DOCSLIB.ORG

Systemic Conditions and Developmental Defects of Enamel

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
Systemic Conditions and Developmental Defects of Enamel SYSTEMIC CONDITIONS AND DEVELOPMENTAL DEFECTS OF ENAMEL IN A COHORT OF VLBW AND NBW INFANTS by HUN SHIM Submitted in partial fulfillment of the requirements for the degree of Master of Science Clinical Research Scholars Program School of Medicine CASE WESTERN RESERVE UNIVERSITY August, 2016 CASE WESTERN RESERVE UNIVERSITY SCHOOL OF GRADUATE STUDIES We hereby approve the thesis/dissertation of Hun Shim, DMD Candidate for the Master of Science degree *. (signed) Suchitra Nelson, PhD . (Chair of committee) James Spilsbury, PhD MPH . Kristin Victoroff, DDS, PhD . __________________________________________ __________________________________________ (Date) May 12, 2016 *We also certify that written approval has been obtained for any proprietary material contained therein. 1 Dedicated to my family and my many mentors who have helped shape my paradigm in education, career, and life. 2 Table of Contents LIST OF TABLES ............................................................................................................. 4 LIST OF FIGURES ........................................................................................................... 5 ACKNOWLEDGEMENTS ............................................................................................... 6 LIST OF ABBREVIATIONS ............................................................................................ 7 ABSTRACT ....................................................................................................................... 8 BACKGROUND AND SIGNIFICANCE ......................................................................... 9 METHODS ...................................................................................................................... 16 RESULTS ........................................................................................................................ 21 DISCUSSION .................................................................................................................. 28 APPENDIX ...................................................................................................................... 35 BIBLIOGRAPHY ............................................................................................................ 39 3 List of Tables Table 1: Characteristics of participants and non-participants .......................................... 21 Table 2: Infant Clinical Risk Grouping (CRG) classification distribution ....................... 22 Table 3: Association of CRG with hypoplasia and demarcated opacity .......................... 22 Table 4: Correlation of maternal sociodemographic and medical risk factors with DDE 23 Table 5: Correlation among CRG and maternal sociodemographic and medical risk factors ................................................................................................................................ 24 Table 6. Hierarchical model of 8-month CRG and maternal sociodemographic and medical risk factors predicting 36-month hypoplasia and demarcated opacities ............. 25 Table 7. Hierarchical model of 8-month CRG and maternal sociodemographic and medical risk factors predicting 36-month enamel hypoplasia stratified by birth group .. 26 4 List of Figures Figure 1: Conceptual Model ............................................................................................. 34 Figure 2: Infant medical abstraction and follow-up medical history form ....................... 35 5 Acknowledgements I would like to thank the following individuals for their guidance and mentorship with this project and my program: Dr. Suchitra Nelson for mentoring me throughout my Mastership, specifically providing valuable feedback to my project’s progress and being a source of inspiration for my career in dentistry as a clinician and researcher. Shelley Curtan for all assistance with administrative needs. Yiying Liu for assistance in data analysis and interpretation My family and church for caring and being the spiritual and social support during challenging times to help me focus on my Mastership 6 List of Abbreviations VLBW Very Low Birth Weight NBW Normal Birth Weight CWRU Case Western Reserve University CDC Centers for