Your search keyword '"Criswell, L. A."' showing total 23 results

1. Novel gene variants associated with cardiovascular disease in systemic lupus erythematosus and rheumatoid arthritis

Author

Leonard, D., Svenungsson, E., Dahlqvist, J., Alexsson, A., Ärlestig, L., Taylor, K. E., Sandling, J. K., Bengtsson, C., Frodlund, M., Jönsen, A., Eketjäll, S., Jensen-Urstad, K., Gunnarsson, I., Sjöwall, C., Bengtsson, A. A., Eloranta, M. -L, Syvänen, A. -C, Rantapää-Dahlqvist, Solbritt, Criswell, L. A., Rönnblom, L., Leonard, D., Svenungsson, E., Dahlqvist, J., Alexsson, A., Ärlestig, L., Taylor, K. E., Sandling, J. K., Bengtsson, C., Frodlund, M., Jönsen, A., Eketjäll, S., Jensen-Urstad, K., Gunnarsson, I., Sjöwall, C., Bengtsson, A. A., Eloranta, M. -L, Syvänen, A. -C, Rantapää-Dahlqvist, Solbritt, Criswell, L. A., and Rönnblom, L.

Abstract

Supplement: 2Meeting Abstract: OP0362

Published

2018

2. A polymorphism in the foxo3a promoter is associated with protection from organ damage in SLE-a pilot study.

Author

Criswell L., Hoi A., Morand E., Yeo A., White S., Raghunath S., Franklyn K., Criswell L., Hoi A., Morand E., Yeo A., White S., Raghunath S., and Franklyn K.

Abstract

Aim: Disease expression and outcome vary greatly in SLE. As well as affecting susceptibility, noncoding gene polymorphisms have been reported to influence disease expression, for example indices of severity. FOXO3A is a transcription factor which induces the anti-inflammatory proteins TGFbeta and GILZ. A gain-of-function FOXO3A promoter single-nucleotide polymorphism (SNP), rs12212067, is associated with anti-inflammatory effects in vitro, and improved outcomes in colitis and RA (Lee et al, Cell, 2013). The association of FOXOoxo3a polymorphisms with disease expression in SLE is unknown. We sought to determine the clinical associations of this SNP in SLE. Method(s): SLE patients (ACR criteria) attending a single centre were recruited for a pilot study. Patients seen between 2007-2012 had disease activity (SLEDAI-2k) recorded at each visit. SLICC-SDI criteria (recorded annually) were used to define end-organ damage. Genomic DNA was isolated from whole blood and genotyped with the Immunochip (Illumina) (SNP) microarray. Result(s): 137 SLE patients (84% female, median age 42 years, disease duration 5 years) were studied. Organ damage (SDI) was highly correlated with disease duration (P < 0.0001), and with time-adjusted mean SLEDAI (AMS) (P < 0.0001) and glucocorticoid exposure (P < 0.0001). The distribution of rs12212067 genotypes observed was TT (78.8%) TG (17.5%) and GG (3.7%). The major finding was that rs12212067-G homozygosity was protective against organ damage in the SLICC-SDI domains of renal disease (P = 0.001), vascular events (P = 0.0002), and glucocorticoid-related damage (P < 0.001), compared to rs12212067-T/T and G/T genotypes. rs12212067-G/T heterozygotes were also protected against vascular events. There was no difference between rs12212067 genotypes in total SLICCSDI, glucocorticoid exposure, AMS, or other demographic, clinical or serological variables. Conclusion(s): These data suggest that a gain-of-function FOXO3A promoter SNP exerts a protective ef

Published

2017

3. A polymorphism in the foxo3a promoter is associated with protection from organ damage in SLE-a pilot study.

Author

Criswell L., Hoi A., Morand E., Yeo A., White S., Raghunath S., Franklyn K., Criswell L., Hoi A., Morand E., Yeo A., White S., Raghunath S., and Franklyn K.

Abstract

Aim: Disease expression and outcome vary greatly in SLE. As well as affecting susceptibility, noncoding gene polymorphisms have been reported to influence disease expression, for example indices of severity. FOXO3A is a transcription factor which induces the anti-inflammatory proteins TGFbeta and GILZ. A gain-of-function FOXO3A promoter single-nucleotide polymorphism (SNP), rs12212067, is associated with anti-inflammatory effects in vitro, and improved outcomes in colitis and RA (Lee et al, Cell, 2013). The association of FOXOoxo3a polymorphisms with disease expression in SLE is unknown. We sought to determine the clinical associations of this SNP in SLE. Method(s): SLE patients (ACR criteria) attending a single centre were recruited for a pilot study. Patients seen between 2007-2012 had disease activity (SLEDAI-2k) recorded at each visit. SLICC-SDI criteria (recorded annually) were used to define end-organ damage. Genomic DNA was isolated from whole blood and genotyped with the Immunochip (Illumina) (SNP) microarray. Result(s): 137 SLE patients (84% female, median age 42 years, disease duration 5 years) were studied. Organ damage (SDI) was highly correlated with disease duration (P < 0.0001), and with time-adjusted mean SLEDAI (AMS) (P < 0.0001) and glucocorticoid exposure (P < 0.0001). The distribution of rs12212067 genotypes observed was TT (78.8%) TG (17.5%) and GG (3.7%). The major finding was that rs12212067-G homozygosity was protective against organ damage in the SLICC-SDI domains of renal disease (P = 0.001), vascular events (P = 0.0002), and glucocorticoid-related damage (P < 0.001), compared to rs12212067-T/T and G/T genotypes. rs12212067-G/T heterozygotes were also protected against vascular events. There was no difference between rs12212067 genotypes in total SLICCSDI, glucocorticoid exposure, AMS, or other demographic, clinical or serological variables. Conclusion(s): These data suggest that a gain-of-function FOXO3A promoter SNP exerts a protective ef

Published

2017

4. Genome-wide Association Study and Expression Analysis Identifies CD84 as a Predictor of Response to Etanercept Therapy in Rheumatoid Arthritis

Author

Cui, J., Stahl, E.A., Saevarsdottir, S., Miceli, C., Diogo, D., Trynka, G., Raj, T., Umicevic-Mirkov, M., Canhao, H., Ikari, K., Terao, C., Okada, Y., Wedrén, S., Askling, J., Yamanaka, H., Momohara, S., Taniguchi, A., Ohmura, K., Matsuda, F., Mimori, T., Gupta, N., Kuchroo, M., Morgan, A.W., Isaacs, J.D., Wilson, A.G., Hyrich, K.L., Herenius, M., Doorenspleet, M.E., Tak, P.P., Crusius, J.B., Horst-Bruinsma, I.E. van der, Wolbink, G.T., Riel, P.L. van, Laar, M. van de, Guchelaar (LUMC), H.J., Shadick, N.A., Allaart, C.F., Huizinga, T.W.J., Toes, R.E., Kimberly, R.P., Bridges Jr, S.L., Criswell, L., Moreland, L.W., Fonseca, J.E., Vries, N. de, Stranger, B.E., Jager, P.L. De, Raychaudhuri, S., Weinblatt, M.E., Gregersen, P.K., Mariette, X., Barton, A., Padyukov, L., Coenen, M.J.H., Karlson, E.W., Plenge, R.M., Cui, J., Stahl, E.A., Saevarsdottir, S., Miceli, C., Diogo, D., Trynka, G., Raj, T., Umicevic-Mirkov, M., Canhao, H., Ikari, K., Terao, C., Okada, Y., Wedrén, S., Askling, J., Yamanaka, H., Momohara, S., Taniguchi, A., Ohmura, K., Matsuda, F., Mimori, T., Gupta, N., Kuchroo, M., Morgan, A.W., Isaacs, J.D., Wilson, A.G., Hyrich, K.L., Herenius, M., Doorenspleet, M.E., Tak, P.P., Crusius, J.B., Horst-Bruinsma, I.E. van der, Wolbink, G.T., Riel, P.L. van, Laar, M. van de, Guchelaar (LUMC), H.J., Shadick, N.A., Allaart, C.F., Huizinga, T.W.J., Toes, R.E., Kimberly, R.P., Bridges Jr, S.L., Criswell, L., Moreland, L.W., Fonseca, J.E., Vries, N. de, Stranger, B.E., Jager, P.L. De, Raychaudhuri, S., Weinblatt, M.E., Gregersen, P.K., Mariette, X., Barton, A., Padyukov, L., Coenen, M.J.H., Karlson, E.W., and Plenge, R.M.

