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Abstract Number: 370

Double Positivity of RA Serologies More Prevalent Yet Associated with Clinical Response in Ethnic Minority Patients with Rheumatoid Arthritis

Mercedes Quinones1, Sharon Dowell2, Ignacio Garcia-Valladares3, Gail S. Kerr4, Christopher Swearingen5, Luis R. Espinoza6, Yusuf Yazici7, Edward L. Treadwell8, Theresa Lawrence Ford9, Yvonne Sherrer10, Angelia Mosley-WIlliams11, Rodolfo Perez Alamino12, Chunqiao Luo13, Akgun Ince14, Adrian Godoy2 and John Amatruda15, 1Division of Rheumatology, Howard University Hospital, Washington, DC, 2Division of Rheumatology, Howard University, Washington, DC, 3Immunology and Rheumatology, Hospital General de Occidente, Zapopan, Jal., Mexico, 4Rheumatology, Washington DC VAMC, Georgetown and Howard University, Washington, DC, 5Pediatrics and Biostatistics, University of Arkansas, Little Rock, AR, 6Medicine-Section of Rheum, LSU Medical Center, New Orleans, LA, 7Department of Medicine, Division of Rheumatology, New York University School of Medicine, New York, NY, 8Dept Medicine Div of Rheum, East Carolina University, Greenville, NC, 9North Georgia Rheumatology Group, PC, Lawrenceville, GA, 10Rheum/Immunology, Centre Rheum Immunol Arthritis, Fort Lauderdale, FL, 11Rheumatology, Detroit VAMC, Detroit, MI, 12internal Medicine, LSUHSC, New Orleans, LA, 13University of Arkansas for Medical Sciences, Little Rock, AR, 14Arthitis Consultants Inc, St. Louis University, St. Louis, MO, 15Rheumatology, Howard University, Washington, DC

Meeting: 2014 ACR/ARHP Annual Meeting

Keywords: ACPA, Clinical Response and Rheumatoid Factor

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Session Information

Title: Rheumatoid Arthritis - Clinical Aspects: Novel Biomarkers and Other Measurements of Disease Activity

Session Type: Abstract Submissions (ACR)

Double Positivity of RA Serologies More Prevalent But Associated with Clinical Response in a Diverse Ethnic Cohort with Rheumatoid Arthritis

Background/Purpose:  The presence of both the anti-citrullinated peptide antibody (ACPA) and a rheumatoid factor (RF) are associated with RA disease severity and portend a poor prognosis. Whether ethnic minorities differ in the prevalence of RA-related serologies from Caucasian RA counterparts is unknown, as is their role as determinants of a clinical response in this patient subset.

Methods: Ethnic Minority RA Consortium (EMRAC) patients with at least one follow up visit were evaluated. Comparisons of demographic (age, gender, race, education, smoking), RA disease status (RF, ACPA, nodules/erosions), RA treatment (prednisone, DMARD, biologics) variables amongst ethnic subsets were made as well as frequencies of clinical response (D MDHAQ – 0.3 and D RAPID3 -3.6) from baseline. Baseline differences between ethnic subsets were compared using Chi-square for categorical and Kruskal-Wallis for continuous variables. Logistic regression associating outcome at follow up and between ethnic subsets were estimated, adjusting for age, smoking, race, education, baseline RAPID3, and double positivity of RA-related serologies.

Results: Follow up visits in 671 EMRAC patients provided data for analyses (Table). African American patients were older (p=0.02), and had longer follow up compared to either Caucasians or Hispanics (p< 0.001). Either a positive ACPA (60%, 46.3% vs 14.3%, respectively, p<0.001) or RF (79.6%, 71.7%, respectively vs 42.1%, p<0.001) were more frequent in AA and Hispanics versus Caucasian patients. In patients who were double positive, the odds ratio for a clinical response was 2.7 (95% CI 1.37, 5.35) for MDHAQ and 3 fold (95% CI 1.37, 6.76) for RAPID3.  There was a greater frequency of both ACPA+/RF+ in ethnic subsets who had a clinical response in both MDHAQ (AA 57.9%, Hispanics 46.9% vs Caucasian 16.7%) and RAPID3 (AA 64.9%, Hispanic 55% vs Caucasian 17.9%). Hispanic patients with RF+/CCP+ had a 67% increased odds of a RAPID response compared to Caucasians and 8% to AA, while AA had a 55% increase in odds for clinical response compared to Caucasians – but none achieving statistical significance.