Disease Control DDE Developmental Defects of Enamel NICU Neonatal Intensive Care Unit CRG Clinical Risk Grouping BPD Bronchopulmonary Dysplasia RDS Respiratory Distress Syndrome 7 Systemic Conditions and Developmental Defects of Enamel in a Cohort of VLBW and NBW Infants Abstract by HUN SHIM This retrospective cohort study investigated the effects of VLBW and NBW infants’ systemic health on DDE. The sample consisted of 293 infant-caregiver dyads that attended all three visits based on an original cohort study. Infants’ systemic conditions were classified by a modified CRG index for 8 and 18-month visits. Developmental defects of enamel (DDE: hypoplasia and demarcated opacities) were obtained from 36- month dental examination records. A hierarchical negative binomial model was utilized. The model controlling for maternal sociodemographic and prenatal factors indicated that severe 8-month CRG level compared to healthy significantly increased 36-month hypoplasia (p<0.05), but not for demarcated opacities. Caregiver’s low socioeconomic status and prenatal smoking also significantly influenced 36-month hypoplasia also. The model stratified by birth group indicated that severe CRG affected hypoplasia significantly in VBLW infants, but not in NBW infants. In conclusion, severe systemic conditions were significantly associated with enamel hypoplasia. 8 Background and Significance Facts about VLBW Infants Preterm births (< 37weeks gestation) and very low birth weight (VLBW: < 1500 grams) lead to chronic conditions and physical and mental developmental anomalies in infants (Hack et al., 1993); Recent national survey (Center for Disease Control: CDC) in 2014 estimated that 1 in 10 births are VLBW in the United States. Studies have found that caregiver risk factors such as education attainment below high school, younger maternal age at birth, history of substance abuse including smoking (Hack et al., 1993; Kleinment et al., 1985; Diaz et al., 2001; Najati and Gojazadeh, 2010), and being in non-Hispanic African American race (Kempe et al., 1992) increased the risk of infants born preterm and VLBW. VLBW infants are susceptible to numerous systemic problems that include the following: Necrotizing entercolitis a disease that impairs the function of the enteral system in absorption of sugars, proteins, vitamins, and other key nutrients (Patel et al., 2012); bronchopulmonary dysplasia (BPD) and respiratory distress syndrome (RDS), which affect 68% VLBW infants and are the most common causes of pulmonary mortalities in this population (Kair et al., 2012; Beam et al., 2014); Anemia of prematurity and jaundice as a result of hyperbilirubinemia following excessive red blood cell breakdown (Watchko and Maisels, 2003) with as much as 76.6% in VLBW susceptible to jaundice and 37.3% with more severe levels of anemia and jaundice to require transfusion in order to recover appropriate blood cell levels (Narang et al., 2001); Patent ductus arteriosus, a pathologic communication in the circulation bypassing the respiratory system, 9 contributing to low blood cell levels predisposing VLBW infants to sepsis that can be life threatening (Hornik et al., 2012); neurological conditions such as intraventricular hemorrhage and periventricular leukomalacia that have been implicated in cognitive disabilities and neurodevelopmental delays (McCrea and Ment, 2008; Pellicer et al., 2009; Linsell et al., 2015). Due to the complex, multi-system nature of VLBW infant’s systemic conditions, barriers still remain in consolidating evidence for the most effective interventions to reduce the morbidity and mortality burdens of the VLBW cohort and restore them to comparable health of NBW infants (Patel et al., 2012; Eber et al., 2001; Ballot et al., 2015; Kusuda et al., 2008). VLBW infants are also susceptible to oral conditions. Being born VLBW predisposes infants to delayed eruption patterns. Studies have shown that birth weight is inversely related to eruption of the first deciduous teeth (Ramos et al., 2006; Khalifa et al., 2014; Nelson et al., 2013). VLBW infants are also subject to malocclusion; Seow et al., 1987 suggested that VLBW infants with more severe cases of medical compromise may experience space loss leading to malocclusion in deciduous and thereby succadaneous teeth. Most importantly, VLBW infants are subject to developmental defects of enamel (DDE) in