucocorticosteroids administered as monotherapy or in combination with other immunosuppressants remain the mainstay of dermatomyositis treatment, and in the absence of satisfactory improvement, intravenous immunoglobulins are used. In addition, in case of interstitial lung disease, the use of cyclophosphamide may be necessary. The choice of a therapy, as well as the rate of dose reduction, depend on the dynamics of the disease, symptoms, diagnosed immunological disorders, as well as comorbidities and the drugs used. Each diagnostic and therapeutic decision must take into account the individual clinical data of the patient and current scientific reports.
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- 2021
18. Long-term treatment of chronic plaque psoriasis with biological drugs can control platelet activation: targeting the bridge between inflammation and atherothrombosis
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Joanna Narbutt, Aleksandra Lesiak, Andrzej Langner, Bartłomiej Kwiek, and Anna Sysa-Jędrzejowska
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medicine.medical_specialty ,lcsh:Internal medicine ,Dermatology ,030204 cardiovascular system & hematology ,comorbidities ,Gastroenterology ,Etanercept ,030207 dermatology & venereal diseases ,03 medical and health sciences ,0302 clinical medicine ,Psoriasis Area and Severity Index ,Psoriasis ,Internal medicine ,atherothrombosis ,Ustekinumab ,medicine ,Adalimumab ,lcsh:Dermatology ,Immunology and Allergy ,Platelet ,Platelet activation ,lcsh:RC31-1245 ,Original Paper ,business.industry ,psoriasis ,lcsh:RL1-803 ,medicine.disease ,Infliximab ,humanities ,Immunology ,platelets ,P-selectin ,business ,biological ,medicine.drug - Abstract
Introduction : Platelet activation is elevated in moderate to severe psoriasis, and the reduction in platelet activation during short-term treatment has already been demonstrated. Soluble P-selectin is a well-established marker of platelet activation. Aim : To show whether the long-term treatment of psoriasis with biological drugs can reduce elevated platelet activation. Material and methods : An observational study of 27 patients with chronic plaque psoriasis, treated with infliximab, adalimumab, etanercept, or ustekinumab for up to 12 months was conducted. Psoriasis area and severity index (PASI), serum P-selectin and interleukin (IL)-6 were monitored throughout the treatment. Results : There was no significant correlation between PASI and platelet activation in our patients. After 3 months of treatment, a significant reduction in PASI and IL-6 was found, while P-selectin was not significantly reduced. When a cohort of patients who had shown elevated P-selectin prior to the treatment was evaluated, a significant reduction in P-selectin was observed in all 8 patients following 3 months; a reduction that was sustained after 6 and 12 months of therapy. Conclusions : We conclude that PASI is not a good predictor of platelet activity in patients with PASI near to 10. Biological drugs reduce platelet activation in patients who have increased platelet activation prior to treatment, and this effect is stable during chronic therapy.
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- 2017
19. Systemic sclerosis – diagnostic and therapeutic recommendations of the Polish Dermatological Society. Part 1: diagnosis and monitoring
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Lidia Rudnicka, Dorota Krasowska, Slawomir Majewski, Anna Woźniacka, Joanna Czuwara, Anna Sysa-Jędrzejowska, Anna Wojas-Pelc, Anna Lis-Święty, Joanna Maj, Grażyna Chodorowska, and Aleksandra Dańczak-Pazdrowska
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medicine.medical_specialty ,systemic sclerosis ,business.industry ,lcsh:R ,lcsh:Medicine ,Dermatology ,lcsh:RL1-803 ,monitoring ,diagnostics ,lcsh:Dermatology ,Physical therapy ,Medicine ,guidelines ,business ,Intensive care medicine - Abstract
Systemic sclerosis is an immune-mediated disease characterized by a chronic and progressive course. It often leads to multiorgan failure and patient disability, and contributes to significant reduction in the quality of life. Systemic sclerosis affects the skin, subcutaneous tissue, muscles, osteoarticular system and internal organs. The complexity and diversity of clinical presentations require an individual approach and multidisciplinary collaboration both at the stage of diagnosis and treatment. Critical factors in systemic sclerosis include early diagnosis, assessment of internal organ involvement, identification of patients at potential risk of organ complications, assessment of disease dynamics and activity, and implementation of optimal therapy. Part 1 presents current recommendations for the diagnostics and monitoring of patients with systemic sclerosis. Attention is given to classification criteria, clinical forms of systemic sclerosis, assessment of skin thickness and systemic sclerosis microangiopathy, significance of antinuclear antibodies, diagnosis of interstitial lung disease and pulmonary arterial hypertension, renal crisis and cardiac abnormalities, and evaluation of the gastrointestinal tract and osteoarticular and muscular systems.
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- 2017
20. Localized scleroderma (morphea) : diagnostic and therapeutic recommendations of the Polish Dermatological Society
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Lidia Rudnicka, Joanna Czuwara, Dorota Krasowska, Anna Wojas-Pelc, Anna Woźniacka, Slawomir Majewski, Anna Sysa-Jędrzejowska, Joanna Maj, Anna Lis-Święty, Aleksandra Dańczak-Pazdrowska, and Grażyna Chodorowska
- Subjects
medicine.medical_specialty ,treatment ,business.industry ,lcsh:R ,lcsh:Medicine ,Dermatology ,lcsh:RL1-803 ,clinical picture ,classification ,Localized scleroderma morphea ,medicine ,lcsh:Dermatology ,business ,Localized Scleroderma ,localized scleroderma - Abstract
Localized scleroderma (morphea) is a chronic autoimmune disease of the connective tissue. Its etiopathogenesis is unknown. Most often the disease affects the skin, but may also involve the subcutis, muscles, and the osteoarticular system. The clinical presentation and the course of disease may be diverse. This article presents clinical characteristics of various types of the disease, the classification of its subtypes, recommendations for differential diagnosis and treatment.
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- 2019
21. Medium dose ultraviolet A1 phototherapy and mRNA expression of interleukin 8, interferon γ, and chemokine receptor 4 in acute skin lesions in atopic dermatitis
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Anna Wozniacka, Jarosław Bogaczewicz, Anna Sysa-Jędrzejowska, and Karolina Malinowska
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medicine.medical_specialty ,lcsh:Internal medicine ,Dose ,Dermatology ,030207 dermatology & venereal diseases ,03 medical and health sciences ,Chemokine receptor ,0302 clinical medicine ,Interferon ,Internal medicine ,medicine ,lcsh:Dermatology ,Immunology and Allergy ,030212 general & internal medicine ,SCORAD ,Interleukin 8 ,lcsh:RC31-1245 ,Original Paper ,Messenger RNA ,medicine.diagnostic_test ,atopic dermatitis ,business.industry ,interleukin ,Interleukin ,Atopic dermatitis ,interferon ,lcsh:RL1-803 ,medicine.disease ,Endocrinology ,UVA ,business ,medicine.drug ,phototherapy - Abstract
Introduction : Mechanisms responsible for UVA1 efficacy in atopic dermatitis (AD) are not fully elucidated. Aim: To investigate IL-8, CCR-4, and IFN-γ mRNA expression in AD before and after UVA1, to identify correlations among them, and to determine whether and to what degree mRNA expression is influenced by UVA1. Material and methods : Twenty-five patients with AD underwent medium dose UVA1-phototherapy at daily dosages of 10, 20, 30, 45, and then continuing 45 J/cm 2 up to 20 days, from Monday to Friday for 4 weeks. Before and after UVA1, biopsies from acute skin lesions were studied using reverse-transcription and RT-PCR. Results : The levels of CCR-4 mRNA correlated with those of IFN-γ, both before and after UVA1 phototherapy (p < 0.05). A significant correlation was found after UVA1 between mRNA levels of IL-8 and IFN-γ (p < 0.05). After UVA1 an increase in IL-8 mRNA expression in comparison to the baseline assessment (p = 0.02) was found, while no significant difference was revealed in the expression of CCR-4 and IFN-γ mRNA. UVA1 improved both SCORAD and severity of AD (p < 0.001). SCORAD and the severity of AD did not correlate with the degree of expression of measured cytokine mRNA, neither before nor after UVA1. Conclusions : CCR-4 is expressed in parallel with IFN-γ in acute skin lesions of patients with AD both before and after UVA1 phototherapy. UVA1 significantly improves SCORAD index, lessens the severity of AD and increases the expression of IL-8, with no direct effects on other studied molecules.
