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Author: Ngozi Nnonyelum Nwizu Publisher: ISBN: Category : Languages : en Pages : 434
Book Description
Background: Periodontal disease typically presents as a chronic, low grade inflammatory process involving the periodontium. However, it also has the potential to produce systemic effects at distant organs sites and has been linked to several systemic conditions including cancer. Epidemiological studies on the association between periodontal disease and cancer risk are however limited, but most suggest a positive association. Only three studies (3) so far have examined total cancer risk in a prospective study. With respect to individual cancer sites, to our knowledge, no large epidemiological prospective study has examined the association between periodontal disease and colorectal cancer. This is in spite of evidence from experimental studies linking an established periodontal pathogen, Fusobacterium nucleatum, to premalignant and cancerous lesions of the colorectum. This prospective study evaluated the association between periodontal disease and risk of diagnosis of incident total-, as well as, colorectal cancer. Since periodontal disease may influence cancer risk through its ability to induce a chronic, low-grade, systemic inflammation, and serum CRP is an established biomarker of systemic inflammation; this study also investigated the association between prevalence and severity of measured periodontal disease, and serum hsCRP levels. Furthermore, independent evaluations of the role of active gingival inflammation, and presence of select periodontal pathogens, in influencing serum hsCRP levels respectively were conducted. Potential interactions of each of these measures with periodontal disease in relation to serum hsCRP levels were also explored. Methods: These studies were conducted utilizing data from the Women's Health Initiative Observational Study (WHI-OS). The study included three aims. Aim 1: evaluated the associations between periodontal disease and total cancer; Aim 2: evaluated the association of periodontal disease and colorectal cancer; and Aim 3 evaluated the association of periodontal disease and serum CRP levels. For the total cancer risk study, an analytic cohort of 65,869 postmenopausal women was used, while the colorectal cancer risk study involved 78,835 postmenopausal women. Periodontal disease status for these 2 studies was determined by self-report from the Year 5 Women's Health Initiative Observational Study (WHI-OS) follow-up questionnaire administered from 1999 through 2003. These women were between the ages of 54-86 years at the time the periodontal questionnaire was administered and were followed up for a maximum period of 15 years. Total cancer and colorectal cancer were evaluated using the first diagnosis of any incident cancer or colorectal cancer reported after the year-5 visit respectively.^Adjudication of cancer cases was determined via medical records by physicians. The risk of diagnosis of incident total-, regional-, site-specific and colorectal cancers were evaluated using Cox proportional hazards regression. For the association between periodontal disease and serum CRP levels, we conducted a cross-sectional study utilizing data from 620 postmenopausal women (aged 53-83 years) in an ancillary study of the Women's Health Initiative Observational Study (WHI-OS) in Buffalo NY, the OsteoPerio Study. Periodontal disease status was determined using clinical measures based on the Center for Disease Control and Prevention/American Academy of Periodontology (CDC/AAP) clinical case definition for periodontal disease; and independent measures of whole mouth mean, and worst site involvement of periodontal probing depth (PPD), and clinical attachment loss (CAL), respectively. Serum hsCRP concentration was evaluated using an immunoturbidimetric assay. Mean percentage of bleeding sites on gentle probing (>50% cut point), was used to confirm the presence of active gingival inflammation; while presence of select periodontal pathogens (Porphyromonas gingivalis, Tannerella Forsythia, Fusobacterium nucleatum, Prevotella intermedia, and Campylobacter rectus), were detected by immunofluorescence and phase contrast microscopy using pooled sub-gingival plaque samples. All statistical tests were two-sided. Results: 7,678 cases of primary incident cancer were diagnosed over a mean follow-up of 8. 32 years. Periodontal disease history was associated with a 12% statistically significant increased risk of diagnosis of cancer overall, after adjusting for potential confounders [HR 1. 12, 95% CI 1. 07-1. 18]. This finding remained significant among the sample of 34,097 women who had never smoked [HR 1. 11, 95% CI 1. 02-1. 20]. Statistically significant associations were also observed for cancers of the breast [HR 1. 10, 95% CI 1. 01-1. 19]; lung [HR 1. 31, 95% CI 1. 14-1. 51]; esophagus [HR 3. 28, 95% CI 1. 64-6. 53]; gallbladder [HR 1. 73, 95% CI 1. 01-2. 95]; and melanoma skin cancers [HR 1. 23, 95% CI 1. 02-1. 48]. There was a near significant association with stomach cancer [HR 1. 58, 95% CI 0. 94-2. 