deciduous teeth. DDE or enamel defects can be divided into enamel hypoplasia and opacities: enamel hypoplasia is defined as a break in continuity of enamel leading to reduced thickness and enamel pits and grooves; opacities are defined as alterations in translucency of the enamel in demarcated or diffused form of which demarcated is more prevalent in VLBW infants (Commision on Oral Health 1992). A recent literature review investigated preterm birth as etiology for oral morbidities and found DDE as the most 10 prevalent overall compared to other conditions including delayed eruption and malocclusion (Zaidi et al., 2015). The prevalence of DDE ranges from 62.3% to 96%, depending on the birth weight of the infant (Lai et al., 1997; Aine et al., 2000; Cruvinel et al., 2012). The consequences of DDE are substantial and multifaceted. On a social psychological level, DDE has been shown to be a source of embarrassment and dissatisfaction to adolescents and caregivers due to
Load more

Recommended publications
  • Dental and Temporomandibular Joint Pathology of the Kit Fox (Vulpes Macrotis)
    Author's Personal Copy J. Comp. Path. 2019, Vol. 167, 60e72 Available online at www.sciencedirect.com ScienceDirect www.elsevier.com/locate/jcpa DISEASE IN WILDLIFE OR EXOTIC SPECIES Dental and Temporomandibular Joint Pathology of the Kit Fox (Vulpes macrotis) N. Yanagisawa*, R. E. Wilson*, P. H. Kass† and F. J. M. Verstraete* *Department of Surgical and Radiological Sciences and † Department of Population Health and Reproduction, School of Veterinary Medicine, University of California, Davis, California, USA Summary Skull specimens from 836 kit foxes (Vulpes macrotis) were examined macroscopically according to predefined criteria; 559 specimens were included in this study. The study group consisted of 248 (44.4%) females, 267 (47.8%) males and 44 (7.9%) specimens of unknown sex; 128 (22.9%) skulls were from young adults and 431 (77.1%) were from adults. Of the 23,478 possible teeth, 21,883 teeth (93.2%) were present for examina- tion, 45 (1.9%) were absent congenitally, 405 (1.7%) were acquired losses and 1,145 (4.9%) were missing ar- tefactually. No persistent deciduous teeth were observed. Eight (0.04%) supernumerary teeth were found in seven (1.3%) specimens and 13 (0.06%) teeth from 12 (2.1%) specimens were malformed. Root number vari- ation was present in 20.3% (403/1,984) of the present maxillary and mandibular first premolar teeth. Eleven (2.0%) foxes had lesions consistent with enamel hypoplasia and 77 (13.8%) had fenestrations in the maxillary alveolar bone. Periodontitis and attrition/abrasion affected the majority of foxes (71.6% and 90.5%, respec- tively).
    [Show full text]
  • Dental and Temporomandibular Joint Pathology of the Walrus (Odobenus Rosmarus)
    J. Comp. Path. 2016, Vol. -,1e12 Available online at www.sciencedirect.com ScienceDirect www.elsevier.com/locate/jcpa DISEASE IN WILDLIFE OR EXOTIC SPECIES Dental and Temporomandibular Joint Pathology of the Walrus (Odobenus rosmarus) J. N. Winer*, B. Arzi†, D. M. Leale†,P.H.Kass‡ and F. J. M. Verstraete† *William R. Pritchard Veterinary Medical Teaching Hospital, † Department of Surgical and Radiological Sciences and ‡ Department of Population Health and Reproduction, School of Veterinary Medicine, University of California, Davis, CA, USA Summary Maxillae and/or mandibles from 76 walruses (Odobenus rosmarus) were examined macroscopically according to predefined criteria. The museum specimens were acquired between 1932 and 2014. Forty-five specimens (59.2%) were from male animals, 29 (38.2%) from female animals and two (2.6%) from animals of unknown sex, with 58 adults (76.3%) and 18 young adults (23.7%) included in this study. The number of teeth available for examination was 830 (33.6%); 18.5% of teeth were absent artefactually, 3.3% were deemed to be absent due to acquired tooth loss and 44.5% were absent congenitally. The theoretical complete dental formula was confirmed to be I 3/3, C 1/1, P 4/3, M 2/2, while the most probable dental formula is I 1/0, C 1/1, P 3/3, M 0/0; none of the specimens in this study possessed a full complement of theoretically possible teeth. The majority of teeth were normal in morphology; only five teeth (0.6% of available teeth) were malformed. Only one tooth had an aberrant number of roots and only one supernumerary tooth was encountered.
