1.Correction of a maxillary canine-first premolar transposition using mini-implant anchorage.
Mehmet Oguz OZTOPRAK ; Cigdem DEMIRCAN ; Tulin ARUN
Korean Journal of Orthodontics 2011;41(5):371-378
Transposition is defined as a dental anomaly manifested by a positional interchange of 2 adjacent teeth within the same quadrant of the dental arch. Maxillary canine-first premolar [Mx4-3] transposition is the most frequent tooth transposition reported in the literature. In this case report, an orthodontic correction of a transposition of the maxillary left canine and first premolar with the help of palatally located mini-implant anchorage is described. Esthetic and occlusal evaluations suggested alignment of the transposed teeth to their correct anatomic positions in the dental arch. The clinical result at the end of the treatment was satisfactory. Alignment was obtained, and intercuspation was adequate. Nevertheless, the maxillary canine showed facial recession, probably because it was initially positioned buccally. Supporting tissue was examined after treatment and no alveolar bone damage was observed.
Bicuspid
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Dental Arch
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Tooth
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Tooth Movement
2.Lumbar Disc Herniation in a Patient With Congenital Vertebral Body Anomaly: A Case Report.
Cem ATABEY ; Ahmet EROGLU ; Ali Kivanc TOPUZ ; Murat VELIOGLU ; Mehmet Nusret DEMIRCAN
Korean Journal of Spine 2014;11(4):245-248
Lumbar disc herniation is characterized with low back and leg pain resulting from the degenerated lumbar disc compressing the spinal nerve root. The etiology of degenerative spine is related to age, smoking, microtrauma, obesity, disorders of familial collagen structure, occupational and sports-related physical activity. However, disc herniations induced by congenital lumbar vertebral anomalies are rarely seen. Vertebral fusion defect is one of the causes of congenital anomalies. The pathogenesis of embryological corpus vertebral fusion anomaly is not fully known. In this paper, a 30-year-old patient who had the complaints of low back and right leg pain after falling from a height is presented. She had right L5-S1 disc herniation that had developed on the basis of S1 vertebra corpus fusion anomaly in Lumbar computed tomography. This case has been discussed in the light of literature based on evaluations of Lumbar Computed Tomography (CT) and Magnetic Resonance Imaging (MRI). This case is unique in that it is the first case with development of lumbar disc herniation associated with S1 vertebral corpus fusion anomaly. Congenital malformations with unusual clinical presentation after trauma should be evaluated through advanced radiological imaging techniques.
Adult
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Collagen
;
Humans
;
Leg
;
Magnetic Resonance Imaging
;
Motor Activity
;
Nervous System
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Obesity
;
Smoke
;
Smoking
;
Spinal Nerve Roots
;
Spine
3.Glial Cell Line-Derived Neurotrophic Factor, S-100 Protein and Synaptophysin Expression in Biliary Atresia Gallbladder Tissue
Semra GÜRÜNLÜOĞLU ; Canan CERAN ; Kubilay GÜRÜNLÜOĞLU ; Alper KOÇBIYIK ; Mehmet GÜL ; Turan YILDIZ ; Harika Gözükara BAĞ ; Semir GÜL ; Aytaç TAŞÇI ; Ercan BAYRAKÇI ; Necmettin AKPINAR ; Ecem Serbest ÇIN ; Hasan ATEŞ ; Mehmet DEMIRCAN
Pediatric Gastroenterology, Hepatology & Nutrition 2021;24(2):173-186
Purpose:
Biliary atresia (BA) is a disease that manifests as jaundice after birth and leads to progressive destruction of the ductal system in the liver. The aim of this study was to investigate histopathological changes and immunohistochemically examine the expression of glial cell line-derived neurotrophic factor (GDNF), synaptophysin, and S-100 protein in the gallbladder of BA patients.
Methods:
The study included a BA group of 29 patients and a control group of 41 children with cholecystectomy. Gallbladder tissue removed during surgery was obtained and examined immunohistochemically and histopathologically. Tissue samples of both groups were immunohistochemically assessed in terms of GDNF, S-100 protein, and synaptophysin expression. Expression was classified as present or absent. Inflammatory activity assessment with hematoxylin and eosin staining and fibrosis assessment with Masson's trichrome staining were performed for tissue sample sections of both groups.
Results:
Ganglion cells were not present in gallbladder tissue samples of the BA group.Immunohistochemically, GDNF, synaptophysin, and S-100 expression was not detected in the BA group. Histopathological examination revealed more frequent fibrosis and slightly higher inflammatory activity in the BA than in the control group.
Conclusion
We speculate that GDNF expression will no longer continue in this region, when the damage caused by inflammation of the extrahepatic bile ducts reaches a critical threshold. The study's findings may represent a missing link in the chain of events forming the etiology of BA and may be helpful in its diagnosis.
4.Glial Cell Line-Derived Neurotrophic Factor, S-100 Protein and Synaptophysin Expression in Biliary Atresia Gallbladder Tissue
Semra GÜRÜNLÜOĞLU ; Canan CERAN ; Kubilay GÜRÜNLÜOĞLU ; Alper KOÇBIYIK ; Mehmet GÜL ; Turan YILDIZ ; Harika Gözükara BAĞ ; Semir GÜL ; Aytaç TAŞÇI ; Ercan BAYRAKÇI ; Necmettin AKPINAR ; Ecem Serbest ÇIN ; Hasan ATEŞ ; Mehmet DEMIRCAN
Pediatric Gastroenterology, Hepatology & Nutrition 2021;24(2):173-186
Purpose:
Biliary atresia (BA) is a disease that manifests as jaundice after birth and leads to progressive destruction of the ductal system in the liver. The aim of this study was to investigate histopathological changes and immunohistochemically examine the expression of glial cell line-derived neurotrophic factor (GDNF), synaptophysin, and S-100 protein in the gallbladder of BA patients.
Methods:
The study included a BA group of 29 patients and a control group of 41 children with cholecystectomy. Gallbladder tissue removed during surgery was obtained and examined immunohistochemically and histopathologically. Tissue samples of both groups were immunohistochemically assessed in terms of GDNF, S-100 protein, and synaptophysin expression. Expression was classified as present or absent. Inflammatory activity assessment with hematoxylin and eosin staining and fibrosis assessment with Masson's trichrome staining were performed for tissue sample sections of both groups.
Results:
Ganglion cells were not present in gallbladder tissue samples of the BA group.Immunohistochemically, GDNF, synaptophysin, and S-100 expression was not detected in the BA group. Histopathological examination revealed more frequent fibrosis and slightly higher inflammatory activity in the BA than in the control group.
Conclusion
We speculate that GDNF expression will no longer continue in this region, when the damage caused by inflammation of the extrahepatic bile ducts reaches a critical threshold. The study's findings may represent a missing link in the chain of events forming the etiology of BA and may be helpful in its diagnosis.