Conclusion: In a diverse cohort, double positivity of RA-related serologies while more prevalent, are associated with increased odds of a clinical response regardless of ethnicity

 

RAPID3 Outcomes by Race and Double Positive RA Serology Status

HAQ Response

 Caucasian

 African-American

 Hispanic

 RF-ACPA-

 40(66.7%)

 15(15.8%)

 11(34.4%)

 RF+ACPA-

 10(16.7%)

 20(21.1%)

 5(15.6%)

 RF-ACPA+

 0(0%)

 5(5.3%)

 1(3.1%)

 RF+ACPA+

 10(16.7%)

 55(57.9%)

 15(46.9%)

RAPID Response

 RF-ACPA-

 27(69.2%)

 11(19.3%)

 6(30%)

 RF+ACPA-

 4(10.3%)

 6(10.5%)

 3(15%)

 RF-ACPA+

 1(2.6%)

 3(5.3%)

 0(0%)

 RF+ACPA+

 7(17.9%)

 37(64.9%)

 11(55%)

 


Disclosure:

M. Quinones,

Genentech and Biogen IDEC Inc.,

2,

Pfizer Inc,

2,

Bristol-Myers Squibb,

2;

S. Dowell,

Genentech and Biogen IDEC Inc.,

2,

Pfizer,

2,

Bristol-Myers Squibb,

2;

I. Garcia-Valladares,

Genentech and Biogen IDEC Inc.,

2,

Pfizer,

2,

Bristol-Myers Squibb,

2;

G. S. Kerr,

Genentech and Biogen IDEC Inc.,

2,

Bristol-Myers Squibb,

2,

Pfizer Inc,

2;

C. Swearingen,

Genentech and Biogen IDEC Inc.,

2,

Pfizer Inc,

2,

Bristol-Myers Squibb,

2;

L. R. Espinoza,

Genentech and Biogen IDEC Inc.,

2,

Pfizer,

2,

Bristol-Myers Squibb,

2;

Y. Yazici,

Genentech and Biogen IDEC Inc.,

2,

Pfizer Inc,

2,

Bristol-Myers Squibb,

2,

Abbvie,

5,

Bristol-Myers Squibb,

5,

Celgene,

5;

E. L. Treadwell,

Genentech and Biogen IDEC Inc.,

2,

Pfizer,

2,

Bristol-Myers Squibb,

2;

T. Lawrence Ford,

Genentech and Biogen IDEC Inc.,

2,

Pfizer Inc,

2,

Bristol-Myers Squibb,

2,

Human Genome Sciences, Inc.,

2,

Abbive,

2,

Eli Lilly and Company,

2,

Roche Pharmaceuticals,

2,

Bristol-Myers Squibb,

9,

Questcor,

8,

Abbvie,

8,

UCB,

8,

Pfizer Inc,

8,

Amgen,

8,

Takeda,

8,

Actelion Pharmaceuticals US,

8;

Y. Sherrer,

Genentech,

2,

Pfizer Inc,

2,

Bristol-Myers Squibb,

2;

A. Mosley-WIlliams,

Genentech and Biogen IDEC Inc.,

2,

Pfizer Inc,

2,

Bristol-Myers Squibb,

2;

R. Perez Alamino,

Genentech and Biogen IDEC Inc.,

2,

Pfizer,

2,

Bristol-Myers Squibb,

2;

C. Luo,
None;

A. Ince,

Genentech and Biogen IDEC Inc.,

2,

Pfizer Inc,

2,

Bristol-Myers Squibb,

2;

A. Godoy,
None;

J. Amatruda,
None.

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