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1. Antenna Scattering and Design Considerations

Author

Larry F. Pellett, Douglas Pasquan, and Oren B. Kesler

Subjects
Physics, Microstrip antenna, Optics, Coaxial antenna, business.industry, Antenna measurement, Antenna factor, Antenna (radio), Omnidirectional antenna, business, Radiation pattern, Antenna efficiency
Published
2007
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3. Comparison of DNA detection methods

Author

C.-M. Ng, J Wade, F. Pellett, C. Daniel, and A. van Oosterwijk

Subjects
Dna detection, Immunology, Immunology and Allergy, General Medicine, Computational biology, Mathematics
Published
1994
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4. Contents, Vol. 22, 1978

Author

N.E. Morton, P. Pierce, K. Simola, C.E. Wright, E.J. Yunis, M.E. Chandler, H. Vriesendorp, B.J.B. Keats, C.J. Sherr, K. Bender, R.E. Magenis, H. Oie, B.B. Knowles, J.M. Luciani, M.P. Cowmeadow, I.L. Hansteen, M. Bobrow, G.A. Koch, M. Prensky, P.A. Lalley, N. Shimizu, E.A. Nichols, J. Garver, K. Hirschhorn, A. Brøgger, A.F. Gazdar, S. Hempfling, L.C. Yu, B. Pernis, R. Mausner, S. Leupe-de Smit, R.C.P. Go, A. Westerveld, L. R. Weitkamp, K.E. Toomey, D. Borgaonkar, S. Piomelli, D. Bootsma, T. Campana, E.W. Lovrien, O.J. Miller, H.J. Cooke, F.T. Kao, D.A. Aitken, S. Burgess, L.L. Haley, Y. Boyd, A. Mayerová, T.B. Shows, H.J. Evans, J. Fraisse, K.-H. Grzeschik, V.M. Regina, K.C. Atwood, L.M.M. Wijnen, Liao Law, H.-H. Ropers, M.A. Ferguson-Smith, M.A. Pellegrino, T. Gedde-Dahl, V.A. McKusick, A.C. Leary, J. H. Olving, M.G. Byers, D. Swallow, K.M. Overton, W.F. Witterland, J. Hemmerling, S.J. Funderburk, A. de la Chapelle, N.R. Mendell, U. Francke, Veronica van Heyningen, A.F. Naylor, I.W. Craig, A. Heiberg, R.S. Lemons, J.E. Gray, E. Herbschleb-Voogt, J.J. Yunis, D.B. Amos, C.K. Eun, J.L. Hamerton, L. U. Lamm, N. Oliver, S. Goodnight, F. Pellett, T.M. Dijksman, J.M. Vance, R.E. Eisenman, P. Rubinstein, A. Bratlie, G.A.P. Bruns, V. Kirton, R. Roos, D.L. Slate, M.C. Yoshida, D.L. George, R.C. Schwartz, K.E. Buckton, A.S. Henderson, R. Jonassen, J.A. Robinson, P.L. Pearson, M. Hultén, E. Solomon, A.E. Greene, L.Y. Wang, R. Lange, S. Brown, M.L. Schroeder, P. Karli, A. Krüger, J.M. Robert, B. Lauras, J. Chamberlin, A. Shalev, J. Ott, B.J. Mintz, Elizabeth B. Robson, Per Teisberg, N. Tanigaki, P. M. Conneally, S. Rosenfeld, A.S. Baim, M.L. Rivas, J.A. Brown, R. Johannsmann, N. Suciu-Foca, R. Mierau, T.T. Puck, C.G. Palmer, S.J. Jeremiah, D. Warburton, M. Devictor-Vuillet, J.A. Norton, T. Ho, J.E. Noades, F. Varricchio, E.H.Y. Chu, B. Carritt, R. Schwab, I. Balazs, J. Reiss, C.N. Fear, S. Povey, Erik Thorsby, A. Siverts, D.W. Ball, W. Stanley, L.R. Weitkamp, M.E. Duncan, C. Jones, K. Willecke, S. Philipps, R. Moreland, D.C. Rao, E. Tolley, T. Philip, E. Johnston, M. Monteba-van Heuvel, A.D. Merritt, T.H. Roderick, R.L. Eddy, S. Arias, R.A. Fisher, M.A. Craft, J.H. Edwards, M.C. Sparkes, N.C. Sun, L. Korsnes, D.A. Meyers, M.Y. Tsai, A.W. Johnston, A. Estop, B.M. Turner, K. Berg, S. Guttormsen, W.G. Burgerhout, A.P. Goggin, T. Mohandas, W.K. Stanford, C.W. Bazinet, M. Siniscalco, R.H. Lindenbaum, H.P. Klinger, W.S. Volkers, J. Gavin, K.K. Namboodiri, M.T. Davisson, P.J. McAlpine, W.R.T. Los, M. Meisler, L.J. Donald, F.H. Ruddle, W. Bauch, Timothy A. Donlon, C.R.Y. Sun, R. Bigley, R.S. Sparkes, H. Kaita, P.S. Gerald, E.R. Giblett, I. Berczi, R.C. Elston, S.J. O’Brien, C.T. Falk, L. Scrafford-Wolff, M. Smith, M.K. Fagerhol, J. de Witt, S. Rowe, D. Cox, E.S. Seravalli, T. Borun, M. Lewis, R. Saisson, M.A. Pericak-Vance, R.T. Taggart, R.D.G. McKay, M. Mota, W. R. Mayr, Matthew Parks, F. Freycon, Y. Shimizu, B. Hellkuhl, D.P. Aden, C.A. Slaughter, J.E. Anderson, E. Lovrien, R.M. Denney, N. Lamvik, J. Parekh, B.P. Dorman, A.P.M. Jongsma, M.A. Nijman, C. Verma, J. Wood, M.J. Champion, R. Sanger, A. Bennick, P.L. Yu, A.F. Wilson, W.L. Marsh, L. Pajunen, H. Hameister, B.A. Doppert, J.J. Garver, J.R. Sawyer, P. Meera Khan, P.J.L. Cook, Bjørnar Olaisen, R.C. Karn, J.D. Minna, J.D. Shulkin, B.M. Page, P.M. Sinet, B. Sykes, E.M. Helveston, C.W.H. Partridge, M. Blumenthal, P. Szabo, and E.A. Azen

Subjects
Botany, Genetics, Biology, Molecular Biology, Genetics (clinical)
Published
1978
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5. Subject Index Vol. 22, 1978