Abstract

Contains fulltext : 118481.pdf (publisher's version ) (Open Access)

Published

2013

5. Genome-wide Association Study and Expression Analysis Identifies CD84 as a Predictor of Response to Etanercept Therapy in Rheumatoid Arthritis

Author

Cui, J., Stahl, E.A., Saevarsdottir, S., Miceli, C., Diogo, D., Trynka, G., Raj, T., Umicevic-Mirkov, M., Canhao, H., Ikari, K., Terao, C., Okada, Y., Wedrén, S., Askling, J., Yamanaka, H., Momohara, S., Taniguchi, A., Ohmura, K., Matsuda, F., Mimori, T., Gupta, N., Kuchroo, M., Morgan, A.W., Isaacs, J.D., Wilson, A.G., Hyrich, K.L., Herenius, M., Doorenspleet, M.E., Tak, P.P., Crusius, J.B., Horst-Bruinsma, I.E. van der, Wolbink, G.T., Riel, P.L. van, Laar, M. van de, Guchelaar (LUMC), H.J., Shadick, N.A., Allaart, C.F., Huizinga, T.W.J., Toes, R.E., Kimberly, R.P., Bridges Jr, S.L., Criswell, L., Moreland, L.W., Fonseca, J.E., Vries, N. de, Stranger, B.E., Jager, P.L. De, Raychaudhuri, S., Weinblatt, M.E., Gregersen, P.K., Mariette, X., Barton, A., Padyukov, L., Coenen, M.J.H., Karlson, E.W., Plenge, R.M., Cui, J., Stahl, E.A., Saevarsdottir, S., Miceli, C., Diogo, D., Trynka, G., Raj, T., Umicevic-Mirkov, M., Canhao, H., Ikari, K., Terao, C., Okada, Y., Wedrén, S., Askling, J., Yamanaka, H., Momohara, S., Taniguchi, A., Ohmura, K., Matsuda, F., Mimori, T., Gupta, N., Kuchroo, M., Morgan, A.W., Isaacs, J.D., Wilson, A.G., Hyrich, K.L., Herenius, M., Doorenspleet, M.E., Tak, P.P., Crusius, J.B., Horst-Bruinsma, I.E. van der, Wolbink, G.T., Riel, P.L. van, Laar, M. van de, Guchelaar (LUMC), H.J., Shadick, N.A., Allaart, C.F., Huizinga, T.W.J., Toes, R.E., Kimberly, R.P., Bridges Jr, S.L., Criswell, L., Moreland, L.W., Fonseca, J.E., Vries, N. de, Stranger, B.E., Jager, P.L. De, Raychaudhuri, S., Weinblatt, M.E., Gregersen, P.K., Mariette, X., Barton, A., Padyukov, L., Coenen, M.J.H., Karlson, E.W., and Plenge, R.M.

Abstract

Contains fulltext : 118481.pdf (publisher's version ) (Open Access)

Published

2013

6. Breast Cancer in Systemic Lupus Erythematosus

Author

Tessier Cloutier, B, Clarke, A E, Ramsey-Goldman, R, Wang, Yu, Foulkes, W, Gordon, C, Hansen, J E, Yelin, E, Urowitz, M B, Gladman, D, Fortin, P R, Wallace, D J, Petri, M, Manzi, S, Ginzler, E M, Labrecque, J, Edworthy, S, Dooley, M A, Senécal, J L, Peschken, C A, Bae, S C, Isenberg, D, Rahman, Awahan, Ruiz-Irastorza, G, Hanly, J G, Jacobsen, Søren, Nived, O, Witte, T, Criswell, L A, Barr, S G, Dreyer, L, Sturfelt, G, Bernatsky, S, Tessier Cloutier, B, Clarke, A E, Ramsey-Goldman, R, Wang, Yu, Foulkes, W, Gordon, C, Hansen, J E, Yelin, E, Urowitz, M B, Gladman, D, Fortin, P R, Wallace, D J, Petri, M, Manzi, S, Ginzler, E M, Labrecque, J, Edworthy, S, Dooley, M A, Senécal, J L, Peschken, C A, Bae, S C, Isenberg, D, Rahman, Awahan, Ruiz-Irastorza, G, Hanly, J G, Jacobsen, Søren, Nived, O, Witte, T, Criswell, L A, Barr, S G, Dreyer, L, Sturfelt, G, and Bernatsky, S