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- 2016
22. The Effect of Enzyme Therapy on Skin Symptoms and Immune Responses in Patients with Dermatitis Herpetiformis
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Anna Sysa-Jędrzejowska, Teodor Stelmasiak, Finlay A. Macrae, Elżbieta Waszczykowska, Agnieszka Zebrowska, and Hugh J. Cornell
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Pulmonary and Respiratory Medicine ,chemistry.chemical_classification ,medicine.medical_specialty ,Erythema ,business.industry ,Placebo ,medicine.disease ,Gluten ,Gastroenterology ,Coeliac disease ,Serology ,Clinical trial ,chemistry ,Dermatitis herpetiformis ,Internal medicine ,Immunology ,medicine ,Itching ,medicine.symptom ,business - Abstract
Background: The aetiology of coeliac disease (CD) has many similarities to that of dermatitis herpetiformis (DH), except that DH lesions are mainly manifested in the skin. Mucosal enzyme deficiency plays an important part in CD pathology. Clinical studies indicated that the gluten exposure in CD could be partly corrected by the use of enzyme supplementation. Objective: Enzyme therapy, using enterically coated tablets containing caricain, was investigated as a means of protecting patients with DH against wheat gluten. Methods: A randomized, placebo-controlled clinical trial was carried out on 20 DH patients in clinical remission. The patients were divided into two groups of 10, one group given a placebo daily and the other the enzyme – containing tablets. Both groups were challenged with 6g of gluten daily in a double-blind trial. Symptoms and signs of skin involvement were recorded and graded at the start of the trial, after 7 days and after 14 days. Blood was also taken at the start and after 14 days and assayed for IgA EMA and anti-gliadin antibodies. Results: After 7 days the major features associated with DH were more severe and more common with the placebo compared with enzyme therapy. Before 14 days, seven patients in total, six on placebo, had to withdraw from the trial because of the effects of the gluten challenge whilst 2 patients on therapy developed blisters, erythema and itching. Serological tests indicated that IgA EmA antibodies and anti-gliadin antibodies after 14 days were not affected significantly, but indicated that abnormally high antibodies titers of both types were present in 8 patients at the start of the trial, suggesting the need for enzyme therapy in addition to the normal gluten-free diet for patient well-being. Conclusions: This study supports the use of enzyme supplementation as a safeguard for patients with DH on a nominal gluten-free diet.
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- 2016
23. Medium-dose ultraviolet A1 phototherapy improves SCORAD index and increases mRNA expression of interleukin-4 without direct effect on human β defensin-1, interleukin-10, and interleukin-31
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Anna Sysa-Jędrzejowska, Jarosław Bogaczewicz, Karolina Malinowska, and Anna Wozniacka
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Adult ,Male ,0301 basic medicine ,beta-Defensins ,Adolescent ,Gene Expression ,Dermatology ,Severity of Illness Index ,Ultraviolet therapy ,Dermatitis, Atopic ,Young Adult ,030207 dermatology & venereal diseases ,03 medical and health sciences ,0302 clinical medicine ,Gene expression ,medicine ,Humans ,RNA, Messenger ,SCORAD ,Interleukin 4 ,medicine.diagnostic_test ,business.industry ,Interleukins ,Pruritus ,Interleukin ,Radiotherapy Dosage ,Receptors, Interleukin ,Atopic dermatitis ,Middle Aged ,medicine.disease ,Interleukin-10 ,Interleukin 10 ,030104 developmental biology ,Interleukin 31 ,Immunology ,Female ,Ultraviolet Therapy ,Interleukin-4 ,business - Abstract
Background Effectiveness of ultraviolet (UV)A1 in flares of atopic dermatitis (AD) is thought to influence the expression of cytokines involved in its pathogenesis. The aim of the study was to investigate whether mRNA expression of human β defensin-1 (hβD-1) correlates with that of interleukin (IL)-4, IL-10, and IL-31 in skin lesions in AD before and after UVA1 phototherapy, to determine whether UVA1 decreases the expression of the aforementioned mediators, and to confirm whether changes in mRNA expression correspond with the clinical efficacy of UVA1. Methods Twenty-five patients with AD underwent medium-dose UVA1 phototherapy. Before and after UVA1, biopsies from acute skin lesions were studied using reverse transcription and real-time polymerase chain reaction. Results Levels of mRNA hβD-1 correlated with those of IL-10 and IL-31, levels of IL-4 mRNA correlated with those of IL-10 and IL-31, and IL-10 expression correlated with that of IL-31, both before and after UVA1. Phototherapy with UVA1 improved SCORing of Atopic Dermatitis (SCORAD) values, decreased pruritus, and increased expression of IL-4. After UVA1, no difference was found in the mRNA expression of other molecules. The SCORAD index did not correlate with the expression of any examined mRNA either before or after UVA1. Conclusions hβD-1, IL-4, IL-10, and IL-31 are expressed in acute skin lesions in AD, and their levels correlate with each other. UVA1 improves SCORAD and pruritus and increases the expression of IL-4 without direct effect on other molecules.
- Published
- 2016
24. Morbus Behçet – a rare disease in Central Europe
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Anna Sysa-Jędrzejowska, Marek Kot, Maciej Jabłkowski, Anna Woźniacka, and Piotr Jurowski
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Pathology ,medicine.medical_specialty ,Behçet's disease ,blood vessel inflammation ,business.industry ,Central asia ,General Medicine ,Disease ,Behcet's disease ,medicine.disease ,Dermatology ,classification ,medicine ,Etiology ,In patient ,business ,Stomatitis ,State of the Art Paper ,Rare disease ,Systemic vasculitis - Abstract
Behcet's disease (BD) is a multiorgan inflammatory disease of complex and not entirely elucidated etiology, which was originally diagnosed in patients with aphthous stomatitis, genital ulcerations and ocular manifestations. The entity is endemic in countries of Eastern and Central Asia, especially Turkey and Iran, but rarely seen in Central Europe. As there are no specific diagnostic laboratory tests or histopathologic findings which confirm the preliminary diagnosis, the final diagnosis should be based on clinical criteria. Frequently a definitive diagnosis is established within several years or months after the first manifestations appear. The increased number of cases, recently described worldwide also in the Polish population, indicates that the disease could spread out of endemic areas. The aim of this manuscript is to present the clinical picture, diagnosis criteria and therapeutic approaches of this "international disease" which currently is observed not only in emigrants from Asia but also in native Polish citizens.
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- 2015
25. Cutaneous lupus erythematosus : diagnostic and therapeutic recommendations of the Polish Dermatological Society
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Anna Lis-Święty, Maria Blaszczyk, Jacek C Szepietowski, Dorota Krasowska, Joanna Maj, Lidia Rudnicka, Anna Wojas-Pelc, Anna Sysa-Jędrzejowska, Anna Woźniacka, and Adam Reich
- Subjects
medicine.medical_specialty ,Lupus erythematosus ,business.industry ,Cutaneous Lupus Erythematosus ,Medicine ,Dermatology ,business ,medicine.disease - Published
- 2018
26. Expression of vascular endothelial growth factor and other cytokines in atopic dermatitis, and correlation with clinical features
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Zbigniew Samochocki, Jarosław Bogaczewicz, Anna Sysa-Jędrzejowska, Anna Wozniacka, Ewa Kontny, and Daniel P. McCauliffe
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Adult ,Male ,Vascular Endothelial Growth Factor A ,0301 basic medicine ,Adolescent ,medicine.medical_treatment ,Dermatology ,Severity of Illness Index ,Dermatitis, Atopic ,Pathogenesis ,Young Adult ,030207 dermatology & venereal diseases ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Severity of illness ,medicine ,Humans ,SCORAD ,Chemokine CCL5 ,Interleukin-15 ,medicine.diagnostic_test ,Interleukin-6 ,Tumor Necrosis Factor-alpha ,business.industry ,Interleukin-8 ,Case-control study ,Interleukin ,Atopic dermatitis ,Immunoglobulin E ,Middle Aged ,medicine.disease ,Vascular endothelial growth factor ,030104 developmental biology ,Cytokine ,chemistry ,Case-Control Studies ,Immunology ,Cytokines ,Female ,business - Abstract
Background Vascular endothelial growth factor (VEGF) was found increased in the stratum corneum of patients with atopic dermatitis (AD). However, its potential pathogenic role(s) in AD needs further clarification. Objective The aim of this study was to determine whether VEGF serum levels correlate with other selected cytokine levels and features of AD. Methods VEGF and other cytokine levels were measured in 83 patients with AD and in a control group and then correlated with clinical and laboratory parameters of AD. Results The mean serum concentrations of VEGF and tumor necrosis factor α were significantly higher in patients with AD than in the control group, whereas the mean interleukin eight serum level was lower. VEGF concentrations correlated with the severity of AD as expressed by SCORAD index and objective SCORAD. Conclusion VEGF could be regarded as a potentially important mediator in the pathogenesis of AD, as VEGF levels correlate somewhat with AD severity.