Author

S.J. Funderburk, J.E. Gray, G.A. Koch, L. Korsnes, A.S. Henderson, W.R.T. Los, D.A. Meyers, J.D. Minna, Per Teisberg, J.D. Shulkin, B.M. Page, M.C. Yoshida, K.E. Buckton, M.C. Sparkes, A.P. Goggin, M.L. Rivas, P.S. Gerald, K. Simola, C.E. Wright, W.K. Stanford, J.A. Brown, R.C.P. Go, L. Scrafford-Wolff, P.M. Sinet, D.C. Rao, E.J. Yunis, A. Westerveld, L. R. Weitkamp, B. Sykes, M. Bobrow, N. Oliver, H.-H. Ropers, M.A. Ferguson-Smith, D. Borgaonkar, S. Piomelli, D. Bootsma, C.W. Bazinet, A.F. Wilson, H. Hameister, P.J.L. Cook, E. Herbschleb-Voogt, J.J. Yunis, P. Szabo, S. Philipps, W. R. Mayr, T.B. Shows, E.A. Azen, R.C. Schwartz, J.M. Vance, S. Leupe-de Smit, D. Swallow, A.C. Leary, Bjørnar Olaisen, R.C. Karn, Y. Shimizu, B.J.B. Keats, E. Solomon, M.L. Schroeder, T. Gedde-Dahl, O.J. Miller, V. Kirton, J. H. Olving, S. Brown, R. Roos, D. Cox, F. Pellett, L.Y. Wang, Timothy A. Donlon, R.E. Magenis, E.M. Helveston, N.C. Sun, A. de la Chapelle, J.M. Luciani, A. Heiberg, R.S. Lemons, D.L. George, C.R.Y. Sun, R.D.G. McKay, R.M. Denney, N. Lamvik, A.S. Baim, R. Schwab, I. Balazs, N.E. Morton, L. Pajunen, M. Blumenthal, J.R. Sawyer, Elizabeth B. Robson, R.E. Eisenman, M. Prensky, P.A. Lalley, K.M. Overton, T.M. Dijksman, L.C. Yu, J.A. Robinson, L.M.M. Wijnen, H. Kaita, R.C. Elston, S.J. O’Brien, J. Garver, M.A. Nijman, M. Monteba-van Heuvel, P.L. Pearson, S. Povey, Erik Thorsby, B. Lauras, P. M. Conneally, V.A. McKusick, E. Tolley, K. Willecke, A.D. Merritt, R. Moreland, P. Meera Khan, P. Pierce, T.H. Roderick, M.Y. Tsai, R. Johannsmann, T. Campana, A. Brøgger, E.W. Lovrien, R.L. Eddy, N. Suciu-Foca, C.G. Palmer, C. Jones, A.F. Gazdar, A. Shalev, M.K. Fagerhol, E. Johnston, J. Reiss, C.N. Fear, S. Burgess, L.L. Haley, S. Hempfling, W.S. Volkers, J. Gavin, Liao Law, Y. Boyd, A. Mayerová, J.H. Edwards, M.G. Byers, W. Stanley, L.R. Weitkamp, M.E. Duncan, H.J. Evans, L.J. Donald, B. Hellkuhl, F.H. Ruddle, I.L. Hansteen, B.M. Turner, I.W. Craig, K.-H. Grzeschik, T. Mohandas, A. Siverts, D.W. Ball, K.C. Atwood, R. Bigley, L. U. Lamm, R.S. Sparkes, M. Siniscalco, S. Arias, R.A. Fisher, M. Mota, E.R. Giblett, C.T. Falk, S. Guttormsen, N.R. Mendell, K. Hirschhorn, M. Smith, H. Oie, M.P. Cowmeadow, F.T. Kao, J. de Witt, N. Shimizu, E.A. Nichols, E.S. Seravalli, D.A. Aitken, R. Mausner, M. Hultén, M. Lewis, R. Saisson, A. Bratlie, A.E. Greene, P. Karli, J. Chamberlin, M.T. Davisson, P.J. McAlpine, C.W.H. Partridge, I. Berczi, W.F. Witterland, Veronica van Heyningen, B.P. Dorman, A.P.M. Jongsma, P. Rubinstein, B.B. Knowles, C. Verma, J. Wood, M.J. Champion, B. Pernis, R. Sanger, K.E. Toomey, A. Bennick, P.L. Yu, W.L. Marsh, V.M. Regina, B.A. Doppert, J.J. Garver, U. Francke, J. Fraisse, M.E. Chandler, G.A.P. Bruns, H. Vriesendorp, S. Rowe, A. Krüger, J.M. Robert, B.J. Mintz, K. Bender, R. Lange, T. Borun, J.A. Norton, T. Ho, J.E. Noades, M.A. Pericak-Vance, R.T. Taggart, N. Tanigaki, M.A. Craft, K. Berg, Matthew Parks, F. Freycon, D.P. Aden, C.A. Slaughter, H.J. Cooke, J.E. Anderson, E. Lovrien, A.W. Johnston, A. Estop, J. Parekh, W.G. Burgerhout, M.A. Pellegrino, J. Hemmerling, A.F. Naylor, J.L. Hamerton, S. Goodnight, D.B. Amos, C.K. Eun, D.L. Slate, R. Jonassen, J. Ott, R. Mierau, T.T. Puck, D. Warburton, M. Devictor-Vuillet, C.J. Sherr, R.H. Lindenbaum, H.P. Klinger, K.K. Namboodiri, M. Meisler, S. Rosenfeld, F. Varricchio, E.H.Y. Chu, B. Carritt, T. Philip, W. Bauch, and S.J. Jeremiah

Subjects
Index (economics), Statistics, Genetics, Subject (documents), Biology, Molecular Biology, Genetics (clinical)
Published
1978
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7. Ultraviolet radiation and chemical requirements for experimental contact photosensitivity

Author

C A, Ramsay and F, Pellett

Subjects
Ultraviolet Rays, Guinea Pigs, Animals, Female, Photosensitivity Disorders, Allergens, Patch Tests, Dermatitis, Contact, Salicylanilides
Abstract

Contact photosensitivity to tetrachlorsalicylanilide was induced in albino guinea pigs. For the induction process, different types of ultraviolet radiation were employed and the effect of different doses of chemical was measured. Dose responses for ultraviolet radiation and chemical were determined for the production of positive photopatch tests in photosensitized animals. Successful contact photosensitivity was achieved when UVA alone was used for induction. Contrary to previously published reports, we found that UVB, chemical or physical irritation or immune potentiation were not required. In order to detect all photosensitized animals 0.1 ml of 1% TCSA and 1.65 J/cm2 of UVA were required to produce positive photopatch tests.

Published
1986

9. Association of variably expressed KIR3dl1 alleles with psoriatic disease.

Author

Berinstein J, Pollock R, Pellett F, Thavaneswaran A, Chandran V, and Gladman DD

Subjects
Adult, Alleles, Case-Control Studies, Epitopes chemistry, Female, Genotype, HLA Antigens genetics, HLA-B Antigens genetics, Humans, Inflammation, Male, Middle Aged, Polymerase Chain Reaction, Arthritis, Psoriatic genetics, Genetic Predisposition to Disease, Receptors, KIR3DL1 genetics
Abstract

The purpose of this study is to examine the genetic interaction of variably expressed killer cell immunoglobulin-like receptor (KIR) 3DL1 alleles with their cognate ligand, human leukocyte antigen (HLA)-Bw4, in susceptibility to psoriatic disease (PsD). A novel allelic typing system was developed to differentiate KIR3DL1 alleles (*High, *Low, *Null expression, and 3DS1), in PsD patients, including those with psoriatic arthritis (PsA) and cutaneous psoriasis without arthritis (PsC) and healthy controls. Frequencies of each KIR3DL1 allele, Bw4-80I and Bw4-80T, as well as the genetic interaction between the KIR3DL1 alleles and the Bw4 epitope were analyzed. KIR3DL1 alleles were successfully genotyped in 392 PsA, 260 PsC, and 371 control subjects. Only the KIR3DL1*Null allele was associated with PsD (OR = 0.69, p = 0.008), both in the PsA (OR = 0.69, p = 0.02) and PsC patients (OR = 0.70, p = 0.04) compared to control subjects. No difference in the frequency of KIR3DL1*Null was found between the PsA and PsC patients. The presence of the HLA-Bw4 epitope was significantly associated with PsD, particularly in the PsA patients compared to controls. Bw4-80I was increased in PsD and PsA subjects, but not in PsC patients compared to controls. Bw4-80T was increased in PsA compared to both PsC patients or to controls. No interaction was detected between any of the KIR3DL1 alleles and HLA-Bw4, Bw4-80I, or Bw4-80T. The novel qPCR technique successfully identified the four variably expressed KIR3DL1 alleles. The HLA-Bw4 epitope was associated with psoriatic disease, particularly with PsA, but no genetic interactions with KIR3DL1 alleles were detected.

