Search

Your search keyword '"Terwiel M"' showing total 13 results
Start Over Author "Terwiel M"
13 results on '"Terwiel M"'

2. Family-centred service: differences in what parents of children with cerebral palsy rate important

Author

Terwiel, M., Alsem, M. W., Siebes, R. C., Bieleman, K., Verhoef, M., Ketelaar, M., ARD - Amsterdam Reproduction and Development, and Rehabilitation medicine

Abstract

BackgroundA family-centred approach to services of children with disabilities is widely accepted as the foundational approach to service delivery in paediatric health care. The 56 items of the Measure of Processes of Care questionnaire (MPOC-56) all reflect elements of family-centred service. In this study, we investigated which elements of family-centred service are rated important by parents of children with cerebral palsy by adding a question on importance to each item of the MPOC-56 (MPOC-56-I). MethodsIn total, 175 parents of children with cerebral palsy completed the MPOC-56-I. For each MPOC item, parents were asked to rate the importance on a 5-point scale ranging from 0 (not important at all) up to and including 4 (very important). We used Spearman's rank correlation coefficient to further explore the variation in parents' importance ratings. ResultsParents' importance ratings of the MPOC-56 items varied. The percentage of parents rating an item important (importance rating 3 or 4) varied between 43.8% and 96.8%. The percentage of parents rating an item unimportant (rating 0 or 1) varied between 0.0% and 20.3%, and the percentage of parents rating an item neutral (rating 2) varied between 3.0% and 36.0%. Most diverse importance ratings were found for five items concerning the provision of general information. Three correlations between these items and child and parent characteristics were found. Six items were rated important by almost all (95%) parents. These items concern elements of specific information about the child, co-ordinated and comprehensive care for child and family and enabling and partnership. ConclusionsParents rate the importance of family-centred services for their situation in various ways. These findings endorse that family-centred services should recognize the uniqueness of families and should be tailored to what parents find important

Published
2017

3. The HOPE (Heart Outcomes Prevention Evaluation) Study: The design of a large, simple randomized trial of an angiotensin converting enzyme inhibitor (ramipril) and vitamin E in patients at high risk of cardiovascular events