    [Show full text]
  • Review Article Autoimmune Diseases and Their Manifestations on Oral Cavity: Diagnosis and Clinical Management
    Hindawi Journal of Immunology Research Volume 2018, Article ID 6061825, 6 pages https://doi.org/10.1155/2018/6061825 Review Article Autoimmune Diseases and Their Manifestations on Oral Cavity: Diagnosis and Clinical Management Matteo Saccucci , Gabriele Di Carlo , Maurizio Bossù, Francesca Giovarruscio, Alessandro Salucci, and Antonella Polimeni Department of Oral and Maxillo-Facial Sciences, Sapienza University of Rome, Viale Regina Elena 287a, 00161 Rome, Italy Correspondence should be addressed to Matteo Saccucci; [email protected] Received 30 March 2018; Accepted 15 May 2018; Published 27 May 2018 Academic Editor: Theresa Hautz Copyright © 2018 Matteo Saccucci et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. Oral signs are frequently the first manifestation of autoimmune diseases. For this reason, dentists play an important role in the detection of emerging autoimmune pathologies. Indeed, an early diagnosis can play a decisive role in improving the quality of treatment strategies as well as quality of life. This can be obtained thanks to specific knowledge of oral manifestations of autoimmune diseases. This review is aimed at describing oral presentations, diagnosis, and treatment strategies for systemic lupus erythematosus, Sjögren syndrome, pemphigus vulgaris, mucous membrane pemphigoid, and Behcet disease. 1. Introduction 2. Systemic Lupus Erythematosus Increasing evidence is emerging for a steady rise of autoim- Systemic lupus erythematosus (SLE) is a severe and chronic mune diseases in the last decades [1]. Indeed, the growth in autoimmune inflammatory disease of unknown etiopatho- autoimmune diseases equals the surge in allergic and cancer genesis and various clinical presentations.
    [Show full text]
  • Unusual Enamel Hypoplasia Associated with Teeth Mobility in a 13 Year Old Girl with Wilson Disease Nehal F
    ndrom Sy es tic & e G n e e n G e f Hassib et al., J Genet Syndr Gene Ther 2012, 3:4 T o Journal of Genetic Syndromes h l e a r n a DOI: 10.4172/2157-7412.1000118 r p u y o J & Gene Therapy ISSN: 2157-7412 Case Report Open Access Unusual Enamel Hypoplasia Associated with Teeth Mobility in a 13 Year Old Girl with Wilson Disease Nehal F. Hassib*, Maie A. Mahmoud, Nevin M. Talaat and Tarek H. El-Badry National Research Centre, Giza, Egypt Abstract Wilson disease is an autosomal recessive disorder caused by mutations in the ATP7B gene. It is characterized by the progressive accumulation of copper in the body leading to liver cirrhosis and neuropsychological deterioration. This case may be the first one reported Wilson disease in association with remarkable enamel hypoplasia and teeth mobility leading to severe teeth destruction and pulp exposure. The objective of this investigation was to introduce the dental management for a 13 year old female patient with Wilson disease. The patients restored her smile and she was highly satisfied of the dental work. In conclusion, the dental management of patients with Wilson disease should become the focus of research because of the difficulty in patients’ management as our patient was suffering from dystonia restricting the mouth opening and in addition of being a mouth breather which affected the time and quality of the dental work. Keywords: Wilson disease; Enamel hypoplasia; Periodontal disease; lips and prominent philtrum (Figure 1a). Intraoral examination showed Copper disorder metabolism high arched palate, anterior open bite and enamel hypoplasia (Figures 1b and c).