Published

2013

7. Preferential Binding to Elk-1 by SLE-Associated IL10 Risk Allele Upregulates IL10 Expression

Author

Sakurai, D., Zhao, J., Deng, Y., Kelly, J. A., Brown, E. E., Harley, J. B., Bae, S. C., Alarcón-Riquelme, M. E., Edberg, J. C., Kimberly, R. P., Ramsey-Goldman, R., Caeiro, F., Soriano, E. R., Bertoli, A., Prigione, C., Ramos, F. A., Romero, E. J., Tsao, B. P., Chen, W., Truedsson, L., Yu, C. Y., Migliarese, S., García, M. A., Marcos, J. C., Eimon, A., Sánchez-Román, J., Battagliotti, C. G., Kaufman, K. M., Vyse, T. J., Jacob, C. O., Gaffney, P. M., Sebastiani, G. D., Ramón, Enrique de, Hahn, B. H., Song, Y. W., Grossman, J. M., Sivils, K. M., James, J. A., Kamen, D. L., Gilkeson, G. S., Niewold, T. B., D'Alfonso, Sandra, Merrill, J. T., Martín, J., Scofield, R. H., Chang, D. M., Criswell, L. A., Langefeld, C. D., Stevens, A. M., Cantor, R. M., Frostegård, Johan, Boackle, S. A., Kim, J. H., Choi, J., Pons-Estel, B. A., Freedman, Barry I., Sabio, José Mario, Anaya, J. M., Ortego-Centeno, N., Callejas-Rubio, J. L., González-Escribano, María Francisca, Buchanan, G., Graf, C. E., Paira, S., Galeazzi, M., Witte, Torsten, Lauwerys, B. R., Endreffy, E., Kovács, L., Vasconcelos, C., Silva, B. M. da, Scherbarth, H. R., Catoggio, L. J., Manni, J., Caprarulo, C., Guillerón, C., Marino, P. C., Motta, E. L., Gamron, S., Drenkard, C., Menso, E., Allievi, A., Roverano, S., Tate, G. A., Bertero, E., Presas, J. L., Navarro, S. M., Parque, S., Grimaudo, S., Palatnik, S. A., Abdala, M., Acevedo, E., Bearzotti, M., Santos, C. D., Alvarellos, A., Berbotto, G. A., Jorfen, M., Marcos, A. I., Perandones, C. E., Cucho, M., Torre, I. G. de la, Ríos, M. C., Moctezuma, J. F., Ceceña, M. M., Petri, M. A., Vilá, Luis M., Reveille, J. D., Alarcón, G. S., Sakurai, D., Zhao, J., Deng, Y., Kelly, J. A., Brown, E. E., Harley, J. B., Bae, S. C., Alarcón-Riquelme, M. E., Edberg, J. C., Kimberly, R. P., Ramsey-Goldman, R., Caeiro, F., Soriano, E. R., Bertoli, A., Prigione, C., Ramos, F. A., Romero, E. J., Tsao, B. P., Chen, W., Truedsson, L., Yu, C. Y., Migliarese, S., García, M. A., Marcos, J. C., Eimon, A., Sánchez-Román, J., Battagliotti, C. G., Kaufman, K. M., Vyse, T. J., Jacob, C. O., Gaffney, P. M., Sebastiani, G. D., Ramón, Enrique de, Hahn, B. H., Song, Y. W., Grossman, J. M., Sivils, K. M., James, J. A., Kamen, D. L., Gilkeson, G. S., Niewold, T. B., D'Alfonso, Sandra, Merrill, J. T., Martín, J., Scofield, R. H., Chang, D. M., Criswell, L. A., Langefeld, C. D., Stevens, A. M., Cantor, R. M., Frostegård, Johan, Boackle, S. A., Kim, J. H., Choi, J., Pons-Estel, B. A., Freedman, Barry I., Sabio, José Mario, Anaya, J. M., Ortego-Centeno, N., Callejas-Rubio, J. L., González-Escribano, María Francisca, Buchanan, G., Graf, C. E., Paira, S., Galeazzi, M., Witte, Torsten, Lauwerys, B. R., Endreffy, E., Kovács, L., Vasconcelos, C., Silva, B. M. da, Scherbarth, H. R., Catoggio, L. J., Manni, J., Caprarulo, C., Guillerón, C., Marino, P. C., Motta, E. L., Gamron, S., Drenkard, C., Menso, E., Allievi, A., Roverano, S., Tate, G. A., Bertero, E., Presas, J. L., Navarro, S. M., Parque, S., Grimaudo, S., Palatnik, S. A., Abdala, M., Acevedo, E., Bearzotti, M., Santos, C. D., Alvarellos, A., Berbotto, G. A., Jorfen, M., Marcos, A. I., Perandones, C. E., Cucho, M., Torre, I. G. de la, Ríos, M. C., Moctezuma, J. F., Ceceña, M. M., Petri, M. A., Vilá, Luis M., Reveille, J. D., and Alarcón, G. S.

Abstract

Immunoregulatory cytokine interleukin-10 (IL-10) is elevated in sera from patients with systemic lupus erythematosus (SLE) correlating with disease activity. The established association of IL10 with SLE and other autoimmune diseases led us to fine map causal variant(s) and to explore underlying mechanisms. We assessed 19 tag SNPs, covering the IL10 gene cluster including IL19, IL20 and IL24, for association with SLE in 15,533 case and control subjects from four ancestries. The previously reported IL10 variant, rs3024505 located at 1 kb downstream of IL10, exhibited the strongest association signal and was confirmed for association with SLE in European American (EA) (P = 2.7×10-8, OR = 1.30), but not in non-EA ancestries. SNP imputation conducted in EA dataset identified three additional SLE-associated SNPs tagged by rs3024505 (rs3122605, rs3024493 and rs3024495 located at 9.2 kb upstream, intron 3 and 4 of IL10, respectively), and SLE-risk alleles of these SNPs were dose-dependently associated with elevated levels of IL10 mRNA in PBMCs and circulating IL-10 protein in SLE patients and controls. Using nuclear extracts of peripheral blood cells from SLE patients for electrophoretic mobility shift assays, we identified specific binding of transcription factor Elk-1 to oligodeoxynucleotides containing the risk (G) allele of rs3122605, suggesting rs3122605 as the most likely causal variant regulating IL10 expression. Elk-1 is known to be activated by phosphorylation and nuclear localization to induce transcription. Of interest, phosphorylated Elk-1 (p-Elk-1) detected only in nuclear extracts of SLE PBMCs appeared to increase with disease activity. Co-expression levels of p-Elk-1 and IL-10 were elevated in SLE T, B cells and monocytes, associated with increased disease activity in SLE B cells, and were best downregulated by ERK inhibitor. Taken together, our data suggest that preferential binding of activated Elk-1 to the IL10 rs3122605-G allele upregulates IL10 expressio

Published

2013

8. Breast Cancer in Systemic Lupus Erythematosus

Author

Tessier Cloutier, B, Clarke, A E, Ramsey-Goldman, R, Wang, Yu, Foulkes, W, Gordon, C, Hansen, J E, Yelin, E, Urowitz, M B, Gladman, D, Fortin, P R, Wallace, D J, Petri, M, Manzi, S, Ginzler, E M, Labrecque, J, Edworthy, S, Dooley, M A, Senécal, J L, Peschken, C A, Bae, S C, Isenberg, D, Rahman, Awahan, Ruiz-Irastorza, G, Hanly, J G, Jacobsen, Søren, Nived, O, Witte, T, Criswell, L A, Barr, S G, Dreyer, L, Sturfelt, G, Bernatsky, S, Tessier Cloutier, B, Clarke, A E, Ramsey-Goldman, R, Wang, Yu, Foulkes, W, Gordon, C, Hansen, J E, Yelin, E, Urowitz, M B, Gladman, D, Fortin, P R, Wallace, D J, Petri, M, Manzi, S, Ginzler, E M, Labrecque, J, Edworthy, S, Dooley, M A, Senécal, J L, Peschken, C A, Bae, S C, Isenberg, D, Rahman, Awahan, Ruiz-Irastorza, G, Hanly, J G, Jacobsen, Søren, Nived, O, Witte, T, Criswell, L A, Barr, S G, Dreyer, L, Sturfelt, G, and Bernatsky, S

Published

2013

9. Analysis of autosomal genes reveals gene-sex interactions and higher total genetic risk in men with systemic lupus erythematosus