Author

Mindlen, F., Nordaby, R., Ruiz, M., Zavala, A., Guzman, L., Martinez, F., Diaz, Rr, Mackey, C., Marino, M., Romero, G., Zapata, G., Cuneo, C., Kawamura, T., Coelho, O., Massayochi, O., Braga, J., Labrunie, A., Bodanese, L., Manenti, E., Vitola, D., Nicolau, J., Amodeo, C., Armaganijan, D., Bertolami, M., Caramelli, B., Carvalho, A., Cirenza, C., Fichino, M., Franken, R., Ghorayeb, N., Kadri, T., Leao, P., Malheiros, F., Pavanello, R., Ramires, F., Ramires, J., Savioli, F., Sousa, A., Tanajura, L., Topps, D., Korner, L., Martinez, V., Baptie, B., Basinger, M., Baylis, B., Beresford, P., Edwards, A., Giannaccaro, P., Groenewoud, Y., Grose, M., Kellen, J., Lam, S., Lesoway, R., Ma, P., Meldrum, D., Mitchell, D., Mitchell, Lb, Roth, D., Shumak, S., Simon, M., Stone, J., Warnica, W., Wyse, D., Neffgen, C., Neffgen, J., Armstrong, F., Armstrong, W., Bell, N., Black, W., Brass, N., Brenneis, F., Brownoff, R., Chaytors, G., Debanne, D., Derksen, C., Donoff, M., Dzavik, V., Goeres, M., Greenwood, P., Gulamhusein, S., Hui, W., Hutchison, K., Kasian, L., Kasza, L., Krikke, E., Kvill, L., Lakhani, Z., Linklater, D., Mackel, J., Martin, S., Montague, T., Moores, D., Musseau, A., Muzyka, T., Paradis, J., Prosser, A., Ryan, E., Senaratne, M., Stenerson, P., Talibi, T., Teo, K., Young, C., Zuk, V., White, R., Browne, K., Browne, M., Happel, K., Irving, A., Plesko, A., Donnelly, R., Radomsky, N., Felker, P., Larsen, D., Morse, J., Rowntree, C., Thompson, J., Wedel, R., Bloomberg, G., Chomin, G., Dahl, M., Leong, W., Moy, V., Heath, J., Marshall, J., Terwiel, M., Kenefick, G., Kuritzky, R., Stevens, K., Weddings, K., Barban, K., Imrie, J., Woo, K., Ashton, T., Calvert, K., Bishop, W., Sweeney, R., Breakwell, L., Kornder, J., Pearce, S., Polasek, P., Richardson, P., Ghosh, S., Rielly, M., Wagner, K., Bemstein, V., Dawson, K., Lee, P., Lewis, J., Macdonald, K., Mcgee, L., Thompson, C., Hilton, D., Illott, K., Klinke, P., Mcconnell, J., Rabkin, S., Ong, A., Ong, G., Bedard, D., Hoeschen, R., Mehta, P., Mohammad, I., Morris, A., Bessoudo, R., Dobbins, N., Mclellan, L., Milton, J., Davis, R., Okeefe, D., Smith, R., Joyce, C., Parsons, M., Skanes, J., Sussex, B., Tobini, M., Ravalia, M., Sherman, G., Worrall, G., Atkinson, A., Hatheway, R., Johnson, B., Barnhill, S., Bata, I., Cosseet, J., Johnstone, D., Macfarlane, M., Sheridan, W., Crossman, L., Folkins, D., Shirley, M., Machel, T., Morash, J., Gupta, M., Mayich, M., Vakani, T., Baitz, T., Macphee, E., Turton, E., Turton, M., Chan, N., Misterski, J., Raco, D., Curnew, G., Fallen, E., Finkelstein, L., Gerstein, H., Hardman, P., Lawand, S., Lonn, E., Magi, W., Mcqueen, M., Panju, A., Patterson, R., Sullivan, B., Sullivan, H., Sullivan, M., Taylor, K., Worron, I., Yusuf, S., Cameron, W., Noseworthy, C., Houlden, R., Lavalle, T., Fowlis, R., Janzen, I., Arnold, M., Cann, M., Carroll, S., Dumaresq, S., Edmonds, M., Furlong, P., Geddes, C., Graham, E., Harris, K., Hramiak, I., Kennedy, R., Kostuk, W., Krupa, M., Lent, B., Lovell