    [Show full text]
  • Analysis of the COL17A1 in Non-Herlitz Junctional Epidermolysis Bullosa and Amelogenesis Imperfecta
    333-337 29/6/06 12:35 Page 333 INTERNATIONAL JOURNAL OF MOLECULAR MEDICINE 18: 333-337, 2006 333 Analysis of the COL17A1 in non-Herlitz junctional epidermolysis bullosa and amelogenesis imperfecta HIROYUKI NAKAMURA1, DAISUKE SAWAMURA1, MAKI GOTO1, HIDEKI NAKAMURA1, MIYUKI KIDA2, TADASHI ARIGA2, YUKIO SAKIYAMA2, KOKI TOMIZAWA3, HIROSHI MITSUI4, KUNIHIKO TAMAKI4 and HIROSHI SHIMIZU1 1Department of Dermatology, 2Research Group of Human Gene Therapy, Hokkaido University Graduate School of Medicine, Sapporo 060-8638; 3Department of Dermatology, Ebetsu City Hospital, Hokkaido; 4Department of Dermatology, Faculty of Medicine, University of Tokyo, Tokyo, Japan Received January 31, 2006; Accepted March 27, 2006 Abstract. Non-Herlitz junctional epidermolysis bullosa (nH- truncated polypeptide expression and to a milder clinical JEB) disease manifests with skin blistering, atrophy and tooth disease severity in nH-JEB. Conversely, we failed to detect enamel hypoplasia. The majority of patients with nH-JEB any pathogenic COL17A1 defects in AI patients, in either harbor mutations in COL17A1, the gene encoding type XVII exon or within the intron-exon borders of AI patients. This collagen. Heterozygotes with a single COL17A1 mutation, nH- study furthers the understanding of mutations in COL17A1 JEB defect carriers, may exhibit only enamel hypoplasia. In causing nH-JEB, and clearly demonstrates that the mechanism this study, to further elucidate COL17A1 mutation phenotype/ of enamel hypoplasia differs between nH-JEB and AI genotype correlations, we examined two unrelated families diseases. with nH-JEB. Furthermore, we hypothesized that COL17A1 mutations might underlie or worsen the enamel hypoplasia seen Introduction in amelogenesis imperfecta (AI) patients that are characterized by defects in tooth enamel formation without other systemic Type XVII collagen, 180-kDa bullous pemphigoid antigen is manifestations.
    [Show full text]
  • Focus on Shingles and the Shingles Vaccines - by Allen Lefkovitz
    October 2018 THE OMNICARE HealthLine Focus on Shingles and the Shingles Vaccines - by Allen Lefkovitz he current estimates from the Centers for Disease The risk of complications associated with shingles also TControl and Prevention (CDC) are that one in three increases with age. Complications associated with persons in the United States and 50% of adults 85 years shingles include, but are not limited to the following: or older will develop shingles (aka herpes zoster). Shingles Postherpetic neuralgia is a painful, localized skin rash that is caused by the same Scarring virus as chickenpox [i.e., the varicella zoster virus (VZV)]. (PHN) Following chickenpox, VZV remains in the body, but may Bacterial skin infections Vision and/or hearing reactivate many years later resulting in shingles. Shingles (e.g., Staphylococcus aureus) impairment is generally characterized by pain followed by a rash on one side of the body (usually in one or two areas called Pneumonia Social isolation dermatomes). The rash goes on to develop into fluid-filled blisters that typically scab over in 7 to 10 days, and then Brain inflammation Hepatitis gradually resolve in 2 to 4 weeks. Beyond pain and itching, other symptoms of shingles may include fever, headache, Weakness or paralysis Death sensitivity to light, and/or nausea. While exposure to someone with shingles does not PHN is the most common complication of shingles and increase your risk of shingles, individuals who have never may occur in up to 20% of individuals with shingles. PHN had chickenpox and who have never been vaccinated for involves persistent pain in the area where the rash used chickenpox are at risk of contracting VZV.
