Autoantibody profiling to follow evolution of lupus syndromes

Nancy J. Olsen; Quan Zhen Li; Jiexia Quan; Ling Wang; Azza Mutwally; David R. Karp

doi:10.1186/ar3927

Autoantibody profiling to follow evolution of lupus syndromes

Nancy J. Olsen, Quan Zhen Li, Jiexia Quan, Ling Wang, Azza Mutwally, David R. Karp

Research output: Contribution to journal › Article › peer-review

68 Scopus citations

Abstract

Introduction: Identification of patients who are in early stages of lupus is currently done through clinical evaluation and is not greatly facilitated by available diagnostic tests. Profiling for patient characteristics and antibody specificities that predict disease would enhance the ability of physicians to identify and treat early cases prior to onset of organ damaging illness.Methods: A group of 22 patients with 4 or fewer diagnostic criteria for lupus were studied for changes in clinical and autoantibody profiles after a mean follow up period of 2.4 years. An array with more than 80 autoantigens was used to profile immunoglobulin G (IgG) and immunoglobulin M (IgM) autoantibodies. Correlations with clinical disease progression were examined.Results: 3 of the 22 patients (14%) added sufficient criteria during follow up to satisfy a diagnosis of systemic lupus erythematosus (SLE) or to acquire a diagnosis of SLE renal disease. Patients who progressed were all females and were younger than those who did not progress (P=0.00054). IgG but not IgM autoreactivity showed greater increases in the progressor group than in the non-progressor group (P=0.047). IgG specificities that were higher at baseline in progressors included proliferating cell nuclear antigen (PCNA), beta 2 microglobulin, C1q and hemocyanin (P<0.019). Progressors had significant increases in La/SSB and liver cytosol type 1 (LC1) IgG autoantibodies over the period of evaluation (P≤0.0072). A quantitative risk profile generated from baseline demographic and autoantibody variables yielded highly different scores for the progressor and non-progressor groups (P=1.38 × 10 ^-7). Conclusions: In addition to demographic features, autoantibody profiles using an expanded array of specificities were correlated with the risk of progressive disease in patients with lupus. These findings suggest the feasibility of developing a simple diagnostic that could be applied by nonspecialists to screen for lupus and permit effective triage for specialty care.

Original language	English (US)
Article number	R174
Journal	Arthritis Research and Therapy
Volume	14
Issue number	4
DOIs	https://doi.org/10.1186/ar3927
State	Published - Jul 27 2012

ASJC Scopus subject areas

Rheumatology
Immunology and Allergy
Immunology

Access to Document

10.1186/ar3927

Cite this

@article{9f057dc3c9d94998ac4312aeb70ab4a7,

title = "Autoantibody profiling to follow evolution of lupus syndromes",

abstract = "Introduction: Identification of patients who are in early stages of lupus is currently done through clinical evaluation and is not greatly facilitated by available diagnostic tests. Profiling for patient characteristics and antibody specificities that predict disease would enhance the ability of physicians to identify and treat early cases prior to onset of organ damaging illness.Methods: A group of 22 patients with 4 or fewer diagnostic criteria for lupus were studied for changes in clinical and autoantibody profiles after a mean follow up period of 2.4 years. An array with more than 80 autoantigens was used to profile immunoglobulin G (IgG) and immunoglobulin M (IgM) autoantibodies. Correlations with clinical disease progression were examined.Results: 3 of the 22 patients (14%) added sufficient criteria during follow up to satisfy a diagnosis of systemic lupus erythematosus (SLE) or to acquire a diagnosis of SLE renal disease. Patients who progressed were all females and were younger than those who did not progress (P=0.00054). IgG but not IgM autoreactivity showed greater increases in the progressor group than in the non-progressor group (P=0.047). IgG specificities that were higher at baseline in progressors included proliferating cell nuclear antigen (PCNA), beta 2 microglobulin, C1q and hemocyanin (P<0.019). Progressors had significant increases in La/SSB and liver cytosol type 1 (LC1) IgG autoantibodies over the period of evaluation (P≤0.0072). A quantitative risk profile generated from baseline demographic and autoantibody variables yielded highly different scores for the progressor and non-progressor groups (P=1.38 × 10 -7). Conclusions: In addition to demographic features, autoantibody profiles using an expanded array of specificities were correlated with the risk of progressive disease in patients with lupus. These findings suggest the feasibility of developing a simple diagnostic that could be applied by nonspecialists to screen for lupus and permit effective triage for specialty care.",

author = "Olsen, {Nancy J.} and Li, {Quan Zhen} and Jiexia Quan and Ling Wang and Azza Mutwally and Karp, {David R.}",

note = "Funding Information: NJO has equity interest in ArthroChip LLC and research grants from Roche and Savient Pharmaceuticals. DRK has research grants from Human Genome Sciences and Centocor. The other authors have no competing interests. Funding Information: This work was supported by NIH/NIAMS P50AR0455503. We appreciate the assistance of Justin Ribault, Maha Yousif, Pratik Doshi and Tiffany Lin for enrolling and evaluating the individuals in DRADR. Michelle Christadoss and Ferdicia Carr-Johnson processed the samples and carried out the ANA measurements. Benjamin F Chong, MD, and Heidi Jacobe, MD, of the Department of Dermatology at UT Southwestern shared with us a set of skin-specific autoantigens for inclusion on the protein arrays, and we appreciate their input. We are also grateful to Chandra Mohan, MBBS, PhD and Ward Wakeland, PhD, for helpful discussions and support. This work is dedicated to the memory of our colleague Valerie K Branch, MS, MBA.",

year = "2012",

month = jul,

day = "27",

doi = "10.1186/ar3927",

language = "English (US)",

volume = "14",

journal = "Arthritis Research and Therapy",

issn = "1478-6354",

publisher = "BioMed Central",

number = "4",

}

TY - JOUR

T1 - Autoantibody profiling to follow evolution of lupus syndromes

AU - Olsen, Nancy J.