, M., Maclean, C., Massel, D., Mcmanus, R., Mcsherry, J., Munoz, C., Occhipinti, J., Oosterveld, L., Pflugfelder, P., Powers, S., Southern, R., Spence, D., Squires, P., Wetmore, S., Willing, J., Wisenberg, G., Wolfe, B., Kannampuzha, P., Rebane, T., Sluzar, V., Hess, A., Chan, Y., Thomson, D., Baigrie, R., Dubbin, J., Liuni, C., Tan, Kw, Brankston, E., Hewson, P., Hrycyshyn, B., Kapusta, W., Knox, L., Lockner, C., Whitsitt, P., Baird, M., Conroy, D., Davies, Ra, Davies, Rf, Fraser, M., Hagar, S., Hierlihy, P., Keely, E., Khan, S., Lau, Dgw, Marois, L., Nemeth, K., Reeves, E., Turek, M., Vexler, R., Young, D., Kumar, G., Kuruvilla, G., Kuruvilla, P., Lowe, D., Kwok, K., Blakely, J., Styling, S., Bozek, B., Charles, J., Fell, D., Fell, Da, Goode, E., Grossman, Ld, Matthews, E., Nitkin, R., Ricci, J., Selby, A., Singh, N., Swan, J., Emmett, J., Weingert, M., Ganjavi, F., Hill, D., Nawaz, S., Hessian, R., Kwiatkowski, K., Lai, C., Mulaisho, C., Okeefe, H., Smith, H., Weeks, A., Andrews, J., Barnie, A., Drobac, M., Hacker, P., Hanna, A., Iwanochko, M., Kenshole, A., Langer, A., Liu, P., Maclean, S., Moe, G., Sasson, Z., Sternberg, L., Trachuk, C., Walters, J., Zinman, B., Cheung, M., Cina, C., Yao, L., Man, K., Fulop, J., Glanz, A., Sibbick, M., Carter, P., Hickey, J., Mcmillian, E., Dion, D., Sthilaire, R., Coutu, D., Damours, G., Starra, R., Brooks, J., Dechamps, P., Kiwan, G., Kouz, S., Laforest, M., Remillard, C., Bellamy, D., Brossoit, R., Carrier, S., Houde, A., Labonte, I., Belanger, A., Kandalaft, N., Quenneville, L., Sandi, M., Auger, P., Bilodeau, N., Delage, F., Dumont, F., Giroux, R., Loisel, R., Poirier, C., Saulnier, D., Carmichael, P., Lemay, C., Lenis, J., Arisjilwan, N., Bedard, H., Casavant, C., Chiasson, J., Dagenais, D., Fitchett, D., Gossard, D., Halle, H., Hamel, N., Joyal, M., Magnan, O., Methe, M., Pedneault, L., Pilon, C., Poisson, D., Primeau, L., Rondeau, C., Roy, C., Ruel, M., Serpa, A., Sestier, F., Smilovitch, M., Theroux, P., Beaudoin, J., Boudreault, Jr, D Amours, D., Douville, T., Giguere, G., Houde, G., Labbe, R., Lachance, S., Lessard, L., Mercier, G., Noel, Hp, Talbot, P., Tremblay, J., Karabatsos, A., Maclellan, K., Wilson, P., Bogaty, P., Laforge, D., Langlais, M., Leblanc, M., Samson, M., Turcotte, J., Campeau, J., Dupuis, R., Lauzon, C., Ouimet, F., Pruneau, G., Desmaris, C., Frechetto, I., Gervais, P., James Brophy, Leroux, S., Bester, S., Meunier, L., Sayeed, M., Hart, M., Moumne, I., Thomasse, G., Walker, J., Walker, M., Ahmed, S., Habib, Nm, Kuny, P., Lopez, J., Klein, W., Grisold, M., Heyndrickx, L., Fiasse, A., Degaute, Jp, Mockel, J., Duprez, D., Chaudron, Jm, Bodson, A., Krzentowski, G., Boland, J., Kolendorf, K., Winther, B., Juhl, H., Hamalainen, T., Siitonen, O., Gin, H., Rigalleau, V., Hensen, J., Riel, R., Oehmenbritsch, R., Schulzeschleppinghoff, B., Hopf, R., Moller, A., Rosak, C., Wetzel, H., Hasslacher, C., Martin, T., Stein, J., Erdmann, E., Bohm, M., Hartmann, D., Breidert, M., Fritzen, R., Scherbaum, W., Mann, J., Maus, J., Schroeder, C., Henrichs, H., Unger, H., Ickenstein, G., Kromer, E., Riegger, G., Schunkert, H., Basan, B., Hampel, R., Crean, P., Garadah, T., White, U., Marini, N., Paciaroni, E., Saccomano, G., Diluzio, S., Magnani, B., Mantovani, B., Pareschi, P., Stucchi, N., Nanni, D., Rusticali, F., Simoni, C., Brunelli, C., Caponnetto, S., Gatto, E., Mazzantini, A., Molinari, O., Morello, R., Degiorgio, L., Imparato, C., Barbaresi, F., Cotogni, A., Pasqualini, M., Frigeni, G., Landoni, M., Polese, A., Cernigoi, A., Merni, M., Tortul, C., Velussi, M., Aina, F., Cernigliaro, C., Dellavesa, P., Dejoannon, U., Pierfranceschi, G., Zavaroni, D., Emilia, R., Manicardi, E., Minelli, E., Penazzoli, F., Portioli, I., Rossi, E., Giani, P., Roccaforte, R., Casaccia, M., Larovere, R., Miglierina, E., Repetto, S., Centofante, P., Vincenzi, M., Nieuwenhuijzen, Ac, Sels, J., Wolffenbuttel, Bhr, Kip, J., Mantingh, L., Mulder, H., Vandoorn, Lg, Hjerkinn, E., Reikvam, A., Cardona, M., Sanz, G., Karoni, A., Bescos, Ll, Albert, X., Masia, R., Alvarez, A., Saenz, L., Astrom, L., Press, R., Sjostedt, P., Tabrizi, F., Bergbom, I., Hansson, P., Held, C., Kahan, T., Ryden, B., Andersson, O., Wysocki, M., Karlsson, E., Sartor, G., Smith, L., Katzman, P., Ljungdahl, L., Noren, P., Hallberg, A., Olsson, Po, Asbrink, S., Molgaard, J., Nilsson, V., Nystrom, F., Ohman, P., Andersson, C., Ekholm, L., Svensson, Ka, Torebo, E., Fagher, B., Svenstam, I., Thulin, T., Ericsson, Ub, Ahnberg, K., Henning, R., Jacobsson, L., Taghavi, A., Ahlstrom, P., Rosenqvist, U., Ericson, C., Gertow, O., Kristensson, Be, Stahl, L., Bergsten, L., Harden, R., Jagren, C., Leijd, B., Lennerhagen, P., Ostergrens, J., Sandstrom, V., Sundelin, R., Hagg, A., Morlin, C., Pettersson, F., Wanders, A., Bjorkman, H., Karlsson, G., Larsson, H., Lonndahl, Y., Weber, P., Cozzi, R., Gerber, P., Moccetti, T., Safwan, E., Sessa, F., Binder, T., Boman, P., Kiowski, W., Lehman, R., Lull, B., Spinas, G., Jamieson, A., Kennedy, Ja, Kesson, C., Gryczka, R., Parker, P., Sidiki, S., Small, M., Struthers, S., Manns, J., Smithurst, H., Begg, A., Fisher, Bm, Bedford, C., Heller, S., Marlow, S., Munoz, Ec, Garcia, Hh, Ruiz, Ro, Meaney, E., Flores, Mi, Brown, E., Perry, G., Patel, G., Sarma, R., Szlachcic, Y., Dorman, J., Singh, B., Bailey, G., Clegg, L., Horwitz, L., Leahy, J., Rashkow, A., Hudson, M., Miller, A., Umberger, J., Zoble, R., Orander, P., Sridharan, M., Defrancisco, G., Davidson, M., Islam, N., Mathew, J., Rajanahally, R., French, D., Wickemeyer, W., Effron, M., Goldstein, M., Utley, K., Pierpont, G., Weigenant, J., Farkouh, M., Kubly, V., Rich, M., Wisneski, L., Abrams, J., Garcia, D., Bonora, M., Kohn, R., Muffoletto, E., Brink, D., Lader, E., Singler, A., Pande, P., Powers, J., Hoogwerf, B., Moore, J., Yanak, F., Gupta, S., Williams, D., Danisa, K., Kirk, C., Wescott, B., Grover, J., Mackenzie, M., Amidi, M., Bell, M., Farmer, J., Kingry, C., Young, J., Harms, V., Kennedy, Jw, Letterer, R., Heller, C., and Mack, R.