- Published
- 2015
27. Medium-dose ultraviolet A1 phototherapy and mRNA expression of TSLP, TARC, IL-5, and IL-13 in acute skin lesions in atopic dermatitis
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Anna Sysa-Jędrzejowska, Anna Wozniacka, Karolina Malinowska, and Jarosław Bogaczewicz
- Subjects
Adult ,Male ,Chemokine ,Thymic stromal lymphopoietin ,Dermatology ,Radiation Dosage ,Real-Time Polymerase Chain Reaction ,Severity of Illness Index ,Ultraviolet therapy ,Statistics, Nonparametric ,Dermatitis, Atopic ,Cohort Studies ,Young Adult ,030207 dermatology & venereal diseases ,03 medical and health sciences ,0302 clinical medicine ,Thymic Stromal Lymphopoietin ,Humans ,Medicine ,RNA, Messenger ,SCORAD ,Interleukin 5 ,Interleukin-13 ,medicine.diagnostic_test ,biology ,business.industry ,Atopic dermatitis ,Middle Aged ,medicine.disease ,Treatment Outcome ,Real-time polymerase chain reaction ,Acute Disease ,Interleukin 13 ,Immunology ,biology.protein ,Cytokines ,Female ,Ultraviolet Therapy ,Chemokine CCL17 ,Interleukin-5 ,business ,Biomarkers ,030215 immunology - Abstract
Background The mechanisms responsible for the efficacy of ultraviolet A1 (UVA1) in the treatment of atopic dermatitis (AD) are not fully understood. Objectives This study was designed to investigate mRNA expression of thymic stromal lymphopoietin (TSLP), thymus- and activation-regulated chemokine (TARC), interleukin-5 (IL-5), and IL-13 in AD before and after UVA1 therapy, to determine correlations among them, and to examine whether UVA1 influences their expression and whether it is associated with UVA1 efficacy. Methods Twenty-five patients with AD underwent medium-dose UVA1 phototherapy. Before and after UVA1, biopsies from acute skin lesions were studied using reverse transcription and real-time polymerase chain reaction. Results Levels of mRNA TSLP correlated with those of TARC, IL-5, and IL-13, and levels of TARC correlated with those of IL-5 and IL-13, both before and after UVA1. Expression of IL-5 correlated with that of IL-13 only before UVA1. SCORAD (SCORing of Atopic Dermatitis) indices correlated with levels of TARC and IL-5 before irradiation. After UVA1, no mRNA level correlated with the SCORAD index. Phototherapy with UVA1 improved SCORAD values (P < 0.001) and increased expression of TARC (P < 0.05) but did not affect mRNA expression of TSLP, IL-5, or IL-13. Conclusions Expression levels of the mediators TSLP, TARC, IL-5, and IL-13 in AD are interrelated. Phototherapy with UVA1 improves SCORAD indices and increases expression of TARC but has no direct effects on the expression of other molecules. It is likely that UVA1 also interferes with or acts via intermediators on the link between IL-5 and IL-13.
- Published
- 2015
28. Can biologic treatment induce cutaneous focal mucinosis?
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Marcin Włodarczyk, Aleksandra Lesiak, Joanna Sieniawska, Michał Rogowski-Tylman, Joanna Narbutt, Irmina Olejniczak-Staruch, Anna Sysa-Jędrzejowska, and Aleksandra Sobolewska
- Subjects
Pathology ,medicine.medical_specialty ,business.industry ,Case Report ,Dermatology ,psoriasis ,medicine.disease ,Infliximab ,Mucinosis ,medicine.anatomical_structure ,TNF-α antagonists ,Dermis ,Cutaneous focal mucinosis ,biological therapy ,Psoriasis ,Ustekinumab ,medicine ,Adalimumab ,adverse effects ,Immunology and Allergy ,business ,Adverse effect ,medicine.drug ,skin mucinosis - Abstract
Skin mucinosis is a rare skin disease which clinically manifests as firm papules and waxy nodules. We report a case of a 66-year-old female psoriatic patient who developed skin mucinosis during biological therapy. Because of a previous lack of response to the local and conventional systemic treatment of psoriasis, the patient received biological therapy (infliximab from June 2008 to May 2009 - initial clinical improvement and loss of treatment effectiveness in the 36(th) week of the therapy; adalimumab from June 2009 to January 2010 - lack effectiveness; ustekinumab from March 2012 to the present). Throughout 2 months we observed a manifestation of the skin mucinosis as well-demarcated, yellow and brown, papulo-nodular lesions of 5-10 mm in diameter, localized on the back. Histopathological examination with alcian blue staining demonstrated mucin deposits in the dermis. On the basis of clinical and histopathological findings, the diagnosis of cutaneous focal mucinosis was established. We present the case because of the extremely rare occurrence of the disease. Scarce literature and data suggest that there is an association between focal mucinosis and thyroid dysfunction, as well as possible adverse effects of biological therapy with TNF-α antagonists.
- Published
- 2014
29. Cellulite: a cosmetic or systemic issue? Contemporary views on the etiopathogenesis of cellulite
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Sławomir Tokarski, Jarosław Bogaczewicz, Kamila Tokarska, Anna Sysa-Jędrzejowska, and Anna Woźniacka
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lcsh:Internal medicine ,medicine.medical_specialty ,cellulite ,02 engineering and technology ,Dermatology ,endothelial dysfunction ,030207 dermatology & venereal diseases ,03 medical and health sciences ,0302 clinical medicine ,Fibrosis ,Edema ,lcsh:Dermatology ,medicine ,Genetic predisposition ,Immunology and Allergy ,Buttocks ,Endothelial dysfunction ,lcsh:RC31-1245 ,Cellulite ,Review Paper ,adiponectin ,business.industry ,lcsh:RL1-803 ,021001 nanoscience & nanotechnology ,medicine.disease ,body regions ,medicine.anatomical_structure ,hormonal disorders ,Lipodystrophy ,medicine.symptom ,0210 nano-technology ,business - Abstract
Cellulite (also known as gynoid lipodystrophy or orange peel syndrome) is one of the most common lipodystrophy syndromes, which affects millions of post-adolescent women. Cellulite is manifested by topographic disorders of subcutaneous tissue such as nodules, edema, and abnormal fibrosis. It is located mainly on the pelvic area, especially on the buttocks. Its pathogenesis is complexed and unclear. There are several theories about its pathophysiology. Hormonal disorders, endothelial dysfunction and genetic predispositions are taken under consideration.