Published
2017
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10. Clinical and Demographic Characteristics of Erosion-free and Erosion-present Status in Psoriatic Arthritis in a Cohort Study.

Author

Touma Z, Thavaneswaran A, Chandran V, Pellett F, Cook RJ, and Gladman DD

Subjects
Adult, Age Factors, Arthritis, Psoriatic diagnostic imaging, Disease Progression, Female, Follow-Up Studies, Humans, Male, Prognosis, Radiography, Retrospective Studies, Risk Factors, Young Adult, Arthritis, Psoriatic pathology, Joints diagnostic imaging
Abstract

Objective: Psoriatic arthritis (PsA) has been recognized as a severe erosive disease. However, some patients do not develop erosions. We aimed to determine the prevalence, characteristics, and predictors of erosion-free patients (EFP) as compared with erosion-present patients (EPP) among patients with PsA followed prospectively., Methods: This is a retrospective analysis conducted on patients from the Toronto PsA cohort. Patients with at least 10 years of followup and radiographs were analyzed. Radiographs were scored with the modified Steinbrocker method. Baseline (first visit to clinic) characteristics were used to predict the development of erosions with logistic regression models. To examine the effect of time-varying covariates, Cox regression models were fit for the time to development of erosions from baseline., Results: Among 290 patients, 12.4% were EFP and 87.6% were EPP over the study period. The mean time to development of erosion in the EPP over the course of followup was 6.8 ± 6.1 years. EFP were diagnosed with psoriasis at a younger age compared with EPP. In both models, actively inflamed joints and clinically damaged joints were predictive of the development of erosion, whereas a longer duration of psoriasis at baseline decreased the odds of developing erosion. EPP had a higher percentage of unemployment as compared with EFP at baseline and followup visits., Conclusion: Among patients with PsA followed for at least 10 years, 12.4% never develop erosions. The clinical and radiographic findings can ultimately assist in the stratification of a patient's prognosis regarding the development of erosions.

Published
2016
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11. Further Evidence Supporting a Parent-of-Origin Effect in Psoriatic Disease.

Author

Pollock RA, Thavaneswaran A, Pellett F, Chandran V, Petronis A, Rahman P, and Gladman DD

Subjects
Adult, Arthritis, Psoriatic epidemiology, Cohort Studies, Female, Genetic Predisposition to Disease epidemiology, Humans, Male, Middle Aged, Ontario epidemiology, Arthritis, Psoriatic diagnosis, Arthritis, Psoriatic genetics, Genetic Predisposition to Disease genetics, Parents
Abstract

Objective: To further explore the "parent-of-origin" effect in a large cohort of well-phenotyped patients with cutaneous psoriasis without arthritis (PsC) and psoriatic arthritis (PsA)., Methods: Self-reported family history was obtained from PsA patients from Toronto and Newfoundland satisfying the Classification of Psoriatic Arthritis criteria, and PsC patients from Toronto, who were examined by a rheumatologist to exclude PsA. Proportions of probands with paternally and maternally transmitted psoriatic disease were compared by McNemar's and chi-square tests. Baseline clinical and genetic characteristics of probands with paternally and maternally transmitted disease were compared using logistic regression., Results: A total of 849 probands reported a first-degree relative affected with psoriatic disease (PsC or PsA), of which 532 (63%) reported an affected parent. A significantly larger proportion of probands reported an affected father compared to an affected mother with psoriatic disease (289 [57%] versus 220 [43%], respectively; P = 0.003). This paternal transmission bias was evident in PsA (P = 0.006) and PsC probands, although it did not reach statistical significance in PsC probands (P = 0.20). Furthermore, the proportion of paternal PsC-proband PsA pairs (161 of 214 paternal transmissions [75%]) was significantly larger than maternal PsC-proband PsA pairs (103 of 161 maternal transmissions [64%]) (P = 0.02). Newfoundland probands with paternally transmitted disease had higher HLA-B*08 carriage (P = 0.04) and lower MICA-129Met carriage (P = 0.03). Males had higher HLA-B*38 carriage (P = 0.05) and a higher prevalence of nail lesions (P = 0.01)., Conclusion: We have provided further epidemiologic evidence of a paternal transmission bias in psoriatic disease., (© 2015, American College of Rheumatology.)

Published
2015
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12. Minimal disease activity and anti-tumor necrosis factor therapy in psoriatic arthritis.

Author

Haddad A, Thavaneswaran A, Ruiz-Arruza I, Pellett F, Chandran V, Cook RJ, and Gladman DD

Subjects
Adolescent, Adult, Arthritis, Psoriatic diagnosis, Arthritis, Psoriatic immunology, Blood Sedimentation, Drug Administration Schedule, Female, Humans, Male, Middle Aged, Odds Ratio, Predictive Value of Tests, Recurrence, Remission Induction, Reproducibility of Results, Risk Factors, Sex Factors, Time Factors, Treatment Outcome, Young Adult, Anti-Inflammatory Agents administration & dosage, Arthritis, Psoriatic drug therapy, Tumor Necrosis Factor-alpha antagonists & inhibitors
Abstract

Objective: A state of minimal disease activity (MDA) was defined and validated as target for treatment in psoriatic arthritis (PsA). We aimed to identify disease characteristics, outcome, and predictors of MDA in patients treated with tumor necrosis factor α (TNFα) blockers., Methods: Patients fulfilling the Classification of Psoriatic Arthritis criteria treated with TNFα blockers were followed every 3-6 months. Patients were considered in MDA when they meet at least 5 of the 7 criteria. Sustained MDA was defined as an MDA state lasting ≥12 months. Patients achieving MDA were compared to non-MDA patients. A proportional odds discrete time survival analysis model was applied, adjusting for sex, age, PsA duration, abnormal erythrocyte sedimentation rate (ESR) and clinically damaged joint count at each visit to identify predictors for MDA., Results: Of the 306 patients treated with TNFα blockers identified from our database, 23 patients were in an MDA state when treatment was commenced; 57 were taking TNFα blockers prior to enrollment. Therefore, 226 subjects were in a non-MDA state and constituted the study population. One hundred forty-five patients of 226 patients (64%) achieved MDA within a mean ± SD duration of 1.30 ± 1.68 years. The mean ± SD duration of MDA was 3.46 ± 2.25 years. At total of 17 patients withdrew from therapy and remained in an MDA state. Male sex (odds ratio [OR] 1.65, 95% confidence interval [95% CI] 1.08-2.53; P = 0.02) and normal ESR (OR 2.27, 95% CI 1.22-4.17; P = 0.009) increased the odds for achieving MDA., Conclusion: MDA is achieved in 64% of patients treated with TNFα blockers in a clinical setting. Male sex and normal ESR are predictors for MDA. On withdrawal or reduction in treatment, 11.6% of patients maintained MDA state., (© 2015, American College of Rheumatology.)