5. Family history of pulmonary fibrosis impacts prognosis in patients with sarcoidosis.

Author

Planté-Bordeneuve T, Terwiel M, van der Vis JJ, van Es W, Veltkamp M, Grutters JC, and van Moorsel CHM

Abstract

Having a family member with pulmonary fibrosis (PF) impacts the prognosis of sarcoidosis patients, as the majority of patients reporting at least one relative with PF present fibrotic characteristics and one-third develop a progressive phenotype https://bit.ly/40KC7Cr., Competing Interests: Conflict of interest: T. Planté-Bordeneuve reports support for the present manuscript from Bourse de Perfectionnement Fondation Mont Godinne, Fondation Médicale Horlait-Dapsens, and Bourse d'Excellence WBI World; and advisory board meeting fees from Boehringer Ingelheim, outside the submitted work. C.J.M. van Moorsel reports grants from Boehringer Ingelheim outside the submitted work; speaker fees from Boehringer Ingelheim outside the submitted work; and is cochair of the ClinGen ILD gene curation expert panel, disclosure made outside the submitted work. M. Veltkamp reports payment or honoraria for lectures, presentations, speakers’ bureaus, manuscript writing or educational events from Chiesi Pharmaceuticals outside the submitted work; and payment for expert testimony from Boehringer Inghelheim outside the submitted work. W. van Es reports payment or honoraria for lectures, presentations, speakers’ bureaus, manuscript writing or educational events from Boeringher Ingelheim outside the submitted work. M. Terwiel, J.J. van der Vis and J.C. Grutters have nothing to disclose., (Copyright ©The authors 2025.)

Published
2025
Full Text
View/download PDF

6. Genetic testing in interstitial lung disease: An international survey.

Author

Terwiel M, Borie R, Crestani B, Galvin L, Bonella F, Fabre A, Froidure A, Griese M, Grutters JC, Johannson K, Kannengiesser C, Kawano-Dourado L, Molina-Molina M, Prasse A, Renzoni EA, van der Smagt J, Poletti V, Antoniou K, and van Moorsel CHM

Subjects
Genetic Testing, Humans, Pulmonologists, Surveys and Questionnaires, Idiopathic Pulmonary Fibrosis diagnosis, Lung Diseases, Interstitial diagnosis, Lung Diseases, Interstitial genetics
Abstract

Background and Objective: Genetic analysis is emerging for interstitial lung diseases (ILDs); however, ILD practices are not yet standardized. We surveyed patients', relatives' and pulmonologists' experiences and needs on genetic testing in ILD to evaluate the current situation and identify future needs., Methods: A clinical epidemiologist (MT) together with members of the ERS taskforce and representatives of the European Idiopathic Pulmonary Fibrosis and related disorders Federation (EU-IPFF) patient organisation developed a survey for patients, relatives and pulmonologists. Online surveys consisted of questions on five main topics: awareness of hereditary ILD, the provision of information, genetic testing, screening of asymptomatic relatives and clinical impact of genetic analysis in ILD., Results: Survey respondents consisted of 458 patients with ILD, 181 patients' relatives and 352 pulmonologists. Most respondents think genetic testing can be useful, particularly for explaining the cause of disease, predicting its course, determining risk for developing disease and the need to test relatives. Informing patients and relatives on genetic analysis is primarily performed by the pulmonologist, but 88% (218) of pulmonologists identify a need for more information and 96% (240) ask for guidelines on genetic testing in ILD. A third of the pulmonologists who would offer genetic testing currently do not offer a genetic test, primarily because they have limited access to genetic tests. Following genetic testing, 72% (171) of pulmonologists may change the diagnostic work-up and 57% (137) may change the therapeutic approach., Conclusion: This survey shows that there is wide support for implementation of genetic testing in ILD and a high need for information, guidelines and access to testing among patients, their relatives and pulmonologists., (© 2022 Asian Pacific Society of Respirology.)