67], but no associations with cancers of the pancreas or genitourinary system. There was no association between periodontal disease and risk diagnosis of colorectal cancer, after adjusting for potential confounders [hazard ratio (HR) = 1. 08, 95% confidence interval (CI): 0. 92-1. 26]. Similarly, no associations were observed with respect to anatomic location (colon, rectum and recto-sigmoid cancers) and tumor characteristics respectively. There was significant interaction between periodontal disease and diagnosis of colorectal cancer according to hormone therapy (HT) use (p =0. 03), and stratified analyses suggest current HT users, particularly of estrogen plus progestin (E+P), with a history of periodontal disease have a higher risk of being diagnosed with colorectal cancer [HR =1. 76, 95% CI: 1. 20-2. 59]. This effect was enhanced on restriction to colon cancer alone [HR =2. 02, 95% CI: 1. 34-3. 05}. However, dose-response effect was not consistent with time on HT use. Other results from our study indicate that participants with "severe" periodontal disease according to the CDC/AAP Clinical Case Definition demonstrated an almost 2-fold higher odds of having high serum CRP concentrations (>3. 0mg/l), compared to those with no/mild disease, after adjusting for potential confounders (OR 1. 86, 95% CI 1. 06-3. 27). Positive, linear, but statistically insignificant associations were observed between whole mouth mean and worst site PPD and CAL measures. None of the select pathogens examined (alone or in groups), or the presence of active gingival inflammation evidenced by percentage of sites that bled on probing (>50%), were associated with serum hsCRP levels. Also, no significant interaction effects were observed between periodontal disease, and any of the pathogens, (alone or in groups), or mean percentage bleeding sites (>50% cut point), on the serum hsCRP concentrations. Conclusion: Periodontal disease may enhance the risk of being diagnosed with total cancer risk in postmenopausal women; this finding persisted when restricting to never smokers. This risk appears to be higher for certain anatomic sites, particularly those in close proximity to the oral cavity such as the esophagus and upper gastrointestinal regions, but does not appear to extend to lower gastrointestinal tract sites such as the colon and rectum. The observed association between women with periodontal disease who are on hormone therapy and risk of being diagnosed with incident colorectal cancer requires further exploration, and we cannot rule out that it may be due to chance. This study also affirms that chronic inflammation may be one mechanism by which periodontal disease is associated with cancer risk. Additional research in other prospective cohorts is needed.
Author: Ngozi Nnonyelum Nwizu Publisher: ISBN: Category : Languages : en Pages : 434
Book Description
Background: Periodontal disease typically presents as a chronic, low grade inflammatory process involving the periodontium. However, it also has the potential to produce systemic effects at distant organs sites and has been linked to several systemic conditions including cancer. Epidemiological studies on the association between periodontal disease and cancer risk are however limited, but most suggest a positive association. Only three studies (3) so far have examined total cancer risk in a prospective study. With respect to individual cancer sites, to our knowledge, no large epidemiological prospective study has examined the association between periodontal disease and colorectal cancer. This is in spite of evidence from experimental studies linking an established periodontal pathogen, Fusobacterium nucleatum, to premalignant and cancerous lesions of the colorectum. This prospective study evaluated the association between periodontal disease and risk of diagnosis of incident total-, as well as, colorectal cancer. Since periodontal disease may influence cancer risk through its ability to induce a chronic, low-grade, systemic inflammation, and serum CRP is an established biomarker of systemic inflammation; this study also investigated the association between prevalence and severity of measured periodontal disease, and serum hsCRP levels. Furthermore, independent evaluations of the role of active gingival inflammation, and presence of select periodontal pathogens, in influencing serum hsCRP levels respectively were conducted. Potential interactions of each of these measures with periodontal disease in relation to serum hsCRP levels were also explored. Methods: These studies were conducted utilizing data from the Women's Health Initiative Observational Study (WHI-OS). The study included three aims. Aim 1: evaluated the associations between periodontal disease and total cancer; Aim 2: evaluated the association of periodontal disease and colorectal cancer; and Aim 3 evaluated the association of periodontal disease and serum CRP levels. For the total cancer risk study, an analytic cohort of 65,869 postmenopausal women was used, while the colorectal cancer risk study involved 78,835 postmenopausal women. Periodontal disease status for these 2 studies was determined by self-report from the Year 5 Women's Health Initiative Observational Study (WHI-OS) follow-up questionnaire administered from 1999 through 2003. These women were between the ages of 54-86 years at the time the periodontal questionnaire was administered and were followed up for a maximum period of 15 years. Total cancer and colorectal cancer were evaluated using the first diagnosis of any incident cancer or colorectal cancer reported after the year-5 visit respectively.