Published
2015
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13. Immunoglobulin G subclass analysis in psoriatic arthritis.

Author

Haddad A, Thavaneswaran A, Abji F, Pellett F, Chandran V, Wither JE, and Gladman DD

Subjects
Adult, Aged, Arthritis, Psoriatic blood, Biomarkers blood, Blood Sedimentation, C-Reactive Protein metabolism, Cohort Studies, Comorbidity, Female, Humans, Inflammatory Bowel Diseases blood, Inflammatory Bowel Diseases epidemiology, Inflammatory Bowel Diseases immunology, Longitudinal Studies, Male, Middle Aged, Monoclonal Gammopathy of Undetermined Significance blood, Prevalence, Rheumatic Diseases blood, Rheumatic Diseases epidemiology, Rheumatic Diseases immunology, Uveitis blood, Uveitis epidemiology, Uveitis immunology, Arthritis, Psoriatic epidemiology, Arthritis, Psoriatic immunology, Disease Progression, Immunoglobulin G blood, Immunoglobulin G classification, Monoclonal Gammopathy of Undetermined Significance epidemiology, Monoclonal Gammopathy of Undetermined Significance immunology
Abstract

Objective: The occurrence of monoclonal gammopathy of undetermined significance (MGUS) is common in chronic immune mediated disorders. This increased monoclonal antibody production could result from chronic stimulation of lymphocytes, with the immunoglobulin G (IgG) subtype accounting for the majority of cases in psoriatic arthritis (PsA). We aimed to identify IgG subclass profiles in patients with PsA and to determine association with specific disease characteristics., Methods: Serum samples from 221 patients with PsA from a single cohort were analyzed for their serum IgG subclass levels. All patients fulfilled the ClASsification for Psoriatic ARthritis (CASPAR) criteria and were followed at 6-month to 12-month intervals according to a standard protocol. MGUS was defined as the occurrence of a discrete band in the gammaglobulin region on at least 2 separate serum protein electrophoresis tests performed 6 months apart. Patients with high abnormal IgG subclass levels were compared to patients with normal levels using descriptive tests., Results: Elevations of IgG1-4 were common in PsA, with ∼20%-49% of patients having elevations of each subclass, IgG2 being the most common subclass abnormality. However, no clinical-serological correlation was found in the group with abnormal IgG2 levels. Of the 38 patients with MGUS, elevations in IgG1 were most common. Patients with an abnormal IgG1 subclass level were more likely to have a discrete band in the gammaglobulin region, higher prevalence of MGUS, and abnormal erythrocyte sedimentation rate or C-reactive protein levels., Conclusion: Determination of the IgG subclass concentration in PsA did not seem to add any significant value in identifying specific disease manifestations. However, this study provides insight into the pathological process leading to MGUS in PsA.

Published
2014
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14. Fine mapping major histocompatibility complex associations in psoriasis and its clinical subtypes.

Author

Okada Y, Han B, Tsoi LC, Stuart PE, Ellinghaus E, Tejasvi T, Chandran V, Pellett F, Pollock R, Bowcock AM, Krueger GG, Weichenthal M, Voorhees JJ, Rahman P, Gregersen PK, Franke A, Nair RP, Abecasis GR, Gladman DD, Elder JT, de Bakker PI, and Raychaudhuri S

Subjects
Amino Acid Sequence, Arthritis, Psoriatic genetics, Base Sequence, Chromosome Mapping methods, Genetic Association Studies, Genetic Predisposition to Disease, Genotype, HLA-B Antigens genetics, HLA-C Antigens genetics, Humans, Polymorphism, Single Nucleotide, Psoriasis classification, Psoriasis immunology, Histocompatibility Antigens Class I genetics, Histocompatibility Antigens Class II genetics, Major Histocompatibility Complex genetics, Psoriasis genetics
Abstract

Psoriasis vulgaris (PsV) risk is strongly associated with variation within the major histocompatibility complex (MHC) region, but its genetic architecture has yet to be fully elucidated. Here, we conducted a large-scale fine-mapping study of PsV risk in the MHC region in 9,247 PsV-affected individuals and 13,589 controls of European descent by imputing class I and II human leukocyte antigen (HLA) genes from SNP genotype data. In addition, we imputed sequence variants for MICA, an MHC HLA-like gene that has been associated with PsV, to evaluate association at that locus as well. We observed that HLA-C(∗)06:02 demonstrated the lowest p value for overall PsV risk (p = 1.7 × 10(-364)). Stepwise analysis revealed multiple HLA-C(∗)06:02-independent risk variants in both class I and class II HLA genes for PsV susceptibility (HLA-C(∗)12:03, HLA-B amino acid positions 67 and 9, HLA-A amino acid position 95, and HLA-DQα1 amino acid position 53; p < 5.0 × 10(-8)), but no apparent risk conferred by MICA. We further evaluated risk of two major clinical subtypes of PsV, psoriatic arthritis (PsA; n = 3,038) and cutaneous psoriasis (PsC; n = 3,098). We found that risk heterogeneity between PsA and PsC might be driven by HLA-B amino acid position 45 (Pomnibus = 2.2 × 10(-11)), indicating that different genetic factors underlie the overall risk of PsV and the risk of specific PsV subphenotypes. Our study illustrates the value of high-resolution HLA and MICA imputation for fine mapping causal variants in the MHC., (Copyright © 2014 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2014
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15. Serum adipokines in patients with psoriatic arthritis and psoriasis alone and their correlation with disease activity.