    [Show full text]
  • Congenital Hypothyrodism and Its Oral Manifestations Hipotiroidismo Congénito Y Sus Manifestaciones Bucales
    www.medigraphic.org.mx Revista Odontológica Mexicana Facultad de Odontología Vol. 18, No. 2 April-June 2014 pp 133-138 CASE REPORT Congenital hypothyrodism and its oral manifestations Hipotiroidismo congénito y sus manifestaciones bucales Marxy E Reynoso Rodríguez,* María A Monter García,§ Ignacio Sánchez FloresII ABSTRACT RESUMEN Hypothyroidism is one of the most common thyroid disorders. El hipotiroidismo es el más común de los trastornos de la tiroides, Hypothyroidism can be congenital in cases when the thyroid puede ser congénito si la glándula tiroides no se desarrolla correc- gland does not develop normally. Female predominance is a tamente (hipotiroidismo congénito). La predominancia femenina es characteristic of congenital hypothyroidism. Dental characteristics una característica. Entre las características odontológicas del hi- of hypothyroidism are thick lips, a large-sized tongue which, due potiroidismo se observan labios gruesos, lengua de gran tamaño, to its position, can elicit anterior open bite as well as fanned-out que debido a su posición suele producir mordida abierta anterior y anterior teeth. In these cases, delayed eruption of primary and dientes anteriores en abanico, destaca que la dentición temporal y permanent dentitions can be observed, and teeth, even though permanente presentan un retardo eruptivo característico y, aunque normal-sized, are crowded due to the small-sized jaws. This study los dientes son de tamaño normal, suelen estar apiñados por el ta- presents clinical cases of female patients diagnosed with congenital maño pequeño de los maxilares. Se presentan dos casos clínicos hypothyroidism who sought treatment at the Dental Pediatrics Unit de pacientes de sexo femenino que acuden a la clínica de Especia- of the Autonomous University of the State of Mexico.
    [Show full text]
  • Oral Manifestations of Red Blood C Research Article
    z Available online at http://www.journalcra.com INTERNATIONAL JOURNAL OF CURRENT RESEARCH International Journal of Current Research Vol. 10, Issue, 11, pp.75681-75686, November, 2018 DOI: https://doi.org/10.24941/ijcr.33312.11.2018 ISSN: 0975-833X RESEARCH ARTICLE ORAL MANIFESTATIONS OF RED BLOOD CELL DISORDERS: A RECENT ANATOMIZATION 1Swatantra Shrivastava, 2Sourabh Sahu, 3Pavan Kumar Singh, 4Rajeev Kumar Shrivastava, 5, *Soumendu Bikash Maiti and 6Stuti Shukla 1Department of Oral Medicine and Radiology, New Horizon Dental College and Research Institute, Bilaspur, India 2MGM Medical College and Hospital, Aurangabad, India 3Department of Public Health Dentistry, Vyas Dental College and Hospital, India 4Master of Dental Surgery , Department of Prosthodontics and Crown and Bridge, New Horizon Dental College and Research Institute, Bilaspur, Udaipur, India 5Senior Lecturer, Department of Oral Medicine and Radiology, Pacific Dental College and Research Center, India 6Post Graduate, Department of Oral Medicine and Radiology, New horizon Dental College and Research center, Bilaspur India ARTICLE INFO ABSTRACT Article History: Primary objective of the literature is recognize and evaluate the wide array of oral manifestations Received 17th August, 2018 associated with red blood cell disorders which would eventually aid in diagnosis of the lesions Received in revised form associated with the disorders for the practitioners. It starts with petechiae, spontaneous gingival 03rd September, 2018 bleeding, herpetic infection in aplastic anaemia to hunter’s glossitis in pernicious anaemia. Literature Accepted 26th October, 2018 also includes enamel hypoplasia associated with erythroblastis fetalis, atrophic glossitis in iron th Published online 30 November, 2018 deficiency anemia with symptom of glossodynia in megaloblastic anemia. Marked manifestations of pharyngo-esophageal ulcerations and esophageal webs seen in plummer Vinson syndrome and Key Words: periodontitis, taurodontism, agenesia, supernumerary teeth to be seen in fanconi’s anemia.