^Adjudication of cancer cases was determined via medical records by physicians. The risk of diagnosis of incident total-, regional-, site-specific and colorectal cancers were evaluated using Cox proportional hazards regression. For the association between periodontal disease and serum CRP levels, we conducted a cross-sectional study utilizing data from 620 postmenopausal women (aged 53-83 years) in an ancillary study of the Women's Health Initiative Observational Study (WHI-OS) in Buffalo NY, the OsteoPerio Study. Periodontal disease status was determined using clinical measures based on the Center for Disease Control and Prevention/American Academy of Periodontology (CDC/AAP) clinical case definition for periodontal disease; and independent measures of whole mouth mean, and worst site involvement of periodontal probing depth (PPD), and clinical attachment loss (CAL), respectively. Serum hsCRP concentration was evaluated using an immunoturbidimetric assay. Mean percentage of bleeding sites on gentle probing (>50% cut point), was used to confirm the presence of active gingival inflammation; while presence of select periodontal pathogens (Porphyromonas gingivalis, Tannerella Forsythia, Fusobacterium nucleatum, Prevotella intermedia, and Campylobacter rectus), were detected by immunofluorescence and phase contrast microscopy using pooled sub-gingival plaque samples. All statistical tests were two-sided. Results: 7,678 cases of primary incident cancer were diagnosed over a mean follow-up of 8. 32 years. Periodontal disease history was associated with a 12% statistically significant increased risk of diagnosis of cancer overall, after adjusting for potential confounders [HR 1. 12, 95% CI 1. 07-1. 18]. This finding remained significant among the sample of 34,097 women who had never smoked [HR 1. 11, 95% CI 1. 02-1. 20]. Statistically significant associations were also observed for cancers of the breast [HR 1. 10, 95% CI 1. 01-1. 19]; lung [HR 1. 31, 95% CI 1. 14-1. 51]; esophagus [HR 3. 28, 95% CI 1. 64-6. 53]; gallbladder [HR 1. 73, 95% CI 1. 01-2. 95]; and melanoma skin cancers [HR 1. 23, 95% CI 1. 02-1. 48]. There was a near significant association with stomach cancer [HR 1. 58, 95% CI 0. 94-2. 67], but no associations with cancers of the pancreas or genitourinary system. There was no association between periodontal disease and risk diagnosis of colorectal cancer, after adjusting for potential confounders [hazard ratio (HR) = 1. 08, 95% confidence interval (CI): 0. 92-1. 26]. Similarly, no associations were observed with respect to anatomic location (colon, rectum and recto-sigmoid cancers) and tumor characteristics respectively. There was significant interaction between periodontal disease and diagnosis of colorectal cancer according to hormone therapy (HT) use (p =0. 03), and stratified analyses suggest current HT users, particularly of estrogen plus progestin (E+P), with a history of periodontal disease have a higher risk of being diagnosed with colorectal cancer [HR =1. 76, 95% CI: 1. 20-2. 59]. This effect was enhanced on restriction to colon cancer alone [HR =2. 02, 95% CI: 1. 34-3. 05}. However, dose-response effect was not consistent with time on HT use. Other results from our study indicate that participants with "severe" periodontal disease according to the CDC/AAP Clinical Case Definition demonstrated an almost 2-fold higher odds of having high serum CRP concentrations (>3. 0mg/l), compared to those with no/mild disease, after adjusting for potential confounders (OR 1. 86, 95% CI 1. 06-3. 27). Positive, linear, but statistically insignificant associations were observed between whole mouth mean and worst site PPD and CAL measures. None of the select pathogens examined (alone or in groups), or the presence of active gingival inflammation evidenced by percentage of sites that bled on probing (>50%), were associated with serum hsCRP levels. Also, no significant interaction effects were observed between periodontal disease, and any of the pathogens, (alone or in groups), or mean percentage bleeding sites (>50% cut point), on the serum hsCRP concentrations. Conclusion: Periodontal disease may enhance the risk of being diagnosed with total cancer risk in postmenopausal women; this finding persisted when restricting to never smokers. This risk appears to be higher for certain anatomic sites, particularly those in close proximity to the oral cavity such as the esophagus and upper gastrointestinal regions, but does not appear to extend to lower gastrointestinal tract sites such as the colon and rectum. The observed association between women with periodontal disease who are on hormone therapy and risk of being diagnosed with incident colorectal cancer requires further exploration, and we cannot rule out that it may be due to chance. This study also affirms that chronic inflammation may be one mechanism by which periodontal disease is associated with cancer risk. Additional research in other prospective cohorts is needed.
