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İşeme Disfonksiyonu Olan Çocuk Hastalarda Transkütanöz Posterior Tibial Sinir Stimülasyonunun Etkinliği

dc.contributor.advisorDoğan, Hasan Serkan
dc.contributor.authorJafarov, Ruslan
dc.date.accessioned2019-03-04T08:24:32Z
dc.date.issued2019-02-02
dc.date.submitted2019-01-16
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dc.identifier.urihttp://hdl.handle.net/11655/6035
dc.description.abstractNon-pharmacological, pharmacological and invasive treatment methods are used for the treatment of children with voiding dysfunction and non-invasive and invasive methods are used in the diagnosis and follow-up of these patients. At the same time, the search for new diagnostic, treatment and follow-up methods continues. Percutaneous posterior tibial nerve stimulation (PPTNS) is one of the recommended treatment modalities in these patients. There are few studies in the literature to show the role of urine biomarkers in diagnosis and follow-up. Few studies have shown the potential benefits of NGF (nerve growth factor), TGF-beta 1 (transforming growth factor-beta 1), TIMP-2 (tissue inhibitor of metalloproteinases 2). Thus a prospective randomized, controlled study was planned to demonstrate the efficacy of transcutaneous posterior tibial nerve stimulation (TPTNS), which is a less invasive and therefore more tolerable method and to assess the role of urinary biomarkers (NGF, TGF-beta 1, TIMP-2) in the diagnosis and follow-up of children with voiding dysfunction. For this purpose, children between 6-15 years old who stopped treatment due to side effects and who were resistant to medical treatment between 01.2018-09.2018 were included to our study. Patients were divided into two goups; test (N=20) and sham (N=10) group by closed envelope method. TPTNS therapy was applied to the test group for 12 weeks, in 30 minute sessions once a week by stimulation given at certain dose intervals. The same procedure was applied to the sham group without any stimulation. Urine biomarkers, dysfunctional voiding and incontinence scoring system (DVISS), voiding diary, urodynamic or uroflowmetry tests were applied to both groups before and after treatment. In addition, to 14 healthy children without urinary complaints DVISS scores and urine biomarkers were evaluated for control group. In the test group, the frequency of urgency after treatment (p < 0.001), daytime incontinence episodes (p < 0.006), general DVISS scores (p < 0.001), daytime DVISS scores (p < 0.001) and quality of life score (p = 0.019) were significantly decreased. There were also significant decreases in general DVISS scores (p = 0.007), daytime DVISS scores (p = 0.005) and quality of life scores (p = 0.040) in the sham group. There was no difference between NGF (p = 0.199), TGF-beta 1 (p = 0.480), and TIMP-2 (p = 0.940) levels of patient and healthy volunteers group before treatment. Neither the NGF, TGF-beta 1, TIMP-2 levels in the test group (p = 0.250; 0.850; 0.460, respectively) nor the NGF, TGF-beta 1, TIMP-2 levels in the sham group (p = 0.580; 0.580; 0.650, respectively) changed significantly with the treatment. In our study, it was observed that TPTNS treatment provides significant improvement in some parameters of pediatric patients with voiding dysfunction. These findings support that TPTNS has a role in the treatment of pediatric patient group who does not respond to standard medical treatment. The benefit of TPTNS to the aforementioned patient group is observed especially in daytime symptoms. Further studies with greater number of patients are needed on this issue. According to our findings, urine biomarkers (NGF, TGF-beta1, TIMP-2) are not useful for diagnosis and follow-up of these patients.tr_TR