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- 2017
30. Systemic sclerosis - diagnostic and therapeutic recommendations of the Polish Dermatological Society. Part 2 : treatment
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Anna Sysa-Jędrzejowska, Anna Woźniacka, Joanna Maj, Anna Wojas-Pelc, Slawomir Majewski, Aleksandra Dańczak-Pazdrowska, Lidia Rudnicka, Joanna Czuwara, Grażyna Chodorowska, Dorota Krasowska, and Anna Lis-Święty
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medicine.medical_specialty ,Cyclophosphamide ,business.industry ,Sildenafil ,sildenafil ,lcsh:R ,mycophenolate mofetil ,lcsh:Medicine ,Dermatology ,lcsh:RL1-803 ,medicine.disease ,Scleroderma ,methotrexate ,chemistry.chemical_compound ,alprostadil ,chemistry ,medicine ,lcsh:Dermatology ,Methotrexate ,cyclophosphamide ,scleroderma ,guidelines ,business ,medicine.drug - Abstract
Systemic sclerosis is an immune-mediated disease characterized by a chronic progressive course. The complex and diverse clinical features seen in patients require case-by-case approach and cooperation of multiple specialists both at the stage of diagnosis and treatment. Critical factors in systemic sclerosis include early diagnosis, assessment of internal organ involvement, identification of patients at potential risk of organ complications, assessment of disease dynamics and activity, and implementation of optimal therapy. Treatment decisions should be made individually for each patient after careful consideration of such aspects as the severity of skin lesions, duration and activity of the disease, manifestations and possible internal organ involvement. On account of potential organ dysfunctions, patients require a multidisciplinary therapeutic approach and coordinated treatment by experienced specialists or in specialist medical centres. Part 2 presents current guidelines for the treatment of systemic sclerosis.
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- 2017
31. The A/A genotype of an interleukin-17A polymorphism predisposes to increased severity of atopic dermatitis and coexistence with asthma
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A. Salinski, Paweł Majak, M. Wojtczak, Piotr Kuna, K. Przybylowska-Sygut, Anna Sysa-Jędrzejowska, Joanna Narbutt, Aleksandra Lesiak, and A. Zalińska
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Adult ,Male ,Adolescent ,Genotype ,Single-nucleotide polymorphism ,Dermatology ,Biology ,Polymorphism, Single Nucleotide ,Severity of Illness Index ,Dermatitis, Atopic ,Young Adult ,Gene Frequency ,medicine ,Humans ,SNP ,Genetic Predisposition to Disease ,Allele ,Child ,Allele frequency ,Alleles ,Incidence ,Interleukin-17 ,Case-control study ,Infant ,Receptors, Interleukin ,Atopic dermatitis ,medicine.disease ,Asthma ,Case-Control Studies ,Child, Preschool ,Immunology ,Female ,Poland ,Restriction fragment length polymorphism ,Polymorphism, Restriction Fragment Length - Abstract
Summary Introduction Studies have found that the interleukin-23/T helper 17 (IL-23/Th17) pathway plays an important role in the pathogenesis of atopic dermatitis (AD). Inhibition of the IL-23/Th17 pathway with monoclonal antibodies reduces skin inflammation in animal models. Aim To investigate the association between IL-17A and IL-23R gene single nucleotide polymorphisms (SNPs) and the development of AD in a Polish population. Methods Blood samples were collected from 166 patients with AD and 160 controls. We analyzed two SNPs, –152 G/A IL-17A and 1142 G/A IL-23R, using PCR and restriction fragment length polymorphism (RFLP) analysis. Results There was no statistically significant difference between the examined IL-17A SNP and the incidence of AD (P > 0.05 for all comparisons). Analysis of the IL-23R gene SNP showed no relationship between AD and the G/A genotype or presence of the A allele. The study did not establish any links between the IL-23R and IL-17A gene SNPs and the likelihood of developing AD resulting from gene–gene interaction. However, there was a significant relationship between the A/A genotype in the –152 G/A IL1-7A SNP and the coexistence of AD and asthma (P
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- 2014
32. Does inflammation play a role in development of necrobiosis lipoidica?
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Anna Sysa-Jędrzejowska, Iwona Słowik-Kwiatkowska, Joanna Narbutt, Anna Woźniacka, and Aleksandra Lesiak
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medicine.medical_specialty ,Angiogenesis ,lcsh:Medicine ,Dermatology ,Gastroenterology ,Necrobiosis lipoidica ,Pathogenesis ,chemistry.chemical_compound ,angiogenesis ,Internal medicine ,Diabetes mellitus ,medicine ,necrobiosis lipoidica ,lcsh:Dermatology ,Pathological ,business.industry ,Microangiopathy ,Therapeutic effect ,lcsh:R ,lcsh:RL1-803 ,medicine.disease ,Vascular endothelial growth factor ,chemistry ,inflammation ,TNF-α ,business - Abstract
Introduction. Necrobiosis lipoidica (NL) is a granulomatous skin disease of still only partially known pathogenesis. Microangiopathy is considered as one of the most important processes in NL, and vascular endothelial growth factor (VEGF) and endothelin-1 are strongly involved in it. Recent studies have demonstrated the beneficial therapeutic effect of tumor necrosis factor α (TNF-α) inhibitors in treatment of recalcitrant cases of NL, which is due to the important role of TNF-α in development of inflammation and granulomas in the course of NL. Objective. To assess the serum levels of VEGF, endothelin-1 and TNF-α in NL patients. Material and methods . The study group consisted of 17 patients with NL (mean age 48.22 ±15.99 years), 37 patients with diabetes mellitus (mean age 52.11 ±17.41 years) and 23 healthy volunteers (mean age 44.13 ±9.33 years) as a control group. Serum concentrations of TNF-α, VEGF and endothelin-1 were assessed in all patients with the ELISA test. Results. The TNF-α concentration was statistically lower in the controls when compared to the NL patients and diabetic patients (p 0.05 for all comparisons). Endothelin-1 serum values were under the tested values in most cases; however, statistically more frequently these values were found in the controls than in the NL group (p < 0.05). Conclusions. The results of our study suggest that inflammation with enhanced synthesis of TNF-α in NL patients is the primary pathological effect, followed by local impairment of angiogenesis.
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- 2014
33. / Method’s evaluation System for monitoring UV radiation level in phototherapy cabins in Poland
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Aleksandra Lesiak, Anna Sysa-Jędrzejowska, Janusz W. Krzyścin, Bonawentura Rajewska-Więch, Mariola Pawlaczyk, Joanna Narbutt, and Piotr Sobolewski
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Medical staff ,Radiation level ,business.industry ,Adverse health effect ,Primary standard ,medicine ,General Medicine ,Sunburn ,medicine.disease ,business ,Quality assurance ,Ultraviolet radiation ,Remote sensing - Abstract
Introduction Ultraviolet phototherapy (UVP) is widely used in dermatological practice for the treatment of various skin diseases. Numerous studies support its beneficial curing effectiveness; however, overexposure to ultraviolet radiation can cause adverse health effects, such as sunburn reaction, erythema response, cataract, skin aging, etc. For these reasons, it is of special importance to monitor performance of UVP cabins using a calibration system to evaluate the UV doses incident upon the patient. Material and methods A mechanized cabin control system (CCS) is proposed. It consists of radiometers with a wide and narrow field of view to estimate the body irradiation and to identify malfunctioning cabin tubes. Quality control and quality assurance procedures are developed to keep high accuracy of the calibration procedure. The CCS has been used in the examination of two different types of UVP cabins routinely working in Poland. Results It allows precise calculation of UV doses and spatial variability of UV radiance inside the cabin, thus providing uncertainties of the doses assigned by medical staff. The CCS could potentially serve as a primary standard for monitoring various UVP cabins working in Poland. Conclusions The methodology developed to quantify UV doses in UVP cabins may be easily extended to any UV radiation source.