    [Show full text]
  • Developmental Defects of the Enamel and Its Impact on the Oral Health
    Folayan et al. BMC Oral Health (2018) 18:160 https://doi.org/10.1186/s12903-018-0622-3 RESEARCHARTICLE Open Access Developmental defects of the enamel and its impact on the oral health quality of life of children resident in Southwest Nigeria Morenike Oluwatoyin Folayan1,2* , Nneka Maureen Chukwumah3, Bamidele Olubukola Popoola4, Dada Oluwaseyi Temilola1, Nneka Kate Onyejaka5, Titus Ayo Oyedele6,7 and Folake Barakat Lawal4 Abstract Background: Developmental defects of the enamel (DDE) increase the risk for diseases that impact negatively on the quality of life. The objective of this study was to compare the oral health quality of life of children with molar- incisor-hypomineralisation (MIH) and enamel hypoplasia; and assess if caries worsened the impact of these lesions on the quality of life. Methods: This study recruited 853 6 to 16-years-old school children. They filled the Child-OIDP questionnaire. The MIH, enamel hypoplasia, caries and oral hygiene status was assessed. Poisson regression was used to determine the impact of MIH and enamel hypoplasia on the oral health quality of life, after adjusting for the effect of sex, age, socioeconomic class, oral hygiene and caries status. Results: The prevalence of MIH and enamel hypoplasia was 2.9% and 7.6% respectively. There was no significant difference in the mean child-OIDP scores of children with or without MIH (p = 0.57), children with or without enamel hypoplasia (p = 0.48), and children with enamel hypoplasia with and without caries (p = 0.30). Children with enamel hypoplasia and caries had worse outcomes for speaking (p = 0.01).
    [Show full text]
  • Dental and Temporomandibular Joint Pathology of the Polar Bear (Ursus Maritimus)
    J. Comp. Path. 2016, Vol. 155, 231e241 Available online at www.sciencedirect.com ScienceDirect www.elsevier.com/locate/jcpa DISEASE IN WILDLIFE OR EXOTIC SPECIES Dental and Temporomandibular Joint Pathology of the Polar Bear (Ursus maritimus) J. N. Winer*, B. Arzi†, D. M. Leale†,P.H.Kass‡ and F. J. M. Verstraete† *William R. Pritchard Veterinary Medical Teaching Hospital, † Department of Surgical and Radiological Sciences and ‡ Department of Population Health and Reproduction, School of Veterinary Medicine, University of California, Davis, CA, USA Summary Museum specimens (maxillae and/or mandibles) from 317 polar bears (Ursus maritimus) were examined macro- scopically according to predefined criteria and 249 specimens were included in this study. The specimens were acquired between 1906 and 2011. There were 126 specimens (50.6%) from male animals, 93 (37.3%) from fe- male animals and 30 (12.1%) from animals of unknown sex. The ages of the animals ranged from neonate to adult, with 125 adults (50.2%) and 124 young adults (49.8%) included and neonates/juveniles excluded from the study. The number of teeth available for examination was 7,638 (73.5%); 12.3% of teeth were absent ar- tefactually, 0.8% were deemed absent due to acquired tooth loss and 13.4% were absent congenitally. With respect to tooth morphology, 20 teeth (0.26% of available teeth) in 18 specimens (7.2% of available specimens) were small vestigial structures with crowns that were flush with the level of surrounding alveolar bone. One supernumerary tooth and one tooth with enamel hypoplasia were encountered. Persistent deciduous teeth and teeth with an aberrant number of roots were not found.