Published
2022
Full Text
View/download PDF

7. Clustering of lung diseases in the family of interstitial lung disease patients.

Author

Terwiel M, Grutters JC, and van Moorsel CHM

Subjects
Cluster Analysis, Humans, Emphysema, Idiopathic Pulmonary Fibrosis epidemiology, Lung Diseases, Interstitial epidemiology, Lung Neoplasms
Abstract

Background: The presence of familial interstitial lung disease (ILD) has been found to predict development of progressive pulmonary fibrosis. However, the role of non-ILD lung diseases in ILD patients' families has not yet been investigated. We aimed to identify associations between ILDs and non-ILD lung diseases from ILD patients' self-reported family health history., Methods: We analysed questionnaires on family health history of 1164 ILD patients for the occurrence of ILD and non-ILD lung disease in relatives. Logistic regression analysis was used to study associations with diagnosis groups., Results: Familial pulmonary fibrosis was reported by 20% of patients with idiopathic pulmonary fibrosis (IPF; OR 9.2, 95% CI 4.7-17.9), and 15% of patients with unclassifiable pulmonary fibrosis (OR 4.1, 95% CI 2.0-8.2). Familial occurrence was reported by 14% of patients with sarcoidosis (OR 3.3, 95% CI 1.9-5.8). Regarding non-ILD lung disease, significantly more patients with IPF (36%) reported lung cancer in their family (OR 2.3, 95% CI 1.4-3.5), and patients with hypersensitivity pneumonitis (18%) mostly reported COPD (OR 2.3, 95% CI 1.3-4.2). Comparison of sporadic and familial ILD patients' reports showed that emphysema (OR 4.6, 95% CI 1.8-11.6), and lung cancer (OR 2.4, 95% CI 1.2-4.9) were predictive for familial pulmonary fibrosis, particularly when reported both in a family (OR 16.7, 95% CI 3.2-86.6; p < 0.001)., Conclusions: Our findings provide evidence for clustering of ILD and non-ILD lung diseases in families and show that self-reported emphysema and lung cancer of relatives in this population predicts familial pulmonary fibrosis., (© 2022. The Author(s).)

Published
2022
Full Text
View/download PDF

9. Risk and outcome of COVID-19 infection in sarcoidosis patients: results of a self-reporting questionnaire.

Author

Baughman RP, Lower EE, Buchanan M, Rottoli P, Drent M, Sellares J, Terwiel M, Elfferich M, Francesqui J, Barriuso Cabrerizo MR, Sweiss N, Martone F, Al-Hakim T, and Judson MA

Abstract

Background: It has been suggested that sarcoidosis patients, especially those on immunosuppressive medications, are at increased risk for COVID-19 infection and more severe disease., Methods: A questionnaire was developed in four languages (English, Dutch, Italian, and Spanish). The questionnaire queried whether patients had been infected with COVID-19 and outcome of the infection. Risk factors for COVID-19 infection were collected., Results: A total of 5200 sarcoidosis patients completed the questionnaire with 116 (2.23%) reporting infection and 18 (15.8%) required hospitalization. Increased hazard ratio (HR) for COVID-19 infection were seen for those with a COVID-19 infected roommate (HR=27.44, p<0.0001), health care provider (HR=2.4, p=0.0001), pulmonary sarcoidosis (HR=2.48, p=0.001), neurosarcoidosis (HR=2.02, p<0.01), or rituximab treatment (HR=5.40, p<0.0001). A higher rate of hospitalization was found for those with underlying heart disease (HR=3.19 (1.297-7.855), p<0.02). No other feature including race, other immunosuppressive agent, age, or underlying condition was associated with a significant increased risk for infection or more severe disease., Conclusion: The overall rate of COVID-19 was 2.23%, suggesting an increased rate of COVID-19 infection. However, when an analysis of the questionnaires of sarcoidosis and non-sarcoidosis patients was performed in one localized area over this time period, the rate of COVID-19 infection was similar in both groups. Sarcoidosis patients who cohabitated with COVID-19 infected individuals, worked in health care, had pulmonary or neurologic sarcoidosis, or were treated with rituximab had an increased risk for COVID-19 infection. No significant increased risk for hospitalization could be identified based on age, race, gender or any specific immunosuppressive treatment. (Sarcoidosis Vasc Diffuse Lung Dis 2020; 37 (4): e2020009) ., (Copyright: © 2020 SARCOIDOSIS VASCULITIS AND DIFFUSE LUNG DISEASES.)