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- 2014
34. Disturbed Balance between Serum Levels of Receptor Tyrosine Kinases Tie-1, Tie-2 and Angiopoietins in Systemic Sclerosis
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Elżbieta Dziankowska-Zaborszczyk, Bożena Dziankowska-Bartkowiak, Zofia Gerlicz, and Anna Sysa-Jędrzejowska
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Male ,medicine.medical_specialty ,Enzyme-Linked Immunosorbent Assay ,Dermatology ,Risk Assessment ,Sensitivity and Specificity ,Severity of Illness Index ,Statistics, Nonparametric ,Scleroderma ,Receptor tyrosine kinase ,Reference Values ,Internal medicine ,Severity of illness ,medicine ,Humans ,Esophagus ,Receptor ,Aged ,Analysis of Variance ,Scleroderma, Systemic ,biology ,Case-control study ,Angiopoietins ,Receptor, TIE-1 ,Middle Aged ,Prognosis ,medicine.disease ,Receptor, TIE-2 ,medicine.anatomical_structure ,Endocrinology ,Case-Control Studies ,biology.protein ,Female ,Analysis of variance ,Biomarkers - Abstract
Objective: The aim of this study was to determine the characteristic factors for vascular development and maintenance levels as well as correlation between Tie-1 receptors, Tie-2 receptors and the corresponding ligands - angiopoietins - in systemic sclerosis (SSc) patients. Materials and Methods: Serum levels of Tie-1, Tie-2, Ang-1 and Ang-2 were measured in 25 SSc patients and healthy controls. Results: There was a statistically significant difference in serum Tie-1 (p = 0.009) and Ang-2 (p = 0.001) levels in SSc patients compared with healthy controls. Significant correlations between Tie-1 and Tie-2 (ρ = 0.70, p = 0.0001) and between Tie-1 and Ang-2 (ρ = -0.92, p = 0.002) were found in the SSc group. Serum levels of Tie-2 were positively associated with esophagus changes (U = 2.03, p = 0.041) and Ang-1 was negatively correlated with duration of Raynaud's phenomenon (ρ = -0.75, p = 0.00008). Conclusion: The increase in serum concentration of Tie-1 and Ang-2 in patients with SSc may confirm a molecular imbalance between receptor tyrosine kinases Tie and their ligands.
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- 2014
35. Sonic hedgehog pathway dysregulation in skin basal-cell carcinoma of a Polish population
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Dorota Sobolewska-Sztychny, Aleksandra Lesiak, Anna Sysa-Jędrzejowska, Marian Danilewicz, Joanna Narbutt, Michał Sobjanek, Irmina Olejniczak-Staruch, and Michał Rogowski-Tylman
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Male ,Pathology ,medicine.medical_specialty ,Skin Neoplasms ,animal structures ,Histology ,Kruppel-Like Transcription Factors ,Zinc Finger Protein Gli2 ,Biology ,Receptors, G-Protein-Coupled ,Pathology and Forensic Medicine ,Pathogenesis ,GLI2 ,medicine ,Humans ,Hedgehog Proteins ,Basal cell carcinoma ,Sonic hedgehog ,integumentary system ,medicine.diagnostic_test ,Skin Basal Cell Carcinoma ,Nuclear Proteins ,General Medicine ,Middle Aged ,medicine.disease ,Smoothened Receptor ,Hedgehog signaling pathway ,Gene Expression Regulation, Neoplastic ,Carcinoma, Basal Cell ,Skin biopsy ,Sunlight ,biology.protein ,Female ,Poland - Abstract
Sonic hedgehog (Shh) pathway impairment plays a key role in the pathogenesis of basal-cell carcinomas (BCC), the most frequent skin tumor among Caucasians. Shh, Smo, and Gli2 family proteins are necessary for adequate and controlled cell proliferation. The aim of this study was to evaluate Shh, Smo, and Smo expression in BCC skin biopsies taken from sun-exposed areas. 41 BCC skin biopsies and 22 healthy skin specimens (the control group) taken from the same areas served as material for the study. All specimens were immunohistochemically stained with monoclonal antibodies directed against the chosen proteins. Shh and Smo expression (cytoplasmic pattern) were recorded semiquantitatively using a four-grade score (0-3). Gli2 expression (nuclear pattern) was determined using an image analysis system (semiautomatic function). The immunoexpression of the Shh and Smo proteins significantly increased in the BCC group, as compared with the normal controls (for Shh, the mean intensity was 1.67 in BCC vs. 1.17 in the control group, p < 0.001; for Smo, the mean intensity was 1.46 in BCC vs. 0.99 in the control group, p < 0.001). The staining for Gli2 in the BCC group was completely negative, but indicated the presence of Gli2 in the control patients (1.15 Gli2+ cells/100 cells). Sonic hedgehog pathway dysregulation may play an important role in skin cancerogenesis leading to BCC development.
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- 2013
36. Antinuclear antibodies in rosacea patients
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Małgorzata Salamon, Anna Sysa-Jędrzejowska, Anna Woźniacka, and Daniel P. McCauliffe
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musculoskeletal diseases ,medicine.medical_specialty ,Pathology ,Anti-nuclear antibody ,antinuclear antibodies ,Dermatology ,Immunofluorescence ,immune system diseases ,medicine ,Immunology and Allergy ,In patient ,skin and connective tissue diseases ,Original Paper ,Lupus erythematosus ,medicine.diagnostic_test ,biology ,business.industry ,medicine.disease ,rosacea ,stomatognathic diseases ,Titer ,Rosacea ,biology.protein ,Antibody ,business ,Inflammatory disorder - Abstract
Introduction Rosacea is a common inflammatory disorder, characterized by a spectrum of facial manifestations. The clinical similarity to other dermatoses, like lupus erythematosus, might lead to misdiagnosis, particularly in patients with elevated antinuclear antibody titers. Aim To assess the frequency, titer and specificity of antinuclear antibodies in rosacea patients and correlate these findings with clinical features. Material and methods The study included 101 rosacea patients and 26 sex- and age-matched controls. Immunofluorescence antinuclear antibody testing was performed on HEp-2 substrates. Patients’ sera with ANA titers of 1 : 160 or higher were evaluated by Euroline analysis. Results Over a half (53.5%) of rosacea patients had an ANA titer greater than or equal to 1 : 160. Within this group 13.86% had a titer of 1 : 320, 8.91% had a titer of 1 : 640, and 6.93% had a titer of 1 : 1,280 or higher. The specificity of these antibodies could not be identified. Elevated ANA titers were present more often in women (55.8%) than in men (44.15%). Only two of 26 healthy volunteers had elevated ANA titers. One had a titer of 1 : 160 and the other of 1 : 320. During a two-year observation period, after the initial ANA testing, none of the patients with ANA titers above 1 : 640 developed an apparent autoimmune disorder. Conclusions Elevated ANA titers are commonly found in rosacea patients, what with simultaneously existing facial erythema and photosensitivity might lead to misdiagnosis of lupus erythematosus. Clinicians should beware of these findings to avoid misdiagnosing lupus erythematosus in rosacea patients with elevated ANA titers.
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- 2013
37. Pathogenic activity of circulating anti-desmoglein-3 autoantibodies isolated from pemphigus vulgaris patients
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Anna Sysa-Jędrzejowska, Cezary Kowalewski, Joanna Boncela, Joanna Narbutt, Katarzyna Smolarczyk, Aleksandra Lesiak, Katarzyna Wozniak, Czeslaw S. Cierniewski, and Jolanta Dorota Torzecka
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education.field_of_study ,biology ,business.industry ,pemphigus vulgaris ,Acantholysis ,Pemphigus vulgaris ,apoptosis ,Autoantibody ,General Medicine ,keratinocyte culture ,medicine.disease ,Proinflammatory cytokine ,Pemphigus ,HaCaT ,Clinical Research ,Desmoglein 3 ,Immunology ,anti-Dsg-3 antibodies ,medicine ,biology.protein ,Antibody ,education ,business ,acantholysis - Abstract
INTRODUCTION: There are scarce data on immunochemical properties of pemphigus antibodies detected in clinical remission in pemphigus vulgaris (PV) patients. The aim of the study was to compare biological activity of anti-Dsg3 autoantibodies purified from the sera of PV patients in active stage and in clinical remission. MATERIAL AND METHODS: The effect of purified antibodies on expression of procaspase-3, Bax, Bcl-2, uPAR, IL-1β, IL-6, and TNF-α mRNAs in the HaCaT keratinocytes was evaluated by Western blot and RT-PCR method. RESULTS: Incubation of HaCaT cells with anti-Dsg-3 autoantibodies caused their binding to cell membranes surfaces. Anti-Dsg3 autoantibodies isolated from the patients in active stage and clinical remission showed proapoptotic effect, caused enhanced expression of analyzed proinflammatory cytokines' mRNAs and uPAR mRNA. CONCLUSIONS: Our data revealed similar pathogenic activity of anti Dsg-3 autoantibodies isolated from active and clinical remission PV patients.