Author

Eder L, Jayakar J, Pollock R, Pellett F, Thavaneswaran A, Chandran V, Rosen CF, and Gladman DD

Subjects
Adult, Antirheumatic Agents therapeutic use, Arthritis, Psoriatic blood, Arthritis, Psoriatic complications, Arthritis, Psoriatic drug therapy, Biomarkers blood, Cross-Sectional Studies, Female, Humans, Insulin blood, Insulin Resistance physiology, Leptin blood, Male, Metabolic Syndrome blood, Middle Aged, Psoriasis blood, Psoriasis drug therapy, Risk Factors, Severity of Illness Index, Adipokines blood, Metabolic Syndrome etiology, Psoriasis complications
Abstract

Objective: To compare the prevalence of metabolic syndrome (MetS) and the levels of related biomarkers in patients with psoriatic arthritis (PsA) and psoriasis without arthritis (PsC)., Methods: This study compared patients with PsA and patients with PsC. The presence of MetS was determined. Serum levels of insulin, adiponectin and leptin were measured. The homeostasis model assessment for insulin resistance (HOMA-IR) was calculated. HOMA-IR, adiponectin and leptin were log-transformed. Continuous variables were compared using the t test and the χ(2) test was used for discrete variables. Multivariate regression models were used to investigate the association of MetS and adiponectin with PsA compared to PsC after adjusting for potential confounding variables., Results: 203 PsA and 155 PsC patients were analysed. The prevalence of MetS was higher in PsA patients compared to those with PsC. However, this did not reach statistical significance (36.5% vs 27.1%, p=0.056). The levels of adipokines were significantly higher in PsA compared to PsC: adiponectin (8.8±5.2 vs 7.4±4.5 log (µg/ml), p=0.009) and leptin in women (3.1±0.8 vs 2.8±0.8, log (ng/ml), p=0.04). HOMA-IR was also higher in PsA (0.97±0.63 vs 0.68±0.81, p<0.001). No difference was observed in leptin levels in men. In multivariate regression analysis, PsA (p=0.04) and the psoriasis area and severity index score (p=0.02) were associated with MetS. Adiponectin was significantly associated with PsA (p=0.005), the use of anti-tumour necrosis factor α therapy (p=0.03) and active joint count (p=0.001)., Conclusions: MetS and related adipokines correlated with an increased burden of skin and joint inflammation.

Published
2013
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16. UGT2B17 copy number gain in a large ankylosing spondylitis multiplex family.

Author

Uddin M, Maksymowych WP, Inman R, Gladman D, Munn A, Yazdani R, Pellett F, Hamilton S, O'Rielly DD, and Rahman P

Subjects
Case-Control Studies, Cohort Studies, Female, Humans, Male, Minor Histocompatibility Antigens, Pedigree, Polymerase Chain Reaction, DNA Copy Number Variations, Glucuronosyltransferase genetics, Spondylitis, Ankylosing genetics
Abstract

Background: The primary objective of this study is to identify novel copy number variations (CNVs) associated with familial ankylosing spondylitis (AS). A customized genome-wide microarray was designed to detect CNVs and applied to a multiplex AS family with six (6) affected family members. CNVs were detected using the built-in DNA analytics aberration detection method-2 (ADM-2) algorithm. Gene enrichment analysis was performed to observe the segregation. Subsequent validation was performed using real time quantitative fluorescence polymerase reaction (QF-PCR). The frequency of copy number variation for the UGT2B17 gene was then performed on two well-defined AS cohorts. Fisher exact test was performed to quantify the association., Results: Our family-based analysis revealed ten gene-enriched CNVs that segregate with all six family members affected with AS. Based on the proposed function and the polymorphic nature of the UGT2B17 gene, the UGT2B17 gene CNV was selected for validation using real time QF-PCR with full concordance. The frequency of two copies of the UGT2B17 gene CNV was 0.41 in the Newfoundland AS cases and 0.35 in the Newfoundland controls (OR = 1.26(0.99-1.59); p < 0.05)), whereas the frequency of two (2) copies of the UGT2B17 gene CNV was 0.40 in the Alberta AS cases and 0.39 in the Alberta controls (OR = 1.05(95% CI: 0.83-1.33); p < 0.71))., Conclusions: A genome-wide microarray interrogation of a large multiplex AS family revealed segregation of the UGT2B17 gene CNV among all affected family members. The association of the UGT2B17 CNV with AS is particularly interesting given the recent association of this CNV with osteoporosis and the proposed function as it encodes a key enzyme that inhibits androgens. However, two copies of the UGT2B17 gene CNV were only marginally significant in a uniplex AS cohort from Newfoundland but not in a uniplex AS cohort from Alberta.

Published
2013
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17. Serum kallikrein-8 correlates with skin activity, but not psoriatic arthritis, in patients with psoriatic disease.

Author

Eissa A, Cretu D, Soosaipillai A, Thavaneswaran A, Pellett F, Diamandis A, Cevikbas F, Steinhoff M, Diamandis EP, Gladman D, and Chandran V

Subjects
Biomarkers analysis, Biomarkers blood, Biomarkers metabolism, Case-Control Studies, Dermatitis blood, Dermatitis metabolism, Dermatitis pathology, Enzyme-Linked Immunosorbent Assay, Female, Humans, Immunohistochemistry, Kallikreins blood, Kallikreins metabolism, Male, Middle Aged, Psoriasis blood, Psoriasis pathology, Severity of Illness Index, Synovial Fluid chemistry, Synovial Fluid metabolism, Kallikreins analysis, Psoriasis metabolism
Abstract

Background: About 30% of cutaneous psoriasis (PsC) patients develop psoriatic arthritis (PsA) in the joint, which is under-recognized by dermatologists. Biomarkers for PsA are needed so that early referral to a rheumatologist is made. Kallikreins (KLKs) are secreted serine proteases implicated in skin desquamation and inflammation. This study examined KLK potential as serum biomarkers of PsA in cutaneous psoriasis patients., Methods: KLKs were measured by ELISAs in synovial fluids of three PsA patients and three control early osteoarthritis (OA) patients, as well as in a cohort of 152 serum samples collected from age- and sex-matched PsC patients, with (n=76) or without PsA (n=76). KLK expression in psoriatic plaques was examined by immunohistochemistry. Univariate and multivariate logistic regression analyses were conducted to analyze the association between serum KLK levels and disease class (PsC, PsA). Serum KLKs that associated with PsA were correlated with clinical parameters of skin and joint activity., Results: Among the seven KLKs tested, KLK6 and KLK8 were elevated in both PsA synovial fluids and psoriatic plaques, but only serum KLK8 levels were associated with psoriatic disease (odds ratio=2.56, p=0.03). Although significantly elevated in PsC and PsA sera compared to healthy controls, KLK8 did not discriminate PsA from PsC patients. KLK8 correlated positively with the psoriasis area and severity index (PASI) (r=0.43, p=0.001) independent of age, sex and psoriasis duration ( β=1.153, p=0.0003) and exhibited no correlations with tender or swollen joint counts., Conclusions: Increased KLK8 serum level in PsA patients reflects disease activity in the skin but not in the joints. Serum KLK levels are not useful for screening psoriasis patients for PsA.

Published
2013
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18. Differential human leucocyte allele association between psoriasis and psoriatic arthritis: a family-based association study.

Author

Eder L, Chandran V, Pellett F, Shanmugarajah S, Rosen CF, Bull SB, and Gladman DD

Subjects
Arthritis, Psoriatic immunology, Female, Gene Frequency, Genetic Association Studies, Genetic Markers, Genotype, Histocompatibility Testing, Humans, Linkage Disequilibrium, Male, Arthritis, Psoriatic genetics, Family Health, Genetic Predisposition to Disease, HLA-B Antigens genetics, HLA-C Antigens genetics, Population Surveillance
Abstract

Objective: A recent population-based study identified several HLA alleles as conferring a risk for psoriatic arthritis (PsA) among patients with psoriasis. The authors aimed to confirm these results using a family-based association study., Methods: PsA probands, psoriasis probands and their first-degree family members were included. All participants were evaluated for the presence of psoriasis and inflammatory arthritis. HLA-B and -C genotyping was performed. The family-based association test was used to test for differences between PsA and psoriasis patients in transmission of candidate alleles from parents to offspring., Results: A total of 178 PsA and 30 psoriasis probands and 561 first degree family members were analysed. The following HLA alleles were over-transmitted to PsA compared with psoriasis: HLA-C*12 (p=0.005), HLA-B*38 (p=0.04), HLA-B*39 (p=0.03), HLA-B*27 (p=0.002)., Conclusions: HLA-B*27, HLA-B*38, HLA-B*39 and HLA-C*12 alleles are potential PsA-specific genetic markers among patients with psoriasis.