dc.description.sponsorshipHacettepe Üniversitesi Bilimsel Araştırmalar Koordinasyon Birimitr_TR
dc.description.tableofcontentsİÇİNDEKİLER TEŞEKKÜR ii ÖZET iii ABSTRACT iv İÇİNDEKİLER v KISALTMALAR viii ŞEKİLLER DİZİNİ xi TABLOLAR DİZİNİ xii 1. GİRİŞ 1 1.1. Amaç 1 1.2. Hipotez 2 2. GENEL BİLGİLER 3 2.1. Mesane ve Sfinkter Kontrolünün Normal Gelişimi 3 2.2. Normal Değerler 5 2.3. İnkontinan Çocuklarda Değerlendirme 6 2.3.1. Alt Üriner Sistem Semptomları 6 2.3.1.1. İdrarın depolanması ile ilgili semptomlar 6 2.3.1.2. İdrarın boşaltılması ile ilgili semptomlar 7 2.1.1.3. İşeme sonrası ile ilgili semptomlar 8 2.3.2. Hikâye Alma 8 2.3.3. Fizik Muayene 9 2.3.4. İdrar Analizi 10 2.3.5. İdrar Biyobelirteçleri 10 2.3.6. Non-İnvaziv Teknikler 12 2.3.7. İdrar Kaçırma Miktarının Hesaplanması 14 2.3.8. İdrar Akışı 14 2.3.9. Alt ve Üst Üriner Sistemin Ultrason Görüntülemesi 17 2.3.10. İnvaziv Diyagnostik Teknikler 18 2.3.10.1. İşeme sistoüretrografisi (İSUG) 18 2.3.10.2. Videoürodinami (VUD) 19 2.4. Gece ve Gündüz İnkontinansı Olan Çocuklar (Fonksiyonel İşeme Bozuklukları) 22 2.4.1. Prevalans 22 2.4.2. Klinik Değerlendirme 22 2.4.3. Sınıflandırma 23 2.4.3.1. Çocuklarda aşırı aktif mesane 24 2.4.3.2. Disfonksiyonel işeme 26 2.4.3.3. Detrüsör azalmış aktivitesi 27 2.4.3.4. İşemenin ertelenmesi 28 2.4.3.5. Giggle inkontinans (kıkırdama inkontinansı) 28 2.4.3.6. Vezikovajinal tuzak (vaginal reflü) 29 2.4.3.7. Mesane ve bağırsak disfonksiyonu (MBD) 29 2.4.4. Non-Farmakolojik Tedavi İlkeleri 30 2.4.4.1. Mesane rehabilitasyonu ve üroterapi 31 2.4.4.2. Biofeedback tedavisi 32 2.4.4.3. Temiz aralıklı kateterizasyon 32 2.4.4.4. Nörostimulasyon 32 2.4.4.5. Alarm tedavisi 34 2.4.5. Farmakolojik Tedavi 35 2.4.5.1. Antimuskarinik tedavi 35 2.4.5.1.1. Oksibutinin 36 2.4.5.1.2. Propiverin 36 2.4.5.2. Botulinum toksini 37 3. GEREÇ VE YÖNTEM 39 3.1. Yöntem 39 3.2. İstatistik 43 4. BULGULAR 44 4.1. Tedavi Öncesi Hasta Özellikleri 44 4.1.1. Ek Hastalıklar ve Cerrahi Öyküsü 47 4.2. Tedaviden Sonra Test Grubundaki Hastalarda Olan Değişimler 48 4.3. Tedaviden Sonra Sham Grubundaki Hastalarda Olan Değişimler 51 4.4. Test ve Sham Gruplarının Tedaviden Fayda Görme Oranlarının Karşılaştırılması 53 4.5. Test ve Sham Grubundaki Hastalarda Tedavi Sürecinde Klinik Yanıtın Başlama Haftaları 56 4.6. Test ve Sham Grubunda Tedavi Sonrasında Gözlenen Üroflovmetrik Patern Değişimleri 57 5. TARTIŞMA 59 5.1. Genel 59 5.2. Cinsiyet ve Yaş Özellikleri 60 5.3. İdrar Yolu Enfeksiyonu Öyküsü, Kabızlık Durumu ve Mesane Duvar Kalınlıkları 60 5.4. İBSS Bazında Değişimler 61 5.5. Sıkışma ve İdrar Kaçırma Sıklığındaki Değişimler 63 5.6. Ürodinamik Parametrelerdeki Değişimler 64 5.7. Üroflovmetrik Parametrelerdeki Değişimler 66 5.8. Test ve Sham Grubundaki Hastaların Tedaviden Fayda Görme Oranları 68 5.9. Tedavinin Uygulama Dozları, Yanıt Başlama Haftaları, Yan Etkileri ve Uzun Dönem Takip Sonuçları 70 5.10. İdrar Biyobelirteçlerinin Test, Sham ve Kontrol Gruplarında Özellikleri 71 5.11. Çalışmanın Özgün Yönleri 72 5.12. Çalışmanın Kısıtlılıkları 73 6. SONUÇ 74 7. KAYNAKLAR 76 EKLER 87tr_TR
dc.language.isoturtr_TR
dc.publisherTıp Fakültesitr_TR
dc.rightsinfo:eu-repo/semantics/openAccesstr_TR
dc.subjectİşeme disfonksiyonutr_TR
dc.subjectTranskütanöz posterior tibial sinir stimülasyonu
dc.subjectİdrar biyobelirteçleri
dc.subjectSinir büyüme faktörü (NGF)