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- 2012
38. [Skin diseases associated with hepatitis C virus]
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Iwona Walczak-Koszela, Anna Sysa-Jędrzejowska, and Anna Woźniacka
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Microbiology (medical) ,medicine.medical_specialty ,business.industry ,Chronic hepatic ,Hepatitis C virus ,lcsh:R ,lcsh:Medicine ,virus diseases ,Signs and symptoms ,Hepatitis C, Chronic ,medicine.disease ,medicine.disease_cause ,Skin Diseases ,digestive system diseases ,Pathogenesis ,Liver disease ,Infectious Diseases ,Hepatitis B, Chronic ,HCV ,Immunology ,Epidemiology ,Medicine ,Humans ,business ,choroby skóry - Abstract
Chronic hepatic diseases caused by HBV or HCV infection not always demonstrate evident clinical symptoms of liver disease. Non-specific extrahepatic symptoms mainly skin leasions are helpful for establishing the proper diagnosis. This review illustrates the pathogenesis, epidemiology and clinical manifestations of HBV and HCV infections with a special attention to skin signs and symptoms which can associate these infections.
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- 2015
39. Vitamin D serum level changes in psoriatic patients treated with narrowband ultraviolet B phototherapy are related to the season of the irradiation
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Mariola Pawlaczyk, Joanna Narbutt, Janusz W. Krzyścin, Anna Sysa-Jędrzejowska, and Aleksandra Lesiak
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medicine.medical_specialty ,Chemistry ,Immunology ,Human skin ,Dermatology ,General Medicine ,medicine.disease ,Solar irradiance ,medicine.disease_cause ,Effective dose (radiation) ,Narrowband ultraviolet B phototherapy ,Animal science ,Psoriasis ,medicine ,Vitamin D and neurology ,Immunology and Allergy ,Radiology, Nuclear Medicine and imaging ,Irradiation ,Ultraviolet - Abstract
Summary Background Vitamin D is produced in the human skin by short wavelength (290–315 nm) ultraviolet (UV) radiation. Purpose The aim of the study was to investigate how outdoor conditions may influence the serum levels of 25(OH) vitamin D in psoriasis patients under narrowband ultraviolet B (UVB) phototherapy. Methods The winter and summer groups of patients received almost the same narrowband UV (nUVB) doses during whole-body phototherapy. The 25(OH)D serum concentration was measured before and after two series of 10 exposures. The cabinet doses were compared with potentially available cumulative solar doses. The solar doses (unweighted UVB and vitamin D effective dose) and duration of solar intensity sufficient to produce vitamin D were calculated using a model based on local atmospheric data. Results After an initial 10 nUVB treatments, 25(OH)D serum concentration increased by 68% for winter patients in relation to the level before therapy, whereas a 20% increase was found for the summer patients. The next 10 treatments caused a much lower increase in 25(OH)D concentration: 5% and 3.5% for the winter and summer patients, respectively. No statistically significant relationship was observed between post-therapy 25(OH)D serum concentration and solar radiation variability. Conclusions The different baseline values of 25(OH)D serum levels in winter and summer patients result from seasonal variability in solar irradiance. Thus, outdoor solar radiation affects the patients over a much longer period, and artificial UV light is the main factor responsible for increase in 25(OH)D serum level over a 30-day period of cabinet therapy.
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- 2011
40. Repeated Suberythemal UVB Preexposure Protects against High-Dose UVB-Induced Expression of Vitamin D Receptor Protein in Human Skin
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Antony R. Young, Karolina Wódz, Rafał Pawliczak, Anna Sysa-Jędrzejowska, Aleksandra Lesiak, Joanna Narbutt, and Michał Rogowski-Tylman
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medicine.medical_specialty ,Calcitriol ,Erythema ,Human skin ,Cell Biology ,Dermatology ,Biology ,Calcitriol receptor ,Biochemistry ,Dose–response relationship ,Endocrinology ,Internal medicine ,medicine ,medicine.symptom ,skin and connective tissue diseases ,Receptor ,neoplasms ,Molecular Biology ,medicine.drug - Published
- 2011
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41. Photoprovocation in Cutaneous Lupus Erythematosus: A Multicenter Study Evaluating a Standardized Protocol
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Percy Lehmann, Cesar Calderon, Filippa Nyberg, Rainer Hügel, Adam Reich, Anna Wozniacka, Annegret Kuhn, Dick E. de Vries, Anna Sysa-Jędrzejowska, Jacek C Szepietowski, Merle Haust, Vilija Oke, and Regine Gläser
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Adult ,Male ,medicine.medical_specialty ,Adolescent ,Discoid lupus erythematosus ,Ultraviolet Rays ,Dermatology ,Biochemistry ,Subacute cutaneous lupus erythematosus ,Antimalarials ,Young Adult ,Lupus Erythematosus, Discoid ,Lupus Erythematosus, Cutaneous ,medicine ,Humans ,Photosensitivity Disorders ,Young adult ,skin and connective tissue diseases ,Molecular Biology ,Diagnostic Techniques and Procedures ,Aged ,Lupus erythematosus ,Clinical pathology ,business.industry ,Smoking ,Reproducibility of Results ,Dose-Response Relationship, Radiation ,Cell Biology ,Middle Aged ,medicine.disease ,Lupus Erythematosus Tumidus ,Clinical trial ,Cutaneous Lupus Erythematosus ,Female ,business - Abstract
Photosensitivity is an important and distinguishing sign in various subtypes of cutaneous lupus erythematosus (CLE); however, it remains poorly defined. The purpose of this study was to evaluate whether standardized photoprovocation is a reproducible method to assess photosensitivity in subjects with CLE. A total of 47 subjects with CLE (subacute cutaneous lupus erythematosus (SCLE), n=14; discoid lupus erythematosus (DLE), n=20; lupus erythematosus tumidus (LET), n=13) and 13 healthy volunteers underwent photoprovocation at seven European sites. Of these, 22 (47%) subjects (57% SCLE, 35% DLE, and 54% LET) and none of the healthy volunteers developed photoprovoked lesions according to clinical analysis. Of these 22 subjects, 19 (86%) developed lesions that were histopathologically confirmed as specific for lupus erythematosus (LE). In CLE subjects who developed UV-induced lesions, 86% had Fitzpatrick's phototypes I or II, and the mean minimal erythema dose (MED) was significantly lower compared with subjects without UV-induced lesions (P=0.004). No significant differences in photoprovocation results were observed between study sites. Safety parameters showed no clinically meaningful differences between CLE subjects and healthy volunteers after photoprovocation. In conclusion, a standardized, safe, and reproducible protocol for photoprovocation using UVA and UVB radiation induced skin lesions in approximately half of all CLE subjects and showed comparable results across multiple sites. This method may therefore be used for future diagnostic testing and clinical trials.