Published
2012
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19. IL13 gene polymorphism is a marker for psoriatic arthritis among psoriasis patients.

Author

Eder L, Chandran V, Pellett F, Pollock R, Shanmugarajah S, Rosen CF, Rahman P, and Gladman DD

Subjects
Adolescent, Adult, Arthritis, Psoriatic epidemiology, Case-Control Studies, Female, Genetic Markers, Genetic Predisposition to Disease, Genotype, Humans, Male, Ontario epidemiology, Psoriasis epidemiology, Psoriasis genetics, Smoking epidemiology, Young Adult, Arthritis, Psoriatic genetics, Interleukin-13 genetics, Polymorphism, Single Nucleotide
Abstract

Aim: To study the association between smoking and IL13 gene polymorphisms with psoriatic arthritis (PsA) and psoriasis., Methods: The authors genotyped three groups of Caucasians: those with PsA, those with psoriasis without arthritis (PsC) and healthy controls for the rs20541 and rs848 IL13 single nucleotide polymorphisms (SNPs). An additional SNP, rs1800925, was genotyped only in the PsA and PsC groups. The differences in allelic distributions were compared by χ(2) test. The prevalence of smoking was compared between people with PsA and those with PsC. The combined effect of genotype and smoking was tested by comparing the frequencies of different combinations of rs1800925 genotype and smoking status in PsA and PsC., Results: 555 PsA patients, 342 PsC patients and 217 healthy controls were included in the study. Smoking was less prevalent in patients with PsA compared with PsC (47.4% vs 59.4%, p<0.0006). rs20541*G and rs848*C alleles were associated with PsA compared with controls (OR 1.64, p=0.0005, OR 1.61, p=0.0007 respectively). The association between these alleles and PsC compared with controls was only of borderline significance (OR 1.33, p=0.06, OR 1.26, p=0.11 respectively). Two major alleles, rs1800925*C (OR 1.28, p=0.045) and rs848*C (OR 1.30, p=0.047) were increased in PsA compared with PsC. The combination of non-smoking and the genotype rs1800925*CC was associated with increased susceptibility to PsA compared with PsC. Among smokers, rs1800925*CC was not associated with PsA compared with PsC., Conclusions: IL13 gene polymorphism is associated with increased susceptibility to PsA in psoriasis patients.

Published
2011
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20. Differential major histocompatibility complex class I chain-related A allele associations with skin and joint manifestations of psoriatic disease.

Author

Pollock R, Chandran V, Barrett J, Eder L, Pellett F, Yao C, Lino M, Shanmugarajah S, Farewell VT, and Gladman DD

Subjects
Adolescent, Adult, Alleles, Arthritis complications, Arthritis genetics, Case-Control Studies, Female, HLA-B Antigens genetics, HLA-C Antigens genetics, Homozygote, Humans, Linkage Disequilibrium, Male, Middle Aged, Gene Expression Regulation, Histocompatibility Antigens Class I genetics, Joints pathology, Psoriasis genetics, Psoriasis immunology, Skin pathology
Abstract

About 30% of patients with psoriasis have psoriatic arthritis (PsA), an inflammatory arthritis that can affect both axial and peripheral joints. Major histocompatibility complex class I chain-related A (MICA) alleles have previously been shown to be associated with PsA; however it is unclear whether there is a differential association of MICA alleles with skin and joint manifestations of PsA. Here, we describe a case-control study that aims to validate previously reported MICA allele associations with PsA and determine whether MICA alleles differentiate patients with PsA from those with psoriasis without PsA. Two hundred forty-nine unrelated Caucasian PsA patients, 243 psoriasis patients without arthritis, and 248 healthy controls were genotyped for 55 MICA alleles using PCR-SSP, and for human leucocyte antigen (HLA)-B and HLA-C alleles by PCR-SSO reverse line blot. Allele frequencies were calculated and logistic regressions were performed, adjusting for HLA-B and HLA-C alleles previously shown to be associated with psoriasis and/or PsA. Several MICA alleles were associated with psoriatic disease, PsA, and psoriasis compared with controls, and PsA compared with psoriasis in univariate analyses. Haplotype analysis showed evidence of strong linkage disequilibrium (LD) between PsA and psoriasis risk alleles of HLA-C, HLA-B, and MICA. After adjusting for significant HLA-B and HLA-C alleles in multivariate analyses, MICA*016 remained significantly associated with psoriasis [odds ratio (OR) = 5.5, P = 0.008]. MICA*00801 homozygosity was associated with susceptibility to PsA when compared with patients with psoriasis alone (OR = 2.26, P = 0.009). We conclude that most MICA allele associations with psoriasis and PsA are dependent on LD with HLA-B and HLA-C risk alleles. Independent of HLA, only MICA*016 influences the risk of developing psoriasis without arthritis, and homozygosity for MICA*00801 increases the risk of developing PsA in patients with psoriasis., (© 2011 John Wiley & Sons A/S.)

Published
2011
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21. Mechanisms of copy number variation and hybrid gene formation in the KIR immune gene complex.

Author

Traherne JA, Martin M, Ward R, Ohashi M, Pellett F, Gladman D, Middleton D, Carrington M, and Trowsdale J

Subjects
Chromosome Mapping, Gene Duplication, Genes, Immunoglobulin genetics, Haplotypes, Humans, Gene Dosage genetics, Genetic Variation, Multigene Family genetics, Receptors, KIR genetics
Abstract

The fine-scale structure of the majority of copy number variation (CNV) regions remains unknown. The killer immunoglobulin receptor (KIR) gene complex exhibits significant CNV. The evolutionary plasticity of the KIRs and their broad biomedical relevance makes it important to understand how these immune receptors evolve. In this paper, we describe haplotype re-arrangement creating novel loci at the KIR complex. We completely sequenced, after fosmid cloning, two rare contracted haplotypes. Evidence of frequent hybrid KIR genes in samples from many populations suggested that re-arrangements may be frequent and selectively advantageous. We propose mechanisms for formation of novel hybrid KIR genes, facilitated by protrusive non-B DNA structures at transposon recombination sites. The heightened propensity to generate novel hybrid KIR receptors may provide a proactive evolutionary measure, to militate against pathogen evasion or subversion. We propose that CNV in KIR is an evolutionary strategy, which KIR typing for disease association must take into account.

Published
2010
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22. Association of killer cell immunoglobulin-like receptor genotypes with vascular arterial events and anticardiolipin antibodies in patients with lupus.