Author

Hughes, T., Adler, A. J., Merrill, J. T., Kelly, J. A., Kaufman, K. M., Williams, A. H., Langefeld, C. D., Gilkeson, G. S., Sánchez, Elena, Martín, J., Boackle, S. A., Stevens, A. M., Alarcón, G. S., Niewold, T. B., Brown, E. E., Kimberly, R. P., Edberg, J. C., Ramsey-Goldman, R., Petri, M., Reveille, J. D., Criswell, L. A., Vilá, Luis M., Jacob, C. O., Gaffney, P. M., Moser, K. L., Vyse, T. J., Alarcón-Riquelme, M. E., James, J. A., Tsao, B. P., Scofield, R. H., Harley, J. B., Richardson, B. C., Sawalha, A. H., Frostegård, Johan, Truedsson, L., Ramón, Enrique de, Sabio, José Mario, González-Escribano, María Francisca, Ortego-Centeno, N., Callejas-Rubio, J. L., Sánchez-Román, J., D'Alfonso, Sandra, Migliarese, S., Sebastiani, G. D., Galeazzi, M., Witte, Torsten, Lauwerys, B. R., Endreffy, E., Kovács, L., Vasconcelos, C., Silva, B. M. da, Hughes, T., Adler, A. J., Merrill, J. T., Kelly, J. A., Kaufman, K. M., Williams, A. H., Langefeld, C. D., Gilkeson, G. S., Sánchez, Elena, Martín, J., Boackle, S. A., Stevens, A. M., Alarcón, G. S., Niewold, T. B., Brown, E. E., Kimberly, R. P., Edberg, J. C., Ramsey-Goldman, R., Petri, M., Reveille, J. D., Criswell, L. A., Vilá, Luis M., Jacob, C. O., Gaffney, P. M., Moser, K. L., Vyse, T. J., Alarcón-Riquelme, M. E., James, J. A., Tsao, B. P., Scofield, R. H., Harley, J. B., Richardson, B. C., Sawalha, A. H., Frostegård, Johan, Truedsson, L., Ramón, Enrique de, Sabio, José Mario, González-Escribano, María Francisca, Ortego-Centeno, N., Callejas-Rubio, J. L., Sánchez-Román, J., D'Alfonso, Sandra, Migliarese, S., Sebastiani, G. D., Galeazzi, M., Witte, Torsten, Lauwerys, B. R., Endreffy, E., Kovács, L., Vasconcelos, C., and Silva, B. M. da

Abstract

Objectives: Systemic lupus erythematosus (SLE) is a sexually dimorphic autoimmune disease which is more common in women, but affected men often experience a more severe disease. The genetic basis of sexual dimorphism in SLE is not clearly defined. A study was undertaken to examine sex-specific genetic effects among SLE susceptibility loci. Methods: A total of 18 autosomal genetic susceptibility loci for SLE were genotyped in a large set of patients with SLE and controls of European descent, consisting of 5932 female and 1495 male samples. Sex-specific genetic association analyses were performed. The sex-gene interaction was further validated using parametric and non-parametric methods. Aggregate differences in sex-specific genetic risk were examined by calculating a cumulative genetic risk score for SLE in each individual and comparing the average genetic risk between male and female patients. Results: A significantly higher cumulative genetic risk for SLE was observed in men than in women. (P=4.52x10 -8) A significant sex-gene interaction was seen primarily in the human leucocyte antigen (HLA) region but also in IRF5, whereby men with SLE possess a significantly higher frequency of risk alleles than women. The genetic effect observed in KIAA1542 is specific to women with SLE and does not seem to have a role in men. Conclusions: The data indicate that men require a higher cumulative genetic load than women to develop SLE. These observations suggest that sex bias in autoimmunity could be influenced by autosomal genetic susceptibility loci.

Published

2012

10. A functional haplotype of UBE2L3 confers risk for systemic lupus erythematosus

Author

Wang, Shanshan, Adrianto, I., Wiley, G., Lessard, C. J., Kelly, J. A., Adler, A. J., Glenn, S. B., Williams, A. H., Ziegler, Julie, Comeau, M. E., Marion, M. C., Wakeland, B. E., Liang, C., Kaufman, K. M., Guthridge, J. M., Alarcón-Riquelme, M. E., Alarcón, G. S., Anaya, J. M., Bae, S. C., Kim, J. H., Joo, Y. B., Boackle, S. A., Brown, E. E., Petri, M., Ramsey-Goldman, R., Reveille, J. D., Vilá, Luis M., Criswell, L. A., Edberg, J. C., Freedman, Barry I., Gilkeson, G. S., Jacob, C. O., James, J. A., Kamen, D. L., Kimberly, R. P., Martín, J., Merrill, J. T., Niewold, T. B., Pons-Estel, B. A., Scofield, R. H., Stevens, A. M., Tsao, B. P., Vyse, T. J., Langefeld, C. D., Harley, J. B., Wakeland, E. K., Moser, K. L., Montgomery, C. G., Gaffney, P. M., Wang, Shanshan, Adrianto, I., Wiley, G., Lessard, C. J., Kelly, J. A., Adler, A. J., Glenn, S. B., Williams, A. H., Ziegler, Julie, Comeau, M. E., Marion, M. C., Wakeland, B. E., Liang, C., Kaufman, K. M., Guthridge, J. M., Alarcón-Riquelme, M. E., Alarcón, G. S., Anaya, J. M., Bae, S. C., Kim, J. H., Joo, Y. B., Boackle, S. A., Brown, E. E., Petri, M., Ramsey-Goldman, R., Reveille, J. D., Vilá, Luis M., Criswell, L. A., Edberg, J. C., Freedman, Barry I., Gilkeson, G. S., Jacob, C. O., James, J. A., Kamen, D. L., Kimberly, R. P., Martín, J., Merrill, J. T., Niewold, T. B., Pons-Estel, B. A., Scofield, R. H., Stevens, A. M., Tsao, B. P., Vyse, T. J., Langefeld, C. D., Harley, J. B., Wakeland, E. K., Moser, K. L., Montgomery, C. G., and Gaffney, P. M.

Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease with diverse clinical manifestations characterized by the development of pathogenic autoantibodies manifesting in inflammation of target organs such as the kidneys, skin and joints. Genome-wide association studies have identified genetic variants in the UBE2L3 region that are associated with SLE in subjects of European and Asian ancestry. UBE2L3 encodes an ubiquitin-conjugating enzyme, UBCH7, involved in cell proliferation and immune function. In this study, we sought to further characterize the genetic association in the region of UBE2L3 and use molecular methods to determine the functional effect of the risk haplotype. We identified significant associations between variants in the region of UBE2L3 and SLE in individuals of European and Asian ancestry that exceeded a Bonferroni-corrected threshold (P<1 × 10 -4). A single risk haplotype was observed in all associated populations. Individuals harboring the risk haplotype display a significant increase in both UBE2L3 mRNA expression (P=0.0004) and UBCH7 protein expression (P=0.0068). The results suggest that variants carried on the SLE-associated UBE2L3 risk haplotype influence autoimmunity by modulating UBCH7 expression. © 2012 Macmillan Publishers Limited All rights reserved.

Published

2012

11. Role of MYH9 and APOL1 in African and non-African populations with lupus nephritis

Author

Lin, C. P., Adrianto, I., Lessard, C. J., Kelly, J. A., Kaufman, K. M., Guthridge, J. M., Freedman, Barry I., Anaya, J. M., Alarcón-Riquelme, M. E., Pons-Estel, B. A., Martín, J., Glenn, S. B., Petri, M., Criswell, L. A., Ramsey-Goldman, R., Reveille, J. D., Vilá, Luis M., Gilkeson, G. S., Kamen, D. L., Ziegler, Julie, Jacob, C. O., Rasmussen, A., James, J. A., Kimberly, R. P., Merrill, J. T., Niewold, T. B., Scofield, R. H., Stevens, A. M., Tsao, B. P., Vyse, T. J., Langefeld, C. D., Moser, K. L., Harley, J. B., Gaffney, P. M., Montgomery, C. G., Lin, C. P., Adrianto, I., Lessard, C. J., Kelly, J. A., Kaufman, K. M., Guthridge, J. M., Freedman, Barry I., Anaya, J. M., Alarcón-Riquelme, M. E., Pons-Estel, B. A., Martín, J., Glenn, S. B., Petri, M., Criswell, L. A., Ramsey-Goldman, R., Reveille, J. D., Vilá, Luis M., Gilkeson, G. S., Kamen, D. L., Ziegler, Julie, Jacob, C. O., Rasmussen, A., James, J. A., Kimberly, R. P., Merrill, J. T., Niewold, T. B., Scofield, R. H., Stevens, A. M., Tsao, B. P., Vyse, T. J., Langefeld, C. D., Moser, K. L., Harley, J. B., Gaffney, P. M., and Montgomery, C. G.

Abstract

Systemic lupus erythematosus (SLE) is a complex autoimmune disease characterized by autoantibody production and organ damage. Lupus nephritis (LN) is one of the most severe manifestations of SLE. Multiple studies reported associations between renal diseases and variants in the non-muscle myosin heavy chain 9 (MYH9) and the neighboring apolipoprotein L 1 (APOL1) genes. We evaluated 167 variants spanning MYH9 for association with LN in a multiethnic sample. The two previously identified risk variants in APOL1 were also tested for association with LN in European-Americans (EAs) (N=579) and African-Americans (AAs) (N=407). Multiple peaks of association exceeding a Bonferroni corrected P-value of P<2.03 × 10 -3 were observed between LN and MYH9 in EAs (N=4620), with the most pronounced association at rs2157257 (P=4.7 × 10 -4, odds ratio (OR)=1.205). A modest effect with MYH9 was also detected in Gullah (rs8136069, P=0.0019, OR=2.304). No association between LN and MYH9 was found in AAs, Asians, Amerindians or Hispanics. This study provides the first investigation of MYH9 in LN in non-Africans and of APOL1 in LN in any population, and presents novel insight into the potential role of MYH9 in LN in EAs. © 2012 Macmillan Publishers Limited All rights reserved.

Published

2012

12. Evaluation of the TREX1 gene in a large multi-ancestral lupus cohort

Author

Namjou, B., Kothari, P. H., Kelly, J. A., Glenn, S. B., Ojwang, J. O., Adler, A., Alarcon-Riquelme, Marta E., Gallant, Caroline J., Boackle, S. A., Criswell, L. A., Kimberly, R. P., Brown, E., Edberg, J., Stevens, A. M., Jacob, C. O., Tsao, B. P., Gilkeson, G. S., Kamen, D. L., Merrill, J. T., Petri, M., Goldman, R. R., Vila, L. M., Anaya, J-M, Niewold, T. B., Martin, J., Pons-Estel, B. A., Sabio, J. M., Callejas, J. L., Vyse, T. J., Bae, S-C, Perrino, F. W., Freedman, B. I., Scofield, R. H., Moser, K. L., Gaffney, P. M., James, J. A., Langefeld, C. D., Kaufman, K. M., Harley, J. B., Atkinson, J. P., Namjou, B., Kothari, P. H., Kelly, J. A., Glenn, S. B., Ojwang, J. O., Adler, A., Alarcon-Riquelme, Marta E., Gallant, Caroline J., Boackle, S. A., Criswell, L. A., Kimberly, R. P., Brown, E., Edberg, J., Stevens, A. M., Jacob, C. O., Tsao, B. P., Gilkeson, G. S., Kamen, D. L., Merrill, J. T., Petri, M., Goldman, R. R., Vila, L. M., Anaya, J-M, Niewold, T. B., Martin, J., Pons-Estel, B. A., Sabio, J. M., Callejas, J. L., Vyse, T. J., Bae, S-C, Perrino, F. W., Freedman, B. I., Scofield, R. H., Moser, K. L., Gaffney, P. M., James, J. A., Langefeld, C. D., Kaufman, K. M., Harley, J. B., and Atkinson, J. P.

Abstract

Systemic lupus erythematosus (SLE) is a prototypic autoimmune disorder with a complex pathogenesis in which genetic, hormonal and environmental factors have a role. Rare mutations in the TREX1 gene, the major mammalian 3'-5' exonuclease, have been reported in sporadic SLE cases. Some of these mutations have also been identified in a rare pediatric neurological condition featuring an inflammatory encephalopathy known as Aicardi-Goutieres syndrome (AGS). We sought to investigate the frequency of these mutations in a large multi-ancestral cohort of SLE cases and controls. A total of 40 single-nucleotide polymorphisms (SNPs), including both common and rare variants, across the TREX1 gene, were evaluated in similar to 8370 patients with SLE and similar to 7490 control subjects. Stringent quality control procedures were applied, and principal components and admixture proportions were calculated to identify outliers for removal from analysis. Population-based case-control association analyses were performed. P-values, false-discovery rate q values, and odds ratios (OR) with 95% confidence intervals (CI) were calculated. The estimated frequency of TREX1 mutations in our lupus cohort was 0.5%. Five heterozygous mutations were detected at the Y305C polymorphism in European lupus cases but none were observed in European controls. Five African cases incurred heterozygous mutations at the E266G polymorphism and, again, none were observed in the African controls. A rare homozygous R114H mutation was identified in one Asian SLE patient, whereas all genotypes at this mutation in previous reports for SLE were heterozygous. Analysis of common TREX1 SNPs (minor allele frequency (MAF)>10%) revealed a relatively common risk haplotype in European SLE patients with neurological manifestations, especially seizures, with a frequency of 58% in lupus cases compared with 45% in normal controls (P = 0.0008, OR = 1.73, 95% CI = 1.25-2.39). Finally, the presence or absence of specific autoanti

Published

2011

13. Identification of a systemic lupus erythematosus susceptibility locus at 11p13 between PDHX and CD44 in a multiethnic study

Author

Lessard, C. J., Adrianto, I., Kelly, J. A., Kaufman, K. M., Grundahl, K. M., Adler, A. J., Williams, A. H., Gallant, C., Anaya, J. M., Bae, S. C., Boackle, S. A., Brown, E. E., Chang, D. M., Criswell, L. A., Edberg, J. C., Freedman, Barry I., Gregersen, Peter K., Gilkeson, G. S., Jacob, C. O., James, J. A., Kamen, D. L., Kimberly, R. P., Martín, J., Merrill, J. T., Niewold, T. B., Park, Su-Yeon, Petri, M., Pons-Estel, B. A., Ramsey-Goldman, R., Reveille, J. D., Song, Y. W., Stevens, A. M., Tsao, B. P., Vilá, Luis M., Vyse, T. J., Yu, C. Y., Guthridge, J. M., Bruner, G. R., Langefeld, C. D., Montgomery, C. G., Harley, J. B., Scofield, R. H., Gaffney, P. M., Moser, K. L., Lessard, C. J., Adrianto, I., Kelly, J. A., Kaufman, K. M., Grundahl, K. M., Adler, A. J., Williams, A. H., Gallant, C., Anaya, J. M., Bae, S. C., Boackle, S. A., Brown, E. E., Chang, D. M., Criswell, L. A., Edberg, J. C., Freedman, Barry I., Gregersen, Peter K., Gilkeson, G. S., Jacob, C. O., James, J. A., Kamen, D. L., Kimberly, R. P., Martín, J., Merrill, J. T., Niewold, T. B., Park, Su-Yeon, Petri, M., Pons-Estel, B. A., Ramsey-Goldman, R., Reveille, J. D., Song, Y. W., Stevens, A. M., Tsao, B. P., Vilá, Luis M., Vyse, T. J., Yu, C. Y., Guthridge, J. M., Bruner, G. R., Langefeld, C. D., Montgomery, C. G., Harley, J. B., Scofield, R. H., Gaffney, P. M., and Moser, K. L.