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- 2011
42. An enhanced risk of basal cell carcinoma is associated with particular polymorphisms in the VDR and MTHFR genes
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Joanna Narbutt, Aleksandra Lesiak, Karolina Wódz-Naskiewicz, Michał Rogowski-Tylman, Rafał Pawliczak, Michał Sobjanek, Mary Norval, Anna Sysa-Jędrzejowska, and Adam Włodarkiewicz
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medicine.medical_specialty ,integumentary system ,biology ,TaqI ,business.industry ,Dermatology ,medicine.disease_cause ,medicine.disease ,Biochemistry ,Calcitriol receptor ,digestive system diseases ,FokI ,chemistry.chemical_compound ,Endocrinology ,chemistry ,Internal medicine ,Methylenetetrahydrofolate reductase ,Genotype ,medicine ,biology.protein ,Vitamin D and neurology ,Basal cell carcinoma ,Carcinogenesis ,business ,Molecular Biology - Abstract
Background: Vitamin D and folate are influenced by ultraviolet radiation (UVR), and both are implicated in skin carcinogenesis. Polymorphisms in the genes involved in the metabolism of these two compounds may alter the risk of basal cell carcinoma (BCC). Objective: To assess the frequency of four polymorphisms in the gene encoding the vitamin D receptor (VDR) (FokI, BsmI, TaqI and ApaI) and two in the gene encoding methylenetetrahydrofolate reductase (MTHFR) (677C/T and 1286A/C) in 142 patients of Polish origin with BCC and the same number of controls. The expression of VDR and MTHFR proteins in the skin, and the vitamin D status of a subset of patients and controls were also measured. Patients/Methods: The polymorphisms were assayed by PCR-RFLP, the VDR and MTHFR proteins by immunoblotting and vitamin D status as 25-hydroxyvitamin D (25(OH)D) level in the serum by RIA. Results: The presence of the TT genotype in the FokI VDR polymorphism resulted in a >10-fold higher risk of BCC development. The CT genotype in 677C/T MTHFR polymorphism and CC genotype in 1286A/C MTHFR polymorphism also significantly increased the risk of BCC development. The expression of the VDR and MTHFR proteins was significantly higher in BCCs of the patients than in the healthy skin of the controls. The median serum level of 25(OH)D was significantly higher in the control group compared with the patients with BCC. Conclusions: Certain VDR and MTHFR gene polymorphisms increase the risk of BCC development in individuals of Polish origin.
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- 2011
43. Combination therapy with adapalene-benzoyl peroxide and oral lymecycline in the treatment of moderate to severe acne vulgaris: a multicentre, randomized, double-blind controlled study
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Vincenzo Bettoli, F. Paliargues, M. Gómez-Flores, M. Berg, Brigitte Dréno, Peter Foley, M.A. Rodríguez-Castellanos, S. Talarico, N. Kerrouche, Roland Kaufmann, J. De Maubeuge, Anna Sysa-Jędrzejowska, and V. Torres Lozada
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medicine.medical_specialty ,business.industry ,Adapalene/benzoyl peroxide ,Fixed-dose combination ,Dermatology ,Benzoyl peroxide ,medicine.disease ,Tolerability ,Adapalene ,Lymecycline ,medicine ,business ,Acne ,medicine.drug ,Antibacterial agent - Abstract
BACKGROUND: Oral antibiotics in association with a topical retinoid with or without benzoyl peroxide (BPO) are the recommended first-line option in the treatment of moderate to severe acne vulgaris. OBJECTIVES: To evaluate the efficacy and safety of oral lymecycline 300 mg with adapalene 0·1%-BPO 2·5% (A/BPO) fixed-dose gel in comparison with oral lymecycline 300 mg with a vehicle gel in subjects with moderate to severe acne vulgaris. METHODS: A total of 378 subjects were randomized in a double-blind, controlled trial to receive once-daily lymecycline with either A/BPO or vehicle for 12 weeks. Evaluations included percentage changes from baseline in lesion counts, success rate (subjects 'clear' or 'almost clear'), skin tolerability, adverse events and patients' satisfaction. RESULTS: The median percentage reduction from baseline in total lesion counts at week 12 was significantly higher (P < 0·001) in the lymecycline with A/BPO group (-74·1%) than in the lymecycline with vehicle group (-56·8%). The success rate was significantly higher (47·6% vs. 33·7%, P = 0·002) in subjects treated with lymecycline and A/BPO. Both inflammatory and noninflammatory lesions were significantly reduced at week 12 (both P < 0·001) with a rapid onset of action from week 2 for noninflammatory lesions (P < 0·001) and week 4 for inflammatory lesions (P = 0·005). The A/BPO and lymecycline combination was well tolerated. The proportion of satisfied and very satisfied subjects was similar in both groups, but the number in the A/BPO group who were 'very satisfied' was significantly greater (P = 0·031). CONCLUSION: These results demonstrate the clinical benefit of combining A/BPO with lymecycline in the treatment of moderate to severe acne vulgaris.
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- 2011
44. Combined occurrence of filaggrin mutations and IL-10 or IL-13 polymorphisms predisposes to atopic dermatitis
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Tomasz Hawro, Reno S. Bladergroen, Karolina Przybyłowska, Michael van Geel, Joanna Narbutt, Anna Sysa-Jędrzejowska, Paweł Majak, Iwona Stelmach, Aleksandra Lesiak, Marcin Zakrzewski, and Piotr Kuna
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Allergy ,business.industry ,Genome-wide association study ,Dermatology ,Atopic dermatitis ,medicine.disease ,Biochemistry ,Allergic inflammation ,Atopy ,Genotype ,Interleukin 13 ,Immunology ,Medicine ,business ,Molecular Biology ,Filaggrin - Abstract
Background: Although filaggrin mutations are presently believed to play a key role in the development of atopic dermatitis (AD), obviously also immunological factors involved in acquired immune response are important for the development of allergic inflammation. Objective: To assess the frequency of FLG mutations and the polymorphisms 590 C/T in the IL-4 gene, -1082A/G in the IL-10 gene and -1055C/T in the IL-13 gene in patients with AD and their correlations between severity of AD and asthma. Methods: R501X and 2282del4 FLG mutations and IL-4, IL-10 and IL-13 polymorphisms were assayed in 163 patients with AD of Polish origin. Results: In the Polish patients with AD, the prevalence of FLG mutations was higher in patients with AD than in the controls and 2282del4 FLG mutation was more frequent than R501X, and it was associated with a 6-fold higher risk for AD development (P
- Published
- 2011
45. Quality of life and satisfaction with life in SLE patients—the importance of clinical manifestations
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Anna Sysa-Jędrzejowska, Ewa Robak, and Lilianna Kulczycka
- Subjects
Quality of life ,Adult ,Male ,medicine.medical_specialty ,SF-36 ,SLE ,Personal Satisfaction ,Short form 36 ,Disease ,SWLS ,Severity of Illness Index ,Rheumatology ,Internal medicine ,Severity of illness ,medicine ,Humans ,Lupus Erythematosus, Systemic ,Photosensitivity Disorders ,Aged ,Lupus erythematosus ,business.industry ,General Medicine ,Middle Aged ,medicine.disease ,Health Surveys ,humanities ,Clinical manifestations ,Photosensitivity Disorder ,Physical therapy ,Original Article ,Female ,Nervous System Diseases ,business ,Satisfaction with life - Abstract
To assess the correlation between quality of life (QoL) and satisfaction with life (SL) in SLE patients and correlate both with clinical symptoms of the disease. The study was performed in 83 patients. QoL was assessed by Short Form 36, and SL was assessed by the Satisfaction with Life Scale. Clinical manifestations presented at the time of examination were taken into consideration. SLE patients assessed their QoL and SL as rather low. Those with photosensitivity as well as neurological symptoms presented lower QoL in particular domains, while those with renal manifestation of SLE assessed their QoL as higher. Similar observations were made for SL only in relation to neurological symptoms. Moreover, our findings show that although SL is a part of QoL, both these parameters should be distinguished in order to fully assess the state of the patient.