Published
2020
Full Text
View/download PDF

11. Clustering of immune-mediated diseases in sarcoidosis.

Author

Terwiel M, Grutters JC, and van Moorsel CHM

Subjects
Cluster Analysis, Humans, Autoimmune Diseases immunology, Autoimmunity, Sarcoidosis immunology
Abstract

Purpose of Review: Sarcoidosis is an immune-mediated disease of unknown cause. Immune-mediated diseases appear to cluster in patients and in families. We review what is known on this topic for sarcoidosis, and what factors may underlie disease clustering., Recent Findings: In populations of patients with sarcoidosis, relative risk estimates of Sjögren's syndrome, systemic lupus erythematosus, autoimmune hepatitis, ankylosing spondylitis, multiple sclerosis (MS), celiac disease, autoimmune thyroid disease, and ulcerative colitis, varied between 2.1 and 11.6. In relatives of patients with sarcoidosis, relative risk estimates varied between 1.3 and 5.8 for sarcoidosis, MS, celiac disease, type 1 diabetes, Graves' disease, rheumatoid arthritis, Crohn's disease, and ulcerative colitis. Shared risk loci in key immunological pathways provide evidence for a contribution to development of multiple diseases. Identical changes in the immune status, epigenetic alterations, and environmental triggers have been detected in several diseases, and drug-induced disease is likely responsible for a small portion of co-occurring disease., Summary: Clustering of sarcoidosis and other immune-mediated diseases in patients and in their relatives occurs for sarcoidosis, MS, celiac disease, Graves' disease, and ulcerative colitis. Further research is needed to substantiate causal links and risk estimates in patients and their relatives.

Published
2019
Full Text
View/download PDF

12. Clinical epidemiology of familial sarcoidosis: A systematic literature review.

Author

Terwiel M and van Moorsel CHM

Subjects
Black or African American genetics, Family, Female, Humans, Ireland ethnology, Male, Netherlands ethnology, Prevalence, Risk Factors, Sarcoidosis diagnosis, White People genetics, Clinical Decision-Making methods, Ethnicity genetics, Genetic Predisposition to Disease ethnology, Sarcoidosis epidemiology
Abstract

Introduction: Although the presence of familial sarcoidosis has been confirmed, clinical and epidemiological data on its characteristics are scattered and sometimes paradoxical. The objective of this review is to assess what is known on the clinical epidemiology of familial sarcoidosis, by combining data from early case reports with recent population based data; aiming to support in clinical decision making and providing information to patients., Method: A systematic review of the literature in PubMed was done and 27 studies with clinical or epidemiological data on familial sarcoidosis, published between 1947 and 2017, were included., Results: The pooled prevalence proportion of familial sarcoidosis, based on twelve study populations, was 9.5% (CI 4.6-16.1), highest in French, African American, Dutch and Irish patients. A heritability of 60-70% was estimated in diverse studies. Relative types and relationships most often reported in familial sarcoidosis were siblings and mother-child relationships. Familial risk is heterogeneous. In African Americans specific environmental factors have been associated with familial sarcoidosis (OR between 1.5 and 3.2). European American and African American subjects had different relative risks for first degree familial relationships (OR of 16.6 vs 3.1) and relative risk differed between relative types. Clinical findings in familial sarcoidosis are still obscure., Conclusions: Prevalence of familial sarcoidosis is high in specific study populations from countries worldwide. The estimated heritability of 60-70%, suggests a shared determinant, and the heterogeneous familial risk, associated with both genetic and environmental factors. Familial relative risks and clinical phenotypes may differ between ethnic groups and relative types, but require further study., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published
2019
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results