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Dive into the research topics where Marc H. Lebel is active.

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Featured researches published by Marc H. Lebel.


Clinical Infectious Diseases | 1999

Epidemiological Features of Pertussis in Hospitalized Patients in Canada, 1991- 1997: Report of the Immunization Monitoring Program—Active (IMPACT)

Scott A. Halperin; Elaine E. L. Wang; Barbara Law; Elaine L. Mills; Robert Morris; Pierre Déry; Marc H. Lebel; Noni MacDonald; Taj Jadavji; Wendy Vaudry; David W. Scheifele; Gilles Delage; Philippe Duclos

To assess the morbidity associated with the continued high levels of pertussis, we studied all children <2 years of age who were admitted to the 11 Immunization Monitoring Program--Active (IMPACT) centers, which constitute 85% of Canadas tertiary care pediatric beds. In the 7 years preceding implementation of acellular pertussis vaccine, a total of 1,082 pertussis cases were reported, of which 49.1% were culture-confirmed. The median age of the patients was 12.4 weeks; 78.9% of cases were in children <6 months of age. Complications of pertussis were common: pneumonia was reported in 9.4% of cases, new seizures in 2.3%, and encephalopathy in 0.5%. There were 10 deaths (0.9%), all in children < or =6 months of age. Duration of hospitalization was longer (9.3 days vs. 4.9 days; P = .001) and intensive care was required more frequently (19.2% vs. 4.9%; P = .001) in infants under <6 months of age than in those > or =6 months. Pertussis continues to cause significant morbidity and occasional mortality in Canada, particularly in young infants.


Clinical Infectious Diseases | 2003

A Pharmacoeconomic Evaluation of 7-Valent Pneumococcal Conjugate Vaccine in Canada

Marc H. Lebel; James D. Kellner; E. Lee Ford-Jones; Kyle Hvidsten; Edward C. Y. Wang; Vincent Ciuryla; Steve Arikian; Roman Casciano

The objective of this study was to evaluate the projected health benefits, costs, and cost-effectiveness of pneumococcal conjugate vaccination for infants and children aged <5 years in Canada. A health state model incorporating incidence, vaccine efficacy, costs, and transitional probabilities for the health states (well, meningitis, bacteremia, otitis media, pneumonia, and death) was constructed for a 10-year time horizon. Implementation of a pneumococcal conjugate vaccine program in Canada for each annual birth cohort of 340,000 persons observed over 10 years would be expected to save approximately 12 lives and 100,000 cases of pneumococcal disease over 10 years, resulting in total savings of


Pediatric Infectious Disease Journal | 2000

Leukocytosis in children with Escherichia coli O157:H7 enteritis developing the hemolytic-uremic syndrome.

Chantal Buteau; François Proulx; Mahamadou Chaibou; Didier Raymond; Marie José Clermont; Michele M. Mariscalco; Marc H. Lebel; Ernie Seidman

67 million (Canadian dollars [Can


Canadian Journal of Neurological Sciences | 1987

Congenital malformations associated with maternal use of valproic acid.

Celine Huot; Marie Gauthier; Marc H. Lebel; Albert Larbrisseau

]). Vaccination of healthy infants would result in net savings for society if the vaccine costs less than Can


Clinical Infectious Diseases | 2014

The impact of the meningococcal serogroup C conjugate vaccine in Canada between 2002 and 2012

Manish Sadarangani; David W. Scheifele; Scott A. Halperin; Wendy Vaudry; Nicole Le Saux; Raymond S. W. Tsang; Julie A. Bettinger; N. Bridger; Robert Morris; S. Halperin; Karina A. Top; Pierre Déry; Dorothy Moore; Marc H. Lebel; N. Le Saux; Dat Tran; Lee Ford-Jones; Joanne Embree; Barbara Law; R. Tsang; Ben Tan; W. Vaudry; Taj Jadavji; Otto G. Vanderkooi; D. Scheifele; Laura J. Sauvé; J. Bettinger

50 per dose. Moreover, for a vaccine purchase price of Can


Journal of Paediatrics and Child Health | 2007

Prevalence of positive tuberculin skin tests in foreign‐born children

Kristine Fortin; A Carceller; Monique Robert; Isabelle Chevalier; Valérie Lamarre; Marc H. Lebel

67.50, infant vaccination would cost society Can


Journal of Clinical Microbiology | 2014

Characterization of Multiple Cytomegalovirus Drug Resistance Mutations Detected in a Hematopoietic Stem Cell Transplant Recipient by Recombinant Phenotyping

Emilien Drouot; Jocelyne Piret; Marc H. Lebel; Guy Boivin

79,000 per life-year gained. Pneumococcal conjugate vaccination is a potentially cost-effective means of pneumococcal disease prevention.


