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Series GSE23076

Query DataSets for GSE23076

Status

Public on Jul 23, 2010

Title

Gene Expression Profiles in a Rabbit Model of Systemic Lupus Erythematosus

Platform organism

Sample organisms

Homo sapiens; Oryctolagus cuniculus

Experiment type

Expression profiling by array

Summary

We previously reported the establishment of a rabbit (Oryctolagus cuniculus) model of Systemic Lupus Erythematosus (SLE) in which peptide immunization led to lupus-like autoantibody production including anti-Sm, -RNP, -SS-A, -SS-B and -dsDNA. Some neurological symptoms in form of seizures and nystagmus were observed. The animals used in the previous and in the present study were from a National Institute of Allergy and Infectious Diseases colony of rabbits that were pedigreed, immunoglobulin allotype-defined but not inbred. Their genetic heterogeneity may correspond to that found among patients of a given ethnicity. We extended the information about this rabbit model of SLE by microarray based expression profiling. We first demonstrated that human expression arrays could be used with rabbit RNA to yield information on molecular pathways. We then designed a study evaluating gene expression profiles in 8 groups of control and SLE rabbits (46 rabbits in total). Genes significantly upregulated in SLE rabbits were associated with NK cytotoxicity, antigen presentation, leukocyte migration, cytokine activity, protein kinases, RNA spliceosomal ribonucleoproteins, intracellular signaling cascades, and glutamate receptor activity. These results link increased immune activation with up-regulation of components associated with neurological and anti-RNP responses, demonstrating the utility of the rabbit SLE model to uncover biological pathways related to SLE-induced clinical symptoms, including Neuropsychiatric Lupus. Our finding of distinct gene expression patterns in rabbits that made anti-dsDNA compared to those that only made other anti-nuclear antibodies should be further investigated in subsets of SLE patients with different autoantibody profiles.

Overall design

An important goal of biomedical research is to translate basic findings into clinical applications. Models in inbred mice that spontaneously develop SLE, along with various mutant, transgenic and knockout models have documented a variety of genetic defects leading to SLE, but from the clinical perspective, the degree to which these findings using the inbred or homogeneous artificially mutated strains apply to individuals in heterogeneous outbred human populations is open to question. Given that there is still no cure available for SLE, it is important that we continue to explore possibilities using new animal models of SLE including neuropsychiatric lupus (NPSLE). The gene expression study reported here was conducted to expand our understanding of SLE and in particular NPSLE using our rabbit model. We reported earlier that immunization of rabbits with the SM- or GR-MAP peptides led to development of anti-nuclear autoantibodies, including anti-dsDNA, as well as neurological symptoms in the form of seizures and nystagmus in some rabbits. After establishing that it was possible to use the Affymetrix U95 human microarray for the rabbit gene expression studies, through comparative hybridization of identically prepared cRNA from human and rabbit PWBC, the human microarray was used due to lack of rabbit-specific microarrays. We describe unique gene expression changes associated with lupus like serological patterns in immunized rabbits. Our results also demonstrate that caution must be applied when choosing the structure of the carrier Multiple Antigen Peptide (MAP-peptide) for immunization. We discovered that using MAP-4 rather than MAP-8 significantly altered patterns of immune response and gene expression. Currently, microarrays specific for study of gene expression profiles are not available for rabbits. Therefore, we first conducted studies that compared identically prepared rabbit and human cRNA binding to the Affymetrix U95 microarray available for human gene expression analyses. It was determined that the human microarray could be used with rabbit cRNA to yield information on genetic pathways activated and/or suppressed in autoantibody-producing immunized rabbits. In the current report, gene expression profiles of a total of 46 rabbits, from 4 generations within a pedigreed group of control and immunized rabbits, were obtained and analyzed.

Contributor(s)

Rai G, Ray S, Milton J, Yang J, Ren P, Lempicki RA, Mage RG

Citation(s)

Submission date

Jul 22, 2010

Last update date

Dec 13, 2018

Contact name

Richard A Lempicki

E-mail(s)

rlempicki@mail.nih.gov

Phone

301-846-5093

Organization name

Leidos Biomedical Research, Inc.

Department

Clinical Services Program

Lab

Laboratory of Immunopathogenesis and Bioinformatics

Street address

PO Box B

City

Frederick

State/province

MD

ZIP/Postal code

21702

Country

USA

Platforms (1)

[HG_U95Av2] Affymetrix Human Genome U95 Version 2 Array

Samples (66)

More...