Author: Shaul Massry Publisher: Springer Science & Business Media ISBN: 1461342171 Category : Medical Languages : en Pages : 611
Book Description
We present to our readers the proceedings of the Second International Workshop on Phosphate. A short account of the history of the effort led to the Phosphate Workshops is appro priate and can be of interest to the reader. The idea for Phosphate Workshops was born in the early days of November, 1974. One of us (S. G. M. ) suggested the thought to a group of scientists gathered for a luncheon in one of the attrac tive small restaurants in Weisbaden, Germany. The purpose of the workshop was to bring together interested scientists to discuss the newer developments and the recent advances in the field of phosphate metabolism and the other related minerals. An Organizing Committee made of Shaul G. Massry (USA), Louis V. Avioli (USA), Philippe Bordier (France), Herbert Fleisch (Switzerland), and Eduardo Slatopolsky (USA) was formed. The First Workshop was held in Paris during June 5-6, 1975 and was hosted by Dr. Philippe Bordier. Its proceeding was already published. The Second Workshop took place in Heidelberg during June 28-30, 1976 and was hosted by Dr. Eberhard Ritz. Both of these workshops were extremely successful scientific endeavors, and the need for them was demonstrated by the great interest they generated among the scientific community. The Or ganizing Committee, therefore, decided to continue with the tradi tion to hold additional Workshops annually or every other year.
Author: Stella Pelengaris Publisher: John Wiley & Sons ISBN: 1444309080 Category : Science Languages : en Pages : 544
Book Description
This comprehensive text provides a detailed overview of the molecular mechanisms underpinning the development of cancer and its treatment. Written by an international panel of researchers, specialists and practitioners in the field, the text discusses all aspects of cancer biology from the causes, development and diagnosis through to the treatment of cancer. Written by an international panel of researchers, specialists and practitioners in the field Covers both traditional areas of study and areas of controversy and emerging importance, highlighting future directions for research Features up-to-date coverage of recent studies and discoveries, as well as a solid grounding in the key concepts in the field Each chapter includes key points, chapter summaries, text boxes, and topical references for added comprehension and review Supported by a dedicated website at www.blackwellpublishing.com/pelengaris An excellent text for upper-level courses in the biology of cancer, for medical students and qualified practitioners preparing for higher exams, and for researchers and teachers in the field
Author: Claudine Burton-Jeangros Publisher: Springer ISBN: 331920484X Category : Medical Languages : en Pages : 215
Book Description
This open access book examines health trajectories and health transitions at different stages of the life course, including childhood, adulthood and later life. It provides findings that assess the role of biological and social transitions on health status over time. The essays examine a wide range of health issues, including the consequences of military service on body mass index, childhood obesity and cardiovascular health, socio-economic inequalities in preventive health care use, depression and anxiety during the child rearing period, health trajectories and transitions in people with cystic fibrosis and oral health over the life course. The book addresses theoretical, empirical and methodological issues as well as examines different national contexts, which help to identify factors of vulnerability and potential resources that support resilience available for specific groups and/or populations. Health reflects the ability of individuals to adapt to their social environment. This book analyzes health as a dynamic experience. It examines how different aspects of individual health unfold over time as a result of aging but also in relation to changing socioeconomic conditions. It also offers readers potential insights into public policies that affect the health status of a population.