Abstract

Systemic lupus erythematosus (SLE) is considered to be the prototypic autoimmune disease, with a complex genetic architecture influenced by environmental factors. We sought to replicate a putative association at 11p13 not yet exceeding genome-wide significance (p < 5 × 10-8) identified in a genome-wide association study (GWAS). Our GWA scan identified two intergenic SNPs located between PDHX and CD44 showing suggestive evidence of association with SLE in cases of European descent (rs2732552, p = 0.004, odds ratio [OR] = 0.78; rs387619, p = 0.003, OR = 0.78). The replication cohort consisted of >15,000 subjects, including 3562 SLE cases and 3491 controls of European ancestry, 1527 cases and 1811 controls of African American (AA) descent, and 1265 cases and 1260 controls of Asian origin. We observed robust association at both rs2732552 (p = 9.03 × 10-8, OR = 0.83) and rs387619 (p = 7.7 × 10-7, OR = 0.83) in the European samples with pmeta = 1.82 × 10-9 for rs2732552. The AA and Asian SLE cases also demonstrated association at rs2732552 (p = 5 × 10-3, OR = 0.81 and p = 4.3 × 10-4, OR = 0.80, respectively). A meta-analysis of rs2732552 for all racial and ethnic groups studied produced pmeta = 2.36 × 10-13. This locus contains multiple regulatory sites that could potentially affect expression and functions of CD44, a cell-surface glycoprotein influencing immunologic, inflammatory, and oncologic phenotypes, or PDHX, a subunit of the pyruvate dehydrogenase complex. © 2011 The American Society of Human Genetics.

Published

2011

14. Kallikrein genes are associated with lupus and glomerular basement membrane-specific antibody-induced nephritis in mice and humans

Author

Liu, Kui, Li, Quan-Zhen, Delgado-Vega, Angelica M., Abelson, Anna-Karin, Sánchez, Elena, Kelly, Jennifer A., Li, Li, Liu, Yang, Zhou, Jinchun, Yan, Mei, Ye, Qiu, Liu, Shenxi, Xie, Chun, Zhou, Xin J., Chung, Sharon A., Pons-Estel, Bernardo, Witte, Torsten, de Ramón, Enrique, Bae, Sang-Cheol, Barizzone, Nadia, Sebastiani, Gian Domenico, Merrill, Joan T., Gregersen, Peter K., Gilkeson, Gary G., Kimberly, Robert P., Vyse, Timothy J., Kim, Il, D'Alfonso, Sandra, Martin, Javier, Harley, John B., Criswell, Lindsey A., Wakeland, Edward K., Alarcón-Riquelme, Marta E., Mohan, Chandra, Danieli, M.G., Galeazzi, M., Querini, P.R., Migliaresi, S., Scherbarth, H.R., Lopez, J.A., Motta, E.L., Gamron, S., Drenkard, C., Menso, E., Allievi, A., Tate, G.A., Presas, J.L., Palatnik, S.A., Abdala, M., Bearzotti, M., Alvarellos, A., Caeiro, F., Bertoli, A., Paira, S., Roverano, S., Graf, C.E., Bertero, E., Caprarulo, C., Buchanan, G., Guillerón, C., Grimaudo, S., Manni, J., Catoggio, L.J., Soriano, E.R., Santos, C.D., Prigione, C., Ramos, F.A., Navarro, S.M., Berbotto, G.A., Jorfen, M., Romero, E.J., Garcia, M.A., Marcos, J.C., Marcos, A.I., Perandones, C.E., Eimon, A., Battagliotti, C.G., Armadi-Simab, K., Gross, W.L., Gromica-Ihle, E., Peter, H.H., Manger, K., Schnarr, S., Zeidler, H., Schmidt, R.E., Ortego, N., Callejas, J.L., Jiménez-Alonso, J., Sabio, M., Sánchez-Román, J., Garcia-Hernandez, F.J., Camps, M., López-Nevot, M.A., González-Escribano, M.F., Harley, J.H., Riquelme, M.A., Kimberly, R., Criswell, L., Langefeld, C., Tsao, B., Jacob, C., Liu, Kui, Li, Quan-Zhen, Delgado-Vega, Angelica M., Abelson, Anna-Karin, Sánchez, Elena, Kelly, Jennifer A., Li, Li, Liu, Yang, Zhou, Jinchun, Yan, Mei, Ye, Qiu, Liu, Shenxi, Xie, Chun, Zhou, Xin J., Chung, Sharon A., Pons-Estel, Bernardo, Witte, Torsten, de Ramón, Enrique, Bae, Sang-Cheol, Barizzone, Nadia, Sebastiani, Gian Domenico, Merrill, Joan T., Gregersen, Peter K., Gilkeson, Gary G., Kimberly, Robert P., Vyse, Timothy J., Kim, Il, D'Alfonso, Sandra, Martin, Javier, Harley, John B., Criswell, Lindsey A., Wakeland, Edward K., Alarcón-Riquelme, Marta E., Mohan, Chandra, Danieli, M.G., Galeazzi, M., Querini, P.R., Migliaresi, S., Scherbarth, H.R., Lopez, J.A., Motta, E.L., Gamron, S., Drenkard, C., Menso, E., Allievi, A., Tate, G.A., Presas, J.L., Palatnik, S.A., Abdala, M., Bearzotti, M., Alvarellos, A., Caeiro, F., Bertoli, A., Paira, S., Roverano, S., Graf, C.E., Bertero, E., Caprarulo, C., Buchanan, G., Guillerón, C., Grimaudo, S., Manni, J., Catoggio, L.J., Soriano, E.R., Santos, C.D., Prigione, C., Ramos, F.A., Navarro, S.M., Berbotto, G.A., Jorfen, M., Romero, E.J., Garcia, M.A., Marcos, J.C., Marcos, A.I., Perandones, C.E., Eimon, A., Battagliotti, C.G., Armadi-Simab, K., Gross, W.L., Gromica-Ihle, E., Peter, H.H., Manger, K., Schnarr, S., Zeidler, H., Schmidt, R.E., Ortego, N., Callejas, J.L., Jiménez-Alonso, J., Sabio, M., Sánchez-Román, J., Garcia-Hernandez, F.J., Camps, M., López-Nevot, M.A., González-Escribano, M.F., Harley, J.H., Riquelme, M.A., Kimberly, R., Criswell, L., Langefeld, C., Tsao, B., and Jacob, C.