GSM569007	Human_PBMC_NA_NA_Repl_1
GSM569008	Human_PBMC_NA_NA_Repl_2
GSM569009	Human_PBMC_NA_NA_Repl_3

GSM569010	Human_PBMC_NA_NA_Repl_4
GSM569011	Human_PBMC_NA_NA_Repl_5
GSM569012	Human_PBMC_NA_NA_Repl_6
GSM569013	Human_PBMC_NA_NA_Repl_7
GSM569014	Human_PBMC_NA_NA_Repl_8
GSM569015	Human_PBMC_NA_NA_Repl_9
GSM569016	Rabbit_WB_MAP4_GR_Repl_1
GSM569017	Rabbit_WB_MAP4_GR_Repl_2
GSM569018	Rabbit_WB_MAP4_GR_Repl_3
GSM569019	Rabbit_WB_MAP4_GR_Repl_4
GSM569020	Rabbit_WB_MAP4_None_Repl_1
GSM569021	Rabbit_WB_MAP4_None_Repl_2
GSM569022	Rabbit_WB_MAP4_None_Repl_3
GSM569023	Rabbit_WB_MAP4_None_Repl_4
GSM569024	Rabbit_WB_MAP4_SM_Repl_1
GSM569025	Rabbit_WB_MAP4_SM_Repl_2
GSM569026	Rabbit_WB_MAP4_SM_Repl_3
GSM569027	Rabbit_WB_MAP4_SM_Repl_4
GSM569028	Rabbit_WB_MAP4_SM_Repl_5
GSM569029	Rabbit_WB_MAP8_GR_Repl_1
GSM569030	Rabbit_WB_MAP8_GR_Repl_2
GSM569031	Rabbit_WB_MAP8_GR_Repl_3
GSM569032	Rabbit_WB_MAP8_GR_Repl_4
GSM569033	Rabbit_WB_MAP8_GR_Repl_5
GSM569034	Rabbit_WB_MAP8_GR_Repl_6
GSM569035	Rabbit_WB_MAP8_GR_Repl_7
GSM569036	Rabbit_WB_MAP8_GR_Repl_8
GSM569037	Rabbit_WB_MAP8_GR_Repl_9
GSM569038	Rabbit_WB_MAP8_GR_Repl_10
GSM569039	Rabbit_WB_MAP8_GR_Repl_11
GSM569040	Rabbit_WB_MAP8_GR_Repl_12
GSM569041	Rabbit_WB_MAP8_GR_Repl_13
GSM569042	Rabbit_WB_MAP8_None_Repl_1
GSM569043	Rabbit_WB_MAP8_None_Repl_2
GSM569044	Rabbit_WB_MAP8_None_Repl_3
GSM569045	Rabbit_WB_MAP8_None_Repl_4
GSM569046	Rabbit_WB_MAP8_None_Repl_5
GSM569047	Rabbit_WB_MAP8_PBS_Repl_1
GSM569048	Rabbit_WB_MAP8_PBS_Repl_2
GSM569049	Rabbit_WB_MAP8_PBS_Repl_3
GSM569050	Rabbit_WB_MAP8_SM_Repl_1
GSM569051	Rabbit_WB_MAP8_SM_Repl_2
GSM569052	Rabbit_WB_MAP8_SM_Repl_3
GSM569053	Rabbit_WB_MAP8_SM_Repl_4
GSM569054	Rabbit_WB_MAP8_SM_Repl_5
GSM569055	Rabbit_WB_MAP8_SM_Repl_6
GSM569056	Rabbit_WB_MAP8_SM_Repl_7
GSM569057	Rabbit_WB_MAP8_SM_Repl_8
GSM569058	Rabbit_WB_MAP8_SM_Repl_9
GSM569059	Rabbit_WB_None_None_Repl_1
GSM569060	Rabbit_WB_None_None_Repl_2
GSM569061	Rabbit_WB_None_None_Repl_3
GSM569062	Rabbit_WB_None_None_Repl_4
GSM569063	Rabbit_WB_None_None_Repl_5
GSM569064	Rabbit_WB_None_None_Repl_6
GSM569065	Rabbit_WB_None_None_Repl_7
GSM569066	Rabbit_WB_None_None_Repl_8
GSM569067	Rabbit_WB_None_None_Repl_9
GSM569068	Rabbit_WB_None_None_Repl_10
GSM569069	Rabbit_WB_None_None_Repl_11
GSM569070	Rabbit_WB_None_None_Repl_12
GSM569071	Rabbit_WB_None_None_Repl_13
GSM569072	Rabbit_WB_None_None_Repl_14

Relations

BioProject

Download family	Format
SOFT formatted family file(s)	SOFT
MINiML formatted family file(s)	MINiML
Series Matrix File(s)	TXT

Supplementary file	Size	Download	File type/resource
GSE23076_RAW.tar	178.6 Mb	(http)(custom)	TAR (of CEL)
Processed data included within Sample table

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