Author: Josefine Hirschfeld Publisher: Quintessenz Verlag ISBN: 3868675574 Category : Medical Languages : en Pages : 502
Book Description
The association between periodontitis and systemic diseases has become a hot topic in recent years. This comprehensive book reviews the clinical evidence and biological plausibility of the many systemic diseases that have been linked to periodontitis. Edited by Dr Josefine Hirschfeld and Prof Iain L.C. Chapple, experts in each field discuss the mechanisms at work, citing the available key literature and clearly summarising current knowledge and understanding of the associations between periodontitis and diabetes mellitus, cardiovascular diseases, chronic kidney disease, inflammatory bowel diseases, rheumatoid arthritis, respiratory diseases, pregnancy and fertility, malignancy, neurodegenerative diseases, stress and depression, and autoimmunity. Each chapter critically appraises the existing evidence, providing comprehensive, contemporary and well-considered insights into the clinical evidence and biological plausibility of each condition, as well as the limitations of existing studies and how these can be overcome in the future. Periodontitis and Systemic Diseases: Clinical Evidence and Biological Plausibility is an indispensable reference for both clinicians and researchers.
Author: Neal Halfon Publisher: Springer ISBN: 3319471430 Category : Medical Languages : en Pages : 667
Book Description
This book is open access under a CC BY 4.0 license. This handbook synthesizes and analyzes the growing knowledge base on life course health development (LCHD) from the prenatal period through emerging adulthood, with implications for clinical practice and public health. It presents LCHD as an innovative field with a sound theoretical framework for understanding wellness and disease from a lifespan perspective, replacing previous medical, biopsychosocial, and early genomic models of health. Interdisciplinary chapters discuss major health concerns (diabetes, obesity), important less-studied conditions (hearing, kidney health), and large-scale issues (nutrition, adversity) from a lifespan viewpoint. In addition, chapters address methodological approaches and challenges by analyzing existing measures, studies, and surveys. The book concludes with the editors’ research agenda that proposes priorities for future LCHD research and its application to health care practice and health policy. Topics featured in the Handbook include: The prenatal period and its effect on child obesity and metabolic outcomes. Pregnancy complications and their effect on women’s cardiovascular health. A multi-level approach for obesity prevention in children. Application of the LCHD framework to autism spectrum disorder. Socioeconomic disadvantage and its influence on health development across the lifespan. The importance of nutrition to optimal health development across the lifespan. The Handbook of Life Course Health Development is a must-have resource for researchers, clinicians/professionals, and graduate students in developmental psychology/science; maternal and child health; social work; health economics; educational policy and politics; and medical law as well as many interrelated subdisciplines in psychology, medicine, public health, mental health, education, social welfare, economics, sociology, and law.
Author: Publisher: BoD – Books on Demand ISBN: 1838806784 Category : Medical Languages : en Pages : 191
Book Description
This Edited Volume Periodontology - Fundamentals and Clinical Features is a collection of reviewed and relevant research chapters, offering a comprehensive overview of recent developments in the field. The book comprises single chapters authored by various researchers and edited by an expert active in the dental medicine research area. All chapters are complete in themselves but united under a common research study topic. This publication aims at providing a thorough overview of the latest research efforts by international authors in periodontology, and opening new possible research paths for further novel developments.
Author: Ronnie Levine Publisher: Springer ISBN: 3319982079 Category : Medical Languages : en Pages : 105
Book Description
The first edition of this classic text appeared in 1976 with the aim of refining and standardising the advice given to the public and to ensure that such advice was scientifically sound and evidence-based. It was written not only for members of the dental professions and those involved in general healthcare including medical practitioners, school nurses, health visitors, midwives, dieticians, pharmacists and public health practitioners, but also those who influence health in the wider community, such as teachers, child carers and peer educators. While originally written for a UK readership it became clear that it was used in other countries and that a new international edition was needed. To ensure that this new edition would reflect a consensus of international expert opinion and be relevant to a much broader readership, a panel of eminent experts was enlisted from as far afield as Japan, Singapore, Denmark, Switzerland and the USA. The text is consistent with current evidence and guidance from the WHO, and includes comparative guidance from other countries and systematic reviews of research evidence from the Cochrane Collaboration database. It provides information and advice on the main aspects of oral health, including the cause and prevention of dental caries, periodontal disease, dental erosion, oral cancer and dental problems in children under five, and older people. Throughout the book, key points are given at the beginning of each chapter, with an indication of the strength of supporting scientific evidence using a simple scheme.
Author: Ngozi Nnonyelum Nwizu
Author: Ngozi Nnonyelum Nwizu
Author: Shaul Massry
Author: Stella Pelengaris
Author: Claudine Burton-Jeangros
Author: Josefine Hirschfeld
Author: Neal Halfon
Author: Mario Nava-Villalba
Author: 
Author: Willoughby Dayton Miller
Author: Ronnie Levine