AU - Li, Quan Zhen

AU - Quan, Jiexia

AU - Wang, Ling

AU - Mutwally, Azza

AU - Karp, David R.

N1 - Funding Information: NJO has equity interest in ArthroChip LLC and research grants from Roche and Savient Pharmaceuticals. DRK has research grants from Human Genome Sciences and Centocor. The other authors have no competing interests. Funding Information: This work was supported by NIH/NIAMS P50AR0455503. We appreciate the assistance of Justin Ribault, Maha Yousif, Pratik Doshi and Tiffany Lin for enrolling and evaluating the individuals in DRADR. Michelle Christadoss and Ferdicia Carr-Johnson processed the samples and carried out the ANA measurements. Benjamin F Chong, MD, and Heidi Jacobe, MD, of the Department of Dermatology at UT Southwestern shared with us a set of skin-specific autoantigens for inclusion on the protein arrays, and we appreciate their input. We are also grateful to Chandra Mohan, MBBS, PhD and Ward Wakeland, PhD, for helpful discussions and support. This work is dedicated to the memory of our colleague Valerie K Branch, MS, MBA.

PY - 2012/7/27

Y1 - 2012/7/27

N2 - Introduction: Identification of patients who are in early stages of lupus is currently done through clinical evaluation and is not greatly facilitated by available diagnostic tests. Profiling for patient characteristics and antibody specificities that predict disease would enhance the ability of physicians to identify and treat early cases prior to onset of organ damaging illness.Methods: A group of 22 patients with 4 or fewer diagnostic criteria for lupus were studied for changes in clinical and autoantibody profiles after a mean follow up period of 2.4 years. An array with more than 80 autoantigens was used to profile immunoglobulin G (IgG) and immunoglobulin M (IgM) autoantibodies. Correlations with clinical disease progression were examined.Results: 3 of the 22 patients (14%) added sufficient criteria during follow up to satisfy a diagnosis of systemic lupus erythematosus (SLE) or to acquire a diagnosis of SLE renal disease. Patients who progressed were all females and were younger than those who did not progress (P=0.00054). IgG but not IgM autoreactivity showed greater increases in the progressor group than in the non-progressor group (P=0.047). IgG specificities that were higher at baseline in progressors included proliferating cell nuclear antigen (PCNA), beta 2 microglobulin, C1q and hemocyanin (P<0.019). Progressors had significant increases in La/SSB and liver cytosol type 1 (LC1) IgG autoantibodies over the period of evaluation (P≤0.0072). A quantitative risk profile generated from baseline demographic and autoantibody variables yielded highly different scores for the progressor and non-progressor groups (P=1.38 × 10 -7). Conclusions: In addition to demographic features, autoantibody profiles using an expanded array of specificities were correlated with the risk of progressive disease in patients with lupus. These findings suggest the feasibility of developing a simple diagnostic that could be applied by nonspecialists to screen for lupus and permit effective triage for specialty care.

AB - Introduction: Identification of patients who are in early stages of lupus is currently done through clinical evaluation and is not greatly facilitated by available diagnostic tests. Profiling for patient characteristics and antibody specificities that predict disease would enhance the ability of physicians to identify and treat early cases prior to onset of organ damaging illness.Methods: A group of 22 patients with 4 or fewer diagnostic criteria for lupus were studied for changes in clinical and autoantibody profiles after a mean follow up period of 2.4 years. An array with more than 80 autoantigens was used to profile immunoglobulin G (IgG) and immunoglobulin M (IgM) autoantibodies. Correlations with clinical disease progression were examined.Results: 3 of the 22 patients (14%) added sufficient criteria during follow up to satisfy a diagnosis of systemic lupus erythematosus (SLE) or to acquire a diagnosis of SLE renal disease. Patients who progressed were all females and were younger than those who did not progress (P=0.00054). IgG but not IgM autoreactivity showed greater increases in the progressor group than in the non-progressor group (P=0.047). IgG specificities that were higher at baseline in progressors included proliferating cell nuclear antigen (PCNA), beta 2 microglobulin, C1q and hemocyanin (P<0.019). Progressors had significant increases in La/SSB and liver cytosol type 1 (LC1) IgG autoantibodies over the period of evaluation (P≤0.0072). A quantitative risk profile generated from baseline demographic and autoantibody variables yielded highly different scores for the progressor and non-progressor groups (P=1.38 × 10 -7). Conclusions: In addition to demographic features, autoantibody profiles using an expanded array of specificities were correlated with the risk of progressive disease in patients with lupus. These findings suggest the feasibility of developing a simple diagnostic that could be applied by nonspecialists to screen for lupus and permit effective triage for specialty care.

UR - http://www.scopus.com/inward/record.url?scp=84864198971&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=84864198971&partnerID=8YFLogxK

U2 - 10.1186/ar3927

DO - 10.1186/ar3927

M3 - Article

C2 - 22838636

AN - SCOPUS:84864198971

SN - 1478-6354

VL - 14

JO - Arthritis Research and Therapy

JF - Arthritis Research and Therapy

IS - 4

M1 - R174

ER -

Autoantibody profiling to follow evolution of lupus syndromes

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this