- Published
- 2010
46. Effect of chloroquine phosphate treatment on serum MMP-9 and TIMP-1 levels in patients with systemic lupus erythematosus
- Author
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Jolanta Lukamowicz, Aleksandra Lesiak, Joanna Narbutt, Anna Wozniacka, Anna Sysa-Jędrzejowska, and Daniel P. McCauliffe
- Subjects
Adult ,Male ,Pharmacology ,Matrix metalloproteinase ,Antimalarials ,Immune system ,Rheumatology ,Chloroquine ,Healthy volunteers ,Animals ,Humans ,Lupus Erythematosus, Systemic ,Medicine ,In patient ,skin and connective tissue diseases ,Tissue Inhibitor of Metalloproteinase-1 ,Lupus erythematosus ,business.industry ,Anti-Inflammatory Agents, Non-Steroidal ,Drug administration ,Middle Aged ,medicine.disease ,Chloroquine Phosphate ,Treatment Outcome ,Matrix Metalloproteinase 9 ,Female ,business ,medicine.drug - Abstract
Antimalarials are widely used for the treatment of systemic lupus erythematosus. However, their mechanisms of action have not been fully elucidated. Literature data indicate that matrix metalloproteinases may play a role in the immune response and tissue damage that occur in autoimmune skin diseases. The aim of this study was to determine the effect of 3 months of chloroquine treatment on serum levels of MMP-9 and TIMP-1 in patients with systemic lupus erythematosus. The study group consisted of 25 patients with systemic lupus erythematosus and 25 sex- and age-matched healthy volunteers. Before drug administration, serum levels of MMP-9 and TIMP-1 were determined by enzyme-linked immunosorbent assay. The same procedure was performed after chloroquine treatment. We found significantly higher median serum levels of MMP-9 in patients with systemic lupus erythematosus before therapy (57.20 ng/ml) when compared with controls (44.50 ng/ml) (p < 0.001). After chloroquine therapy the median MMP-9 serum level of systemic lupus erythematosus patients decreased significantly (43 ng/ml; p < 0.001). Before treatment the median TIMP-1 serum level in the patients with systemic lupus erythematosus was significantly higher than in the control group (500 vs. 200 ng/ml; p < 0.001), and after therapy it increased significantly (750 ng/ml TIMP-1; p < 0.001). The results suggest that chloroquine treatment may affect the matrix metalloproteinase network, and this effect may contribute to the immunoregulatory and anti-inflammatory properties of antimalarials.
- Published
- 2010
47. Persistent Improvement of Previously Recalcitrant Hailey-Hailey Disease with Electron Beam Radiotherapy
- Author
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Joanna Narbutt, Anna Chrusciel, Anna Rychter, Aleksandra Lesiak, Anna Sysa-Jędrzejowska, and Jacek Fijuth
- Subjects
Male ,medicine.medical_specialty ,Time Factors ,Pemphigus, Benign Familial ,Biopsy ,medicine.medical_treatment ,Dermatology ,Disease ,Recurrence ,medicine ,Humans ,Skin ,medicine.diagnostic_test ,business.industry ,Genodermatosis ,Dose fractionation ,General Medicine ,Middle Aged ,medicine.disease ,Radiation therapy ,Pemphigus ,Axilla ,Treatment Outcome ,medicine.anatomical_structure ,Hailey–Hailey disease ,Female ,Dose Fractionation, Radiation ,business - Abstract
Hailey-Hailey disease, or familial benign chronic pemphigus, is an autosomal dominant genodermatosis. Disease symptoms may contribute to an adverse impact on quality of life and functional limitation and disability. As Hailey-Hailey disease is chronic and frequently recalcitrant to treatment, multiple therapeutic approaches, including surgical options, have been attempted. We describe here three cases of recalcitrant Hailey-Hailey disease that showed long-term improvement with radiotherapy. Axillary lesions were treated with electron beam at an anti-inflammatory dose (energy 6-8 MeV). Patients received 20 Gy in 10 fractions to 90% isodose, at each axilla. No disease recurrence was observed during a 38 months follow-up of the treated sites. The effect of radiotherapy was thus considered to be locally beneficial, but without any positive influence on the general course of the disease.
- Published
- 2010
48. The influence of treatment on quality of life in systemic lupus erythematosus patients
- Author
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Lilianna Kulczycka, Ewa Robak, and Anna Sysa-Jędrzejowska
- Subjects
Autoimmune disease ,medicine.medical_specialty ,Lupus erythematosus ,business.industry ,MEDLINE ,Dermatology ,medicine.disease ,Affect (psychology) ,Infectious Diseases ,Quality of life (healthcare) ,Pharmacotherapy ,medicine ,Physical therapy ,Intensive care medicine ,business ,Socioeconomic status ,Social functioning - Abstract
Objective Systemic lupus erythematosus is an autoimmune disease with uncertain prognosis as to the course. The patients need pharmacotherapy all their life. The main aim of this study was to determinate the impact of therapeutic schedules on patients’ quality of life. Methods The study was performed on 83 patients who were divided into five groups according to methods of treatment used. Quality of life was measured using MOS SF-36. Results Obtained results revealed that therapeutic schedules have the highest influence on patients’ social functioning. The more medicaments the patients use, the lower their quality of life. Conclusions The type of medicaments and therapeutic schemes adopted affect the patients’ quality of life. Nevertheless, quality of life and the patients’ attitude to it are very subjective and are also influenced by the clinical state of the patients as well as many other factors such as socioeconomic and demographic.
- Published
- 2010
49. Chronic mucocutaneous candidiasis with endocrinopathy –
- Author
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Anna Sysa-Jędrzejowska, Joanna Narbutt, Bożena Dziankowska-Bartkowiak, Anna Erkiert-Polguj, and Aleksandra Lesiak
- Subjects
Pathology ,medicine.medical_specialty ,integumentary system ,biology ,business.industry ,Mucosal lesions ,Mucous membrane ,General Medicine ,medicine.disease ,biology.organism_classification ,medicine.anatomical_structure ,Granuloma ,Scalp ,Diabetes mellitus ,medicine ,Chronic mucocutaneous candidiasis ,business ,Candida albicans ,Blepharitis - Abstract
Chronic mucocutaneous candidiasis (CMC) is characterized by Candida infection of the mucous membrane, scalp, skin and nails. We present a case of a 42-year-old man who was treated twice in the Dermatological Department. He was admitted the first time as a 7-year-old boy because of skin and mucosal lesions and then the diagnosis of granuloma candidamyceticum was established. Thirty-one years later he was admitted again with a history of facial skin lesions and blepharitis. For a couple of years he had suffered from diabetes and hypothyroidism. The diagnosis of CMC with endocrinopathy was established in our patient.
- Published
- 2010
50. Systematic administration of chloroquine in discoid lupus erythematosus reduces skin lesions via inhibition of angiogenesis
- Author
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Joanna Narbutt, Radzisław Kordek, Anna Sysa-Jędrzejowska, Mary Norval, Józef Kobos, Aleksandra Lesiak, and Anna Wozniacka
- Subjects
Adult ,Male ,Vascular Endothelial Growth Factor A ,Pathology ,medicine.medical_specialty ,Discoid lupus erythematosus ,Angiogenesis ,Angiogenesis Inhibitors ,Antigens, CD34 ,Dermatology ,Neovascularization ,Young Adult ,chemistry.chemical_compound ,Lupus Erythematosus, Discoid ,Dermis ,Chloroquine ,medicine ,Humans ,Skin ,Lupus erythematosus ,Neovascularization, Pathologic ,integumentary system ,medicine.diagnostic_test ,business.industry ,Middle Aged ,medicine.disease ,Vascular endothelial growth factor ,medicine.anatomical_structure ,chemistry ,Skin biopsy ,Female ,medicine.symptom ,business ,medicine.drug - Abstract
Summary Background. Discoid lupus erythematosus (DLE) is a chronic cutaneous form of lupus erythematosus, characterized by inflammation and scarring skin lesions, with lymphocyte infiltration and vasodilation. Antimalarial drugs have beneficial therapeutic effects in DLE, partially resulting from their immunomodulating and photoprotective properties. The possible influence of these drugs on angiogenesis has not been previously evaluated. Aims. To investigate the impact of chloroquine (CQ) treatment on the expression of vascular endothelial growth factor (VEGF, a major regulator of angiogenesis) and CD34 (a transmembrane glycoprotein expressed on endothelial cells and involved in tethering lymphocytes) in patients with DLE. Methods. A 3-mm skin biopsy was taken from typical skin lesions in 10 people with DLE. Another biopsy was taken from the same area after 3 months of treatment with CQ (250 mg/day). Skin sections were stained with monoclonal antibodies directed against VEGF and CD34. The intensity of epidermal VEGF expression, and the number and area of CD34-positive dermal blood vessels were assessed. Results. CQ treatment induced a reduction in epidermal VEGF expression. It also resulted in a significant decrease in the median number of CD34+ dermal blood vessels (from 219 to 125 vessels per mm2). Furthermore the median vessel area was significantly lowered from 9.76 × 106 to 6.92 × 106 mm2 per mm2 of the dermis. Conclusions. These results indicate that one beneficial effect of CQ treatment in DLE may be due to its antiangiogenic properties.
- Published
- 2009
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