Author

Toloza S, Pellett F, Chandran V, Ibanez D, Urowitz M, and Gladman D

Subjects
Adult, Angina Pectoris blood, Angina Pectoris epidemiology, Angina Pectoris genetics, Antibodies, Anticardiolipin blood, Comorbidity, Female, HLA-C Antigens blood, Humans, Ischemic Attack, Transient blood, Ischemic Attack, Transient epidemiology, Ischemic Attack, Transient genetics, Lupus Erythematosus, Systemic epidemiology, Male, Myocardial Infarction blood, Myocardial Infarction epidemiology, Myocardial Infarction genetics, Peripheral Vascular Diseases blood, Peripheral Vascular Diseases epidemiology, Peripheral Vascular Diseases genetics, Prospective Studies, Risk Factors, Stroke blood, Stroke epidemiology, Stroke genetics, Vasculitis blood, Vasculitis epidemiology, Vasculitis genetics, White People genetics, Young Adult, Genotype, Lupus Erythematosus, Systemic blood, Lupus Erythematosus, Systemic genetics, Receptors, KIR genetics
Abstract

To determine whether killer cell immunologlobulin-like receptor (KIR) genotypes are associated with vasculitis, vascular arterial events or anticardiolipin (aCL) antibodies in patients with lupus. A total of 304 patients followed prospectively at the University of Toronto Lupus Clinic were assessed for the occurrence of vasculitis and vascular arterial events. Molecular HLA-C and KIR (presence or absence of KIR2DL1, 2DL2, 2DL3, 2DS1 and 2DS2) genotyping were performed. Chi-square and logistic regression were used to analyse association between KIR genes and vascular arterial events and aCL antibodies. In patients with vascular arterial events, there was a significant increase in KIR2DS2 (60% vs 45%, P = 0.02) and in KIR2DL2 (62% vs 47%, P = 0.01) compared with patients without events. There was no increase in activating KIR genotypes in patients with vasculitis. In patients with aCL antibodies, significant increases were seen in KIR2DS2 (54% vs 41%, P = 0.03) and KIR2DL2 (58% vs 41%, P = 0.003), but KIR2DL3 was decreased (87% vs 95%, P = 0.03). Logistic regression confirmed independent association of KIR2DS2 with vascular arterial events. We found an increase in KIR2DS2 in lupus patients with vascular arterial events, but not in patients with vasculitis.

Published
2008
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24. KIRs and autoimmune disease: studies in systemic lupus erythematosus and scleroderma.

Author

Pellett F, Siannis F, Vukin I, Lee P, Urowitz MB, and Gladman DD

Subjects
Cadaver, Case-Control Studies, Genotype, Humans, Killer Cells, Natural immunology, Prospective Studies, Receptors, KIR, Tissue Donors, HLA Antigens genetics, Lupus Erythematosus, Systemic genetics, Receptors, Immunologic genetics, Scleroderma, Diffuse genetics
Abstract

We investigated killer immunoglobulin-like receptors (KIRs) and the human leukocyte antigen (HLA)-C ligands for the corresponding inhibitory KIRs in Caucasian patients, 304 with systemic lupus erythematosus (SLE) and 90 with scleroderma [or progressive systemic sclerosis (PSS)] compared with 416 Caucasian controls. Compared with controls, KIR2DS1 in the absence of KIR2DS2 was increased in both SLE (P= 0.04) and PSS (P= 0.02). Only 42% of KIR2DS1-positive PSS patients had the appropriate HLA-C ligand for the corresponding inhibitory KIR compared with 61% of KIR2DS1 positive controls (P= 0.02). In the PSS group the presence of at least either activating KIR2DS1 and/or 2DS2 was significantly increased in patients when compared with controls (P= 0.001). This suggests that KIR receptors play a role in susceptibility to both PSS and SLE.

Published
2007
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25. TNFalpha polymorphisms and risk of psoriatic arthritis.

Author

Rahman P, Siannis F, Butt C, Farewell V, Peddle L, Pellett F, and Gladman D

Subjects
Canada, Female, Gene Frequency, Genetic Predisposition to Disease, Humans, Linkage Disequilibrium, Logistic Models, Male, Middle Aged, Arthritis, Psoriatic genetics, Polymorphism, Genetic, Tumor Necrosis Factor-alpha genetics
Abstract

Background: Tumour necrosis factor alpha (TNFalpha) is a cytokine of critical importance in psoriatic arthritis., Objectives: (1) To examine the association between TNFalpha promoter gene polymorphisms and psoriatic arthritis in two well characterised Canadian populations with the disease; (2) to carry out a meta-analysis of all TNFalpha association studies in white psoriatic arthritis populations., Methods: DNA samples were genotyped for five TNF variants by time of flight mass spectrometry using the Sequenom platform. All five single nucleotide polymorphisms were in the 5' flanking region of TNFalpha gene at the following positions: -1031 (T-->C), -863 (C-->A), -857 (C-->T), -308 (G-->A), and -238 (G-->A). Primary analyses were based on logistic regression. Summary estimates of disease/genotype relations from several studies were derived from random effects meta-analyses., Results: 237 psoriatic arthritis subjects and 103 controls from Newfoundland and 203 psoriatic arthritis subjects and 101 controls from Toronto were studied. A combined analysis of data from both populations, showed a significant association between disease status and the -238(A) variant (p=0.01). The meta-analysis estimate for the -238(A) TNFalpha variant in eight psoriatic arthritis populations was also significant (odds ratio=2.29 (95% confidence interval, 1.48 to 3.55))., Conclusions: Analysis of TNFalpha variants in psoriatic arthritis populations shows that the -238 (A) variant is a significant risk factor for this disease.

Published
2006
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26. HLA markers for susceptibility and expression in scleroderma.

Author

Gladman DD, Kung TN, Siannis F, Pellett F, Farewell VT, and Lee P

Subjects
Adult, Aged, Alleles, Disease Susceptibility epidemiology, Disease Susceptibility immunology, Female, Gene Expression immunology, HLA-A Antigens genetics, HLA-B Antigens genetics, HLA-C Antigens genetics, HLA-DQ Antigens genetics, HLA-DR Antigens genetics, HLA-DRB1 Chains, Humans, Hypertension, Pulmonary genetics, Hypertension, Pulmonary immunology, Hypertension, Pulmonary mortality, Incidence, Male, Middle Aged, Scleroderma, Diffuse immunology, Scleroderma, Diffuse mortality, Scleroderma, Limited immunology, Scleroderma, Limited mortality, Survival Rate, Biomarkers, HLA Antigens genetics, Scleroderma, Diffuse genetics, Scleroderma, Limited genetics
Abstract

Objective: Reported associations between HLA alleles and both susceptibility to and features of scleroderma have been conflicting. Our objective was (1) to determine the role of HLA alleles in the susceptibility to scleroderma; and (2) to determine the role of HLA alleles in various aspects of disease expression., Methods: Consecutive patients were followed in the scleroderma clinic between 1996 and 1998. Clinical data were obtained through chart review. Healthy volunteers as well as cadaveric donors served as controls. Molecular HLA typing was performed (polymerase chain reaction/sequence-specific oligonucleotides). Statistical analysis included Fisher's exact test and multivariate analyses, using logistic and linear regression models., Results: Ninety-five Caucasian patients (75 women, 20 men, age 43.9 yrs, disease duration 11.9 yrs) with scleroderma and 416 controls were studied. HLA-DRB1*01 and HLA-DRB1*11 were associated with susceptibility to scleroderma, whereas HLA-DRB1*07 was protective. HLA-A*30 and HLA-A*32 were also associated with susceptibility to scleroderma, while HLA-B*57 and HLA-Cw*14 were protective. HLA-B*62 and HLA-DRB1*07 had a significant correlation with the presence of diffuse skin involvement in both univariate and multivariate analyses. HLA-DRB1*11 was associated with high skin score values, while lower values were related to the presence of HLA-Cw*14 and HLA-DQB1*06. Both alleles retained significance in a linear regression model. High skin score values were related to the absence of anticentromere antibodies. Pulmonary fibrosis was associated with HLA-B*62 and HLA-Cw*0602, whereas pulmonary hypertension was associated with HLA-B*13 and HLA-B*65., Conclusion: HLA alleles play a role in susceptibility to scleroderma and its disease expression.