Journal of Paediatrics and Child Health | 2008

Antibiotic prophylaxis for childhood urinary tract infection: A national survey

Isabelle Chevalier; Geneviève Benoit; Marie Gauthier; Véronique Phan; Anne-Claude Bernard Bonnin; Marc H. Lebel

Background. Fewer than 10% of children with Escherichia coli O157:H7 enteritis develop hemolytic‐uremic syndrome (HUS). Objective. To determine whether circulating leukocytes are independent risk markers of developing HUS during E. coli O157:H7 enteritis. Methods. We reviewed the charts of all children with culture‐proved E. coli O157:H7 infections seen at Sainte‐Justine Hospital between 1987 and 1997. Epidemiologic data, laboratory indices and circulating leukocytes counts were noted. HUS diagnosis was validated with independent HUS patient lists from the pediatric nephrology services of tertiary care hospitals in the Montreal metropolitan area. The date of onset of enteritis was determined by two independent observers. Leukocyte counts were compared among the following independent groups: (1) uncomplicated O157:H7 enteritis (Group 1); (2) O157:H7 enteritis with the subsequent development of HUS (Group 2); (3) HUS already present at the time of medical consultation (Group 3). Results. There were 369 children with E. coli O157:H7 infection. A complete blood count was not performed in 114 (31%) patients. Observers disagreed on the date of onset of gastroenteritis in 34 (9%) children only (kappa 0.92). The study population thus included 221 patients: Group 1, n = 161; Group 2, n = 27; and Group 3, n = 33. Patients developing HUS (Group 2) presented greater total leukocyte (P < 0.008), polymorphonuclear (P < 0.008) and monocyte (P < 0.07) counts than those with an uncomplicated course (Group 1). Logistic regression analysis showed that young age [odds ratio (OR), 0.98; 95% confidence interval (CI), 0.96 to 0.99], duration of enteric prodrome ≤3 days (OR 4.8, 95% CI 1.13 to 20.7) and initial leukocytosis (OR 1.22, 95% CI, 1.11 to 1.35) were independent predictors of HUS. Conclusions. Based on the variables identified above, further studies are needed to determine whether the inflammatory response of the host represents only a marker of the severity of gastrointestinal infection or whether, alternatively, it is a pathophysiologic factor that leads to HUS.


Anales De Pediatria | 2005

Nuevas tendencias de la endocarditis pediátrica

A Carceller; Marc H. Lebel; G Larose; C Boutin

Two children born with birth defects after intrauterine exposure to valproic acid are reported. The mothers took the drug throughout pregnancy as sole treatment for primary generalized epilepsy. The first baby showed facial dysmorphism, arachnodactyly and triphalangeal thumbs. The second had facial dysmorphism, severe laryngeal hypoplasia, tracheomalacia and an aberrant innominate artery that caused tracheal compression. A left superior vena cava, abnormal pulmonary lobulation, and unilateral hydronephrosis were also found at autopsy. Valproic acid has probable teratogenic potential in humans but the number of reported cases is few and the spectrum of anomalies is broad so it is not possible to delineate a definite fetal valproate syndrome.


The Journal of Pediatrics | 1992

Uvulitis and supraglottitis: Early manifestations of Kawasaki disease

Azimuddin Kazi; Marie Gauthier; Marc H. Lebel; Catherine Ann Farrell; Jacques Lacroix

BACKGROUND Before 2001, the incidence of invasive meningococcal disease (IMD) in Canada was 1.0 per 100 000 per year, with 40% of cases caused by serogroup C organisms. During 2001-2005 all provinces introduced the meningococcal serogroup C conjugate vaccine (MCCV) into their routine infant immunization schedule. METHODS Active, prospective, population-based surveillance of IMD in children and adults was conducted by the Canadian Immunization Monitoring Program, ACTive (IMPACT) during 2002-2012. Inclusion criteria were admission to hospital and identification of Neisseria meningitidis from a sterile site. Incidence was estimated using population census data from Statistics Canada. RESULTS Prior to MCCV introduction, serogroup C disease incidence was 0.07-0.25 per 100 000 per year depending on the province. Following vaccine introduction, serogroup C disease decreased to <0.05 per 100 000 per year, with a reduction of 14% per year (P = .0014). A decrease occurred in all provinces, despite differing schedules being implemented. The largest decrease of 83% (from 0.27 to 0.05 per 100 000 per year) occurred in the 15-24 year age group (P = .0100) who were not vaccinated in all provinces. There was no impact on the incidence of nonserogroup C disease over the same period (P = .9811). CONCLUSIONS MCCV dramatically reduced the incidence of serogroup C IMD in Canada through both direct and indirect effects. The observation that disease incidence decreased with different schedules suggests that the doses at 12 months (common to all provinces) and adolescence (7 of 8 provinces studied) were critical in achieving disease control.

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A Carceller

Université de Montréal

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Marie Gauthier

Université de Montréal

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Bruce Tapiero

Université de Montréal

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Monique Robert

Université de Montréal

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Barbara Law

University of Manitoba

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