    [Show full text]
  • Enamel Pearl Associated with Localized Periodontitis in Hellenistic Age Woman
    T o m o v e t a l . C A S E R E P O R T Enamel pearl associated with localized periodontitis in Hellenistic age woman • Georgi Tomov (1), Elka Popova (2), Rumen Ivanov (3), Nadezhda Atanassova (4) • 1 - Оral Pathology Department, Faculty of Dental Medicine, Medical University, Plovdiv, Bulgaria 2 - Periodontology Department, Faculty of Dental Medicine, Medical University, Plovdiv, Bulgaria 3 - Archeologist 4 – National Anthropological Museum at Institute of Experimental Morphology, Pathology and Anthropology with Museum Address for correspondence: Assoc.Prof. Georgi Tomov, PhD Medical University Plovdiv, Faculty of Dental Medicine, Oral Pathology Department, Plovdiv, Bulgaria Phone: +359896742065 E- mail: [email protected] Bull Int Assoc Paleodont. 2017;11(2):62-66. Abstract Tooth anatomic factors like ectopic enamel pearls are often associated with localized periodontal inflammation and bone loss. There are no existing paleopathological data for such structural anomalies in ancient populations associated with periodontal pathology in the literature. A rare case of enamel pearl on the maxillary right first molar of women associated with localized periodontitis is presented and discussed. Keywords: enamel pearl; localized periodontitis; paleopathology; Hellenistic age Bull Int Assoc Paleodont. Volume 11, Number 2, 2017 www.paleodontology.com 62 Bulletin of the International Association for Paleodontology NO-FEE OPEN ACCESS JOURNAL T o m o v e t a l . C A S E R E P O R T Introduction are found in Plovdiv, Bulgaria (archeological site Bacterial plaque has been implicated as the “Kirkor Azarian” №4) and are provided for primary etiologic factor in the initiation and anthropological study in the Medical University progression of gingivitis and periodontitis (1).
    [Show full text]
  • Hypoplastic Amelogenesis Imperfecta with Multiple Impacted Teeth – Report of Two Cases
    J Clin Exp Dent. 2010;2(4):e207-11. Hypoplastic amelogenesis imperfecta. Journal section: Oral Medicine and Pathology doi:10.4317/jced.2.e207 Publication Types: Case report Hypoplastic amelogenesis imperfecta with multiple impacted teeth – report of two cases Sujatha S. Reddy 1, Aarthi Nisha V 2, Harish BN 3 1 Professor, Departament of Oral Medicine, Diagnosis and Radiology, M. S. Ramaiah Dental College & Hospital, Msrit Post, New Bel Road, Bangalore, Karnataka, India. 2 PG student, Departament of Oral Medicine, Diagnosis and Radiology, M. S. Ramaiah Dental College & Hospital, Msrit Post, New Bel Road, Bangalore, Karnataka, India. 3 Lecturer, Departament of Oral Medicine, Diagnosis and Radiology, M. S. Ramaiah Dental College & Hospital, Msrit Post, New Bel Road, Bangalore, Karnataka, India. Correspondence: Departament of Oral Medicine, Diagnosis and Radiology M.S.Ramaiah Dental College & Hospital, Msrit Post, new bel road, Bangalore-560054 e-mail id: [email protected] Received: 17/06/2010 Accepted: 30/07/2010 Reddy SS, Aarthi Nisha V, Harish BN. Hypoplastic amelogenesis imperfecta with multiple impacted teeth – report of two cases. J Clin Exp Dent. 2010;2(4):e207-11. http://www.medicinaoral.com/odo/volumenes/v2i4/jcedv2i4p207.pdf Article Number: 50332 http://www.medicinaoral.com/odo/indice.htm © Medicina Oral S. L. C.I.F. B 96689336 - eISSN: 1989-5488 eMail: [email protected] Abstract Amelogenesis Imperfecta (AI) represents a group of developmental conditions, genomic in origin, which affect the structure and clinical appearance of enamel of all or nearly all the teeth in a more or less equal manner. It is usually inherited either as an X-linked, autosomal dominant or autosomal recessive trait.
    [Show full text]