Published
2005

27. HLA is a candidate region for psoriatic arthritis. evidence for excessive HLA sharing in sibling pairs.

Author

Gladman DD, Farewell VT, Pellett F, Schentag C, and Rahman P

Subjects
Arthritis, Psoriatic diagnosis, Haplotypes, Humans, Siblings, Arthritis, Psoriatic genetics, Genetic Predisposition to Disease, HLA Antigens genetics
Abstract

Psoriatic arthritis (PsA) is an inflammatory arthritis that may affect as many as 30% of patients with psoriasis (Ps). Genetic factors play an important role in the susceptibility to and the expression of PsA. The objective of this study was to identify whether haplotype sharing among affected sibling pairs of individuals with PsA is increased compared with unaffected sibling pairs. We collected 182 sibling pairs of probands affected with PsA. Extracted genomic DNA was amplified in polymerase chain reactions using locus specific primers homologous to nucleotide sequences for each of the HLA-A, -B, -C, -DR, and -DQ loci. Polymerase chain reaction amplicons were identified by reverse line blot assay using sequence-specific oligonucleotide probes. Evidence for excessive haplotype sharing was examined through Green and Woodrow's test. Results indicate that of the 182 sibling pairs, 46 were affected by PsA, 48 by Ps, and 88 were unaffected. The sharing of 2, 1, and 0 haplotypes for the PsA affected sibling pairs was 14, 27, and 5, respectively (p = 0.04); whereas the haplotype sharing for the Ps affected sibling pairs was 12, 26, and 10, respectively (p = 0.38). In conclusion, the human leukocyte antigen region on chromosome 6p is implicated as one of the candidate regions in PsA.

Published
2003
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28. Cutting edge: susceptibility to psoriatic arthritis: influence of activating killer Ig-like receptor genes in the absence of specific HLA-C alleles.

Author

Martin MP, Nelson G, Lee JH, Pellett F, Gao X, Wade J, Wilson MJ, Trowsdale J, Gladman D, and Carrington M

Subjects
Gene Frequency immunology, HLA-C Antigens metabolism, Humans, Killer Cells, Natural immunology, Ligands, Receptors, Immunologic metabolism, Receptors, KIR, Receptors, KIR2DL1, Receptors, KIR2DL2, Alleles, Arthritis, Psoriatic genetics, Arthritis, Psoriatic immunology, Gene Expression Regulation immunology, Genetic Predisposition to Disease, HLA-C Antigens genetics, Killer Cells, Natural metabolism, Receptors, Immunologic genetics
Abstract

NK cell activity is partially controlled through interactions between killer Ig-like receptors (KIR) on NK cells and their respective HLA class I ligands. Independent segregation of HLA and KIR genes, along with KIR specificity for particular HLA allotypes, raises the possibility that any given individual may express KIR molecules for which no ligand is present. Inhibitory receptor genes KIR2DL2/3 and KIR2DL1 were present in nearly all subjects sampled in this study, whereas their respective activating homologs, KIR2DS2 and KIR2DS1, are each present in about half of the subjects. In this work we report that subjects with activating KIR2DS1 and/or KIR2DS2 genes are susceptible to developing psoriatic arthritis, but only when HLA ligands for their homologous inhibitory receptors, KIR2DL1 and KIR2DL2/3, are missing. Absence of ligands for inhibitory KIRs could potentially lower the threshold for NK (and/or T) cell activation mediated through activating receptors, thereby contributing to pathogenesis of psoriatic arthritis.

Published
2002
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29. HLA-DRB1*04 alleles in psoriatic arthritis: comparison with rheumatoid arthritis and healthy controls.

Author

Gladman DD, Farewell VT, Rahman P, Schentag CT, Pellett F, Ng CM, and Wade JA

Subjects
Adult, Aged, Arthritis, Psoriatic genetics, Arthritis, Rheumatoid genetics, Epitopes, Female, HLA-DRB1 Chains, Humans, Male, Middle Aged, Alleles, Arthritis, Psoriatic immunology, Arthritis, Rheumatoid immunology, HLA-DR Antigens genetics
Abstract

Psoriatic arthritis (PsA) is an inflammatory arthritis associated with psoriasis usually seronegative for rheumatoid factor. An increased frequency of HLA-DR4 has been noted in PsA, particularly among patients with a rheumatoid arthritis like (RA) arthritis. The aim of the current investigation was to compare HLA-DRB1*04 alleles in patients with PsA, patients with RA, and healthy controls. Sample size calculations based on the frequency of HLA-DR4 suggested that 90 individuals in each patient group would be sufficient to address our question. Therefore, 90 HLA-DRB1*04 positive patients from each patient group underwent high resolution molecular typing and were included in this study. Although HLA-DRB1*0401 was the most frequent allele in all groups, its frequency among the PsA patients was lower than that of RA patients and controls. HLA-DRB1*0402 was higher among patients with PsA. Patients with RA were more likely to have more than one shared epitope allele than either PsA or the healthy control group. HLA-DQB1 alleles did not contribute further information. We suggest that the differences in the class II HLA epitope(s) may also be related to interaction specificity with another molecule functioning in the immune response to a putative arthritogenic antigen and result in differences in disease expression.

Published
2001
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30. Ultraviolet radiation and chemical requirements for experimental contact photosensitivity.

Author

Ramsay CA and Pellett F

Subjects
Allergens toxicity, Animals, Female, Guinea Pigs, Patch Tests, Salicylanilides toxicity, Dermatitis, Contact etiology, Photosensitivity Disorders etiology, Ultraviolet Rays adverse effects
Abstract

Contact photosensitivity to tetrachlorsalicylanilide was induced in albino guinea pigs. For the induction process, different types of ultraviolet radiation were employed and the effect of different doses of chemical was measured. Dose responses for ultraviolet radiation and chemical were determined for the production of positive photopatch tests in photosensitized animals. Successful contact photosensitivity was achieved when UVA alone was used for induction. Contrary to previously published reports, we found that UVB, chemical or physical irritation or immune potentiation were not required. In order to detect all photosensitized animals 0.1 ml of 1% TCSA and 1.65 J/cm2 of UVA were required to produce positive photopatch tests.

Published
1986

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