Abstract

Immune-mediated nephritis contributes to disease in systemic lupus erythematosus, Goodpasture syndrome (caused by antibodies specific for glomerular basement membrane [anti-GBM antibodies]), and spontaneous lupus nephritis. Inbred mouse strains differ in susceptibility to anti-GBM antibody-induced and spontaneous lupus nephritis. This study sought to clarify the genetic and molecular factors that maybe responsible for enhanced immune-mediated renal disease in these models. When the kidneys of 3 mouse strains sensitive to anti-GBM antibody-induced nephritis were compared with those of 2 control strains using microarray analysis, one-fifth of the underexpressed genes belonged to the kallikrein gene family,which encodes serine esterases. Mouse strains that upregulated renal and urinary kallikreins exhibited less evidence of disease. Antagonizing the kallikrein pathway augmented disease, while agonists dampened the severity of anti-GBM antibody-induced nephritis. In addition, nephritis-sensitive mouse strains had kallikrein haplotypes that were distinct from those of control strains, including several regulatory polymorphisms,some of which were associated with functional consequences. Indeed, increased susceptibility to anti-GBM antibody-induced nephritis and spontaneous lupus nephritis was achieved by breeding mice with a genetic interval harboring the kallikrein genes onto a disease-resistant background. Finally, both human SLE and spontaneous lupus nephritis were found to be associated with kallikrein genes, particularly KLK1 and the KLK3 promoter, when DNA SNPs from independent cohorts of SLE patients and controls were compared. Collectively, these studies suggest that kallikreins are protective disease-associated genes in anti-GBM antibody-induced nephritis and lupus.

Published

2009

15. Structure and phase transitions of monolayers of intermediate-length n-alkanes on graphite studied by neutron diffraction and molecular dynamics simulation

Author

Diama, A., Matthies, B., Herwig, K. W., Hansen, Flemming Yssing, Criswell, L., Mo, H., Bai, M., Taub, H., Diama, A., Matthies, B., Herwig, K. W., Hansen, Flemming Yssing, Criswell, L., Mo, H., Bai, M., and Taub, H.

Abstract

We present evidence from neutron diffraction measurements and molecular dynamics (MD) simulations of three different monolayer phases of the intermediate-length alkanes tetracosane (n-C24H50 denoted as C24) and dotriacontane (n-C32H66 denoted as C32) adsorbed on a graphite basal-plane surface. Our measurements indicate that the two monolayer films differ principally in the transition temperatures between phases. At the lowest temperatures, both C24 and C32 form a crystalline monolayer phase with a rectangular-centered (RC) structure. The two sublattices of the RC structure each consists of parallel rows of molecules in their all-trans conformation aligned with their long axis parallel to the surface and forming so-called lamellas of width approximately equal to the all-trans length of the molecule. The RC structure is uniaxially commensurate with the graphite surface in its [110] direction such that the distance between molecular rows in a lamella is 4.26 angstrom = root 3a(g), where a(g) = 2.46 angstrom is the lattice constant of the graphite basal plane. Molecules in adjacent rows of a lamella alternate in orientation between the carbon skeletal plane being parallel and perpendicular to the graphite surface. Upon heating, the crystalline monolayers transform to a "smectic" phase in which the inter-row spacing within a lamella expands by similar to 10% and the molecules are predominantly oriented with the carbon skeletal plane parallel to the graphite surface. In the smectic phase, the MD simulations show evidence of broadening of the lamella boundaries as a result of molecules diffusing parallel to their long axis. At still higher temperatures, they indicate that the introduction of gauche defects into the alkane chains drives a melting transition to a monolayer fluid phase as reported previously. (C) 2009 American Institute of Physics. [DOI: 10.1063/1.3212095]

Published

2009

16. Association of PDCD1 genetic variation with risk and clinical manifestations of systemic lupus erythematosus in a multiethnic cohort

Author

Thorburn, C. M., Prokunina-Olsson, L., Sterba, K. A., Lum, R. F., Seldin, M. F., Alarcon-Riquelme, Marta E., Criswell, L. A., Thorburn, C. M., Prokunina-Olsson, L., Sterba, K. A., Lum, R. F., Seldin, M. F., Alarcon-Riquelme, Marta E., and Criswell, L. A.

Abstract

We evaluated the roles of five single-nucleotide polymorphisms (SNPs) within PDCD1, and haplotypes defined by these SNPs, for the development of systemic lupus erythematosus (SLE) and specific sub-phenotypes (nephritis, antiphospholipid antibody positive, arthritis and double-stranded DNA positive) within a multiethnic US cohort of 1036 patients. Family based analyses were performed using 844 simplex families from four ethnic groups (Caucasian, Asian, Hispanic and African American). Subjects were genotyped for five 'tag' SNPs (selected from 15) to provide complete genetic information in all main ethnic groups. We employed transmission disequilibrium testing to assess risk for SLE by allele or haplotype, and multiple logistic regression analysis of SLE cases to examine associations with specific sub-phenotypes. In family based analyses, a haplotype containing the PD1.3A allele was significantly associated with SLE susceptibility among Caucasian families (P=0.01). Among Hispanic families, two novel SNPs were associated with SLE risk (P=0.005 and 0.01). In multivariate logistic regression analyses, five haplotypes were associated with specific sub-phenotypes among the different ethnic groups. These results suggest that PDCD1 genetic variation influences the risk and expression of SLE and that these associations vary according to ethnic background.

Published

2007

17. Comparative study of normal and branched alkane monolayer films adsorbed on a solid surface. I. Structure

Author

Enevoldsen, Ann Dorrit, Hansen, Flemming Yssing, Diama, A., Criswell, L., Taub, H., Enevoldsen, Ann Dorrit, Hansen, Flemming Yssing, Diama, A., Criswell, L., and Taub, H.

Abstract

The structure of a monolayer film of the branched alkane squalane (C30H62) adsorbed on graphite has been studied by neutron diffraction and molecular dynamics (MD) simulations and compared with a similar study of the n-alkane tetracosane (n-C24H52). Both molecules have 24 carbon atoms along their backbone and squalane has, in addition, six methyl side groups. Upon adsorption, there are significant differences as well as similarities in the behavior of these molecular films. Both molecules form ordered structures at low temperatures; however, while the melting point of the two-dimensional (2D) tetracosane film is roughly the same as the bulk melting point, the surface strongly stabilizes the 2D squalane film such that its melting point is 91 K above its value in bulk. Therefore, squalane, like tetracosane, will be a poor lubricant in those nanoscale devices that require a fluid lubricant at room temperature. The neutron diffraction data show that the translational order in the squalane monolayer is significantly less than in the tetracosane monolayer. The authors' MD simulations suggest that this is caused by a distortion of the squalane molecules upon adsorption on the graphite surface. When the molecules are allowed to relax on the surface, they distort such that all six methyl groups point away from the surface. This results in a reduction in the monolayer's translational order characterized by a decrease in its coherence length and hence a broadening of the diffraction peaks. The MD simulations also show that the melting mechanism in the squalane monolayer is the same footprint reduction mechanism found in the tetracosane monolayer, where a chain melting drives the lattice melting.

Published

2007

18. Comparative study of normal and branched alkane monolayer films adsorbed on a solid surface. I. Structure

Author

Enevoldsen, Ann Dorrit, Hansen, Flemming Yssing, Diama, A., Criswell, L., Taub, H., Enevoldsen, Ann Dorrit, Hansen, Flemming Yssing, Diama, A., Criswell, L., and Taub, H.