dc.subjectTransforme edici büyüme faktörü-beta 1 (TGF-beta 1)
dc.subjectMetalloproteinazların doku inhibitörü 2 (TIMP-2)
dc.titleİşeme Disfonksiyonu Olan Çocuk Hastalarda Transkütanöz Posterior Tibial Sinir Stimülasyonunun Etkinliğitr_TR
dc.typeinfo:eu-repo/semantics/doctoralThesistr_TR
dc.description.ozetGünümüzde işeme disfonksiyonu olan çocuk hastaların tedavisi için non-farmakolojik, farmakolojik ve invaziv tedavi yöntemleri uygulanmakta, bu hastaların tanı ve takibinde de non-invaziv ve invaziv yöntemler kullanılmaktadır. Aynı zamanda yeni tanı, tedavi ve takip yöntemlerinin arayışı sürmektedir. Medikal tedaviye dirençli olgularda perkütan posterior tibial sinir stimülasyonu (PPTSS) bu hastalarda önerilen tedavi yöntemlerinden biridir. Literatürde tanı ve takip amaçlı idrar biyobelirteçlerinin rolünü göstermeye yönelik yapılmış ve NGF (Sinir büyüme faktörü), TGF-beta 1 (Transforme edici büyüme faktörü-beta 1), TIMP-2’nin (Metalloproteinazların doku inhibitörü 2) potansiyel yararlarını ortaya koymuş olan az sayıda çalışma mevcuttur. Bu nedenlerle işeme disfonksiyonlu çocuk hastalarda daha az invaziv ve dolayısıyla daha çok tolere edilebilir bir yöntem olan transkütanöz posterior tibial sinir stimülasyonunun (TPTSS) tedavide etkinliğini, idrar biyobelirteçlerinin (NGF, TGF-beta 1, TIMP-2) tanı ve takipte rolünü göstermek amaçlı prospektif, randomize, kontrollü bir çalışma planlanmıştır. Bu amaçla 01.2018-09.2018 tarihleri arasında kliniğimize başvuran medikal tedaviye dirençli ve yan etki nedeniyle tedaviyi bırakmış olan 6-15 yaş arası çocuk hastalar çalışmaya dahil edilmiştir. Hastalar, kapalı zarf yöntemiyle test (N=20) ve sham (N=10) gruplarına ayrılıp test grubuna 12 hafta, haftada 1 kez, 30 dakikalık seanslarla, belli doz aralıklarında uyarı vererek TPTSS tedavisi uygulanmış ve sham grubuna da uyaran verilmeden aynı prosedür uygulanmıştır. Her iki gruba tedavi öncesi ve sonrasında idrar biyobelirteçleri, işeme bozukluğu semptom skoru (İBSS), işeme günlüğü, ürodinami veya üroflovmetri testleri uygulandı. Bunun dışında idrar şikayetleri açısından sağlıklı 14 çocukta bir defaya mahsus İBSS ve idrar biyobelirteçleri bakıldı. Test grubunda tedavi sonrasında sıkışma sıklığı (p<0,001), gündüz inkontinans epizotları (p<0,006), genel İBSS skorları (p<0,001), gündüz İBSS skorları (p<0,001) ve hayat kalitesi skorunda (p=0,019) anlamlı azalma gözlendi. Sham grubunda da genel İBSS skorları (p=0,007), gündüz İBSS skorları (p=0,005) ve hayat kalitesi skorlarında (p=0,040) anlamlı azalma vardı. Tedaviden önce hasta ve sağlıklı grupta bakılan NGF (p=0,199), TGF-beta 1 (p=0,480), TIMP-2 (p=0,940) düzeyleri arasında fark yoktu. Tedavi başı ve sonunda test grubunda NGF, TGF-beta 1, TIMP-2 (sırasıyla p=0,250; 0,850; 0,460) ve sham grubunda NGF, TGF-beta 1, TIMP-2 (sırasıyla p=0,580; 0,580; 0,650) biyobelirteç düzeyi değişimi anlamlı değildi. Çalışmada TPTSS tedavisinin işeme disfonksiyonu olan çocuk hastalarda bazı parametrelerde anlamlı düzelme sağladığı gözlemlendi. Bu bulgular, standart medikal tedaviye cevap vermeyen çocuk hasta grubunda TPTSS’nin yeri olduğunu desteklemektedir. Bahsi geçen hasta grubunda fayda özellikle gündüz semptomlarında görülmektedir. Bu konuda daha fazla hasta sayısı ile yapılacak çalışmalara ihtiyaç vardır. Bizim bulgularımıza göre idrar biyobelirteçleri (NGF, TGF-beta1, TIMP-2) bu grup hastaların tanı ve takibinde katkı sağlamamaktadır.tr_TR
dc.contributor.departmentÜrolojitr_TR
dc.embargo.termsAcik erisimtr_TR
dc.subtypemedicineThesis


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