Abstract

The structure of a monolayer film of the branched alkane squalane (C30H62) adsorbed on graphite has been studied by neutron diffraction and molecular dynamics (MD) simulations and compared with a similar study of the n-alkane tetracosane (n-C24H52). Both molecules have 24 carbon atoms along their backbone and squalane has, in addition, six methyl side groups. Upon adsorption, there are significant differences as well as similarities in the behavior of these molecular films. Both molecules form ordered structures at low temperatures; however, while the melting point of the two-dimensional (2D) tetracosane film is roughly the same as the bulk melting point, the surface strongly stabilizes the 2D squalane film such that its melting point is 91 K above its value in bulk. Therefore, squalane, like tetracosane, will be a poor lubricant in those nanoscale devices that require a fluid lubricant at room temperature. The neutron diffraction data show that the translational order in the squalane monolayer is significantly less than in the tetracosane monolayer. The authors' MD simulations suggest that this is caused by a distortion of the squalane molecules upon adsorption on the graphite surface. When the molecules are allowed to relax on the surface, they distort such that all six methyl groups point away from the surface. This results in a reduction in the monolayer's translational order characterized by a decrease in its coherence length and hence a broadening of the diffraction peaks. The MD simulations also show that the melting mechanism in the squalane monolayer is the same footprint reduction mechanism found in the tetracosane monolayer, where a chain melting drives the lattice melting.

Published

2007

19. Comparative study of normal and branched alkane monolayer films adsorbed on a solid surface. I. Structure

Author

Enevoldsen, Ann Dorrit, Hansen, Flemming Yssing, Diama, A., Criswell, L., Taub, H., Enevoldsen, Ann Dorrit, Hansen, Flemming Yssing, Diama, A., Criswell, L., and Taub, H.

Abstract

The structure of a monolayer film of the branched alkane squalane (C30H62) adsorbed on graphite has been studied by neutron diffraction and molecular dynamics (MD) simulations and compared with a similar study of the n-alkane tetracosane (n-C24H52). Both molecules have 24 carbon atoms along their backbone and squalane has, in addition, six methyl side groups. Upon adsorption, there are significant differences as well as similarities in the behavior of these molecular films. Both molecules form ordered structures at low temperatures; however, while the melting point of the two-dimensional (2D) tetracosane film is roughly the same as the bulk melting point, the surface strongly stabilizes the 2D squalane film such that its melting point is 91 K above its value in bulk. Therefore, squalane, like tetracosane, will be a poor lubricant in those nanoscale devices that require a fluid lubricant at room temperature. The neutron diffraction data show that the translational order in the squalane monolayer is significantly less than in the tetracosane monolayer. The authors' MD simulations suggest that this is caused by a distortion of the squalane molecules upon adsorption on the graphite surface. When the molecules are allowed to relax on the surface, they distort such that all six methyl groups point away from the surface. This results in a reduction in the monolayer's translational order characterized by a decrease in its coherence length and hence a broadening of the diffraction peaks. The MD simulations also show that the melting mechanism in the squalane monolayer is the same footprint reduction mechanism found in the tetracosane monolayer, where a chain melting drives the lattice melting.

Published

2007

20. Intramolecular diffusive motion in alkane monolayers studied by high-resolution quasielastic neutron scattering and molecular dynamics simulations

Author

Hansen, Flemming Yssing, Criswell, L., Fuhrmann, D, Herwig, K.W., Diama, A., Dimeo, R.M., Neumann, D.A., Volkmann, U.G., Taub, H., Hansen, Flemming Yssing, Criswell, L., Fuhrmann, D, Herwig, K.W., Diama, A., Dimeo, R.M., Neumann, D.A., Volkmann, U.G., and Taub, H.

Abstract

Molecular dynamics simulations of a tetracosane (n-C24H50) monolayer adsorbed on a graphite basal-plane surface show that there are diffusive motions associated with the creation and annihilation of gauche defects occurring on a time scale of similar to0.1-4 ns. We present evidence that these relatively slow motions are observable by high-energy-resolution quasielastic neutron scattering (QNS) thus demonstrating QNS as a technique, complementary to nuclear magnetic resonance, for studying conformational dynamics on a nanosecond time scale in molecular monolayers.

Published

2004

21. Intramolecular diffusive motion in alkane monolayers studied by high-resolution quasielastic neutron scattering and molecular dynamics simulations

Author

Hansen, Flemming Yssing, Criswell, L., Fuhrmann, D, Herwig, K.W., Diama, A., Dimeo, R.M., Neumann, D.A., Volkmann, U.G., Taub, H., Hansen, Flemming Yssing, Criswell, L., Fuhrmann, D, Herwig, K.W., Diama, A., Dimeo, R.M., Neumann, D.A., Volkmann, U.G., and Taub, H.

Abstract

Molecular dynamics simulations of a tetracosane (n-C24H50) monolayer adsorbed on a graphite basal-plane surface show that there are diffusive motions associated with the creation and annihilation of gauche defects occurring on a time scale of similar to0.1-4 ns. We present evidence that these relatively slow motions are observable by high-energy-resolution quasielastic neutron scattering (QNS) thus demonstrating QNS as a technique, complementary to nuclear magnetic resonance, for studying conformational dynamics on a nanosecond time scale in molecular monolayers.

Published

2004

22. Slow Diffusive Motions in a Monolayer of Tetracosane Molecules Adsorbed on Graphite

Author

Taub, H., Hansen, Flemming Yssing, Criswell, L., Fuhrmann, D., Herwig, K.W., Diama, A., Mo, H., Dimeo, R.M., Neumann, D.A., Volkmann, U.G., Taub, H., Hansen, Flemming Yssing, Criswell, L., Fuhrmann, D., Herwig, K.W., Diama, A., Mo, H., Dimeo, R.M., Neumann, D.A., and Volkmann, U.G.

Abstract

Monolayers of intermediate-length alkane molecules such as tetracosane (n-C24H50 or C24) serve as prototypes for studying the interfacial dynamics of more complex polymers, including bilayer lipid membranes. Using high-resolution quasielastic neutron scattering (QNS) and exfoliated graphite substrates, we have investigated the relatively slow diffusive motion in C24 monolayers on an energy/time scale of similar to1-36 teV (similar to0.1-4 ns). Upon heating, we first observe QNS in the crystalline phase at similar to160 K. From the crystalline-to-smectic phase transition at similar to215 K to a temperature of similar to230 K, we observe the QNS energy width to be dispersionless, consistent with molecular dynamics simulations showing rotational motion of the molecules about their long axis. At 260 K, the QNS energy width begins to increase with wave vector transfer, suggesting onset of nonuniaxial rotational motion and bounded translational motion. We continue to observe QNS up to the monolayer melting temperature at similar to340 K where our simulations indicate that the only motion slow enough to be visible within our energy window results from the creation of gauche defects in the molecules.

Published

2004

23. Intramolecular diffusive motion in alkane monolayers studied by high-resolution quasielastic neutron scattering and molecular dynamics simulations

Author

Hansen, Flemming Yssing, Criswell, L., Fuhrmann, D, Herwig, K.W., Diama, A., Dimeo, R.M., Neumann, D.A., Volkmann, U.G., Taub, H., Hansen, Flemming Yssing, Criswell, L., Fuhrmann, D, Herwig, K.W., Diama, A., Dimeo, R.M., Neumann, D.A., Volkmann, U.G., and Taub, H.

Abstract

Molecular dynamics simulations of a tetracosane (n-C24H50) monolayer adsorbed on a graphite basal-plane surface show that there are diffusive motions associated with the creation and annihilation of gauche defects occurring on a time scale of similar to0.1-4 ns. We present evidence that these relatively slow motions are observable by high-energy-resolution quasielastic neutron scattering (QNS) thus demonstrating QNS as a technique, complementary to nuclear magnetic resonance, for studying conformational dynamics on a nanosecond time scale in molecular monolayers.

Published

2004