Divergent Pro- and Antiinflammatory Roles for IL-23 and IL-12 in Joint Autoimmune Inflammation

doi:10.1084/jem.20030896

Published online 8 December 2003 doi:10.1084/jem.20030896

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© Rockefeller University Press, 0022-1007/2003/12/1951 $5.00
The Journal of Experimental Medicine, Volume 198, Number 12, 1951-1957

Brief Definitive Report

Divergent Pro- and Antiinflammatory Roles for IL-23 and IL-12 in Joint Autoimmune Inflammation

Craig A. Murphy¹, Claire L. Langrish¹, Yi Chen¹, Wendy Blumenschein², Terrill McClanahan², Robert A. Kastelein¹, Jonathon D. Sedgwick¹ and Daniel J. Cua¹

¹ Discovery Research, DNAX Research Inc., Palo Alto, CA 94304
² Experimental Pathology and Pharmacology, DNAX Research Inc., Palo Alto, CA 94304

Address correspondence to Daniel J. Cua, 901 California Ave., Palo Alto, CA 94304. Phone: (650) 496-1261; Fax: (650) 496-1200; email: daniel.cua{at}dnax.org; or Jonathon D. Sedgwick. Phone: (650) 496-1248; email: jonathon.sedgwick{at}dnax.org

Abstract

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Abstract
Introduction
Materials and Methods
Results and Discussion
References

Interleukin (IL) 23 is a heterodimeric cytokine composed ofa p19 subunit and the p40 subunit of IL-12. IL-23 affects memoryT cell and inflammatory macrophage function through engagementof a novel receptor (IL-23R) on these cells. Recent analysisof the contribution of IL-12 and IL-23 to central nervous systemautoimmune inflammation demonstrated that IL-23 rather thanIL-12 was the essential cytokine. Using gene-targeted mice lackingonly IL-12 (p35^-/-) or IL-23 (p19^-/-), we show that the specificabsence of IL-23 is protective, whereas loss of IL-12 exacerbatescollagen-induced arthritis. IL-23 gene-targeted mice did notdevelop clinical signs of disease and were completely resistantto the development of joint and bone pathology. Resistance correlatedwith an absence of IL-17–producing CD4⁺ T cells despitenormal induction of collagen-specific, interferon- ${gamma}$ –producingT helper 1 cells. In contrast, IL-12–deficient p35^-/-mice developed more IL-17–producing CD4⁺ T cells, as wellas elevated mRNA expression of proinflammatory tumor necrosisfactor, IL-1ß, IL-6, and IL-17 in affected tissuesof diseased mice. The data presented here indicate that IL-23is an essential promoter of end-stage joint autoimmune inflammation,whereas IL-12 paradoxically mediates protection from autoimmuneinflammation.

Key Words: rheumatoid arthritis • collagen-induced arthritis • IL-23 gene–deficient mice • IL-17 • IFN- ${gamma}$

Introduction

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Abstract
Introduction
Materials and Methods
Results and Discussion
References

IL-12 and IL-23 share a common p40 subunit, yet they compriseunique p35 and p19 subunits, respectively (1). Studies havedefined IL-12 as an important factor for the differentiationof naive T cells into IFN- ${gamma}$ –producing Th1 cells (2). Furthermore,gene-targeted mice, which specifically lack IL-12 signalingcapabilities through IL-12R-ß2 mutations (3) or deletionof the IL-12p35 gene (4), exhibit heightened susceptibilityto bacterial infections. This is probably due to poor IFN- ${gamma}$ productionin these mice, given the important role IFN- ${gamma}$ plays in antimicrobialimmunity (5). Thus, an important role for IL-12 in the generationof Th1 cell–mediated immunity has been well established.

The role for IFN- ${gamma}$ during induction of organ-specific autoimmunediseases is less clear (6–9), and the absolute requirementfor IL-12–mediated Th1 responsiveness in autoimmune inflammationhas been questioned in several recent papers (10–12).Collagen-induced arthritis (CIA), a rodent model of the humandisease rheumatoid arthritis, is induced by immunization withheterologous type II collagen (CII) emulsified in CFA (13).Development of CIA is dependent on both cell-mediated and humoralresponses (14) and is characterized by cellular infiltrationand synovitis of the joints, resulting in severe swelling ofthe paws and progressive destruction of bone and cartilage.Loss of IFN- ${gamma}$ signaling has been reported to increase severityof CIA (7, 8).

To determine the relative roles of IL-12 and IL-23 in the establishmentand maintenance of autoimmune inflammation, we have analyzedthe production of inflammatory cytokines and collagen-specificantibodies after the induction of CIA in p19^-/- (IL-23–deficient)mice, p35^-/- (IL-12–deficient) mice, and p40^-/- (IL-12–and IL-23–deficient) mice. Consistent with the dominantrole for IL-23 in central nervous system (CNS) autoimmune inflammation(12), IL-23–deficient mice were resistant to CIA. In contrast,IL-12–deficient mice showed enhanced joint swelling andjoint pathology, and, within affected joint tissue, increasedmRNA levels encoding for inflammatory mediators, such as IL-17and TNF. Absence of IL-12, alone (p35^-/-) or in combinationwith IL-23 (p40^-/- mice), also resulted in increased anticollagenantibody production, but decreased mRNA encoding for IFN- ${gamma}$ injoints of CIA-affected IL-12–deficient mice relative toarthritic WT mice, an outcome consistent with a key role forIL-12 in IFN- ${gamma}$ induction. An increased number of IL-17–producingCD4⁺ T cells was evident in cultured draining LN (DLN) cellsobtained from IL-12–deficient mice. Significantly, thesepotentially pathogenic T cells were absent in mice lacking IL-23.Thus, as in CNS inflammation (12), IL-23 is an essential mediatorof joint inflammation, with at least one of its activities beingto support production of IL-17–producing CD4⁺ T cells.In contrast, IL-12 is not critical for disease generation, butis the key factor in IFN- ${gamma}$ induction. IL-12 appears to regulatethe inflammatory process, possibly through the induction ofIFN- ${gamma}$ .

Materials and Methods

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Abstract
Introduction
Materials and Methods
Results and Discussion
References

Mice.
IL-12p35^-/-, IL-12p40^-/-, and WT control mice on the C57BL/6background were obtained from the Jackson Laboratory. IL-23p19^-/-mice and WT B6 x 129 F2 controls have been described previously(12). p19^-/- mice on the C57BL/6 background were used in intracellularcytokine detection experiments.

CIA.
CIA was induced in male and female C57BL/6 and B6 x 129 F2 miceaged 8–16 wk and clinically assessed as described previously(15). Mice were killed at day 42 after primary immunization;the rear paws were removed, fixed, decalcified in Cal-EX II(Fisher Scientific), and processed for paraffin embedding; andthe sections were cut and stained with hematoxylin and eosin.

T Cell Proliferation and Cytokine Production.
For T cell proliferation assay, cells were stimulated with 0–200µg/ml denatured chicken CII (boiled for 10 min) and culturedfor 72 h with [³H]thymidine addition during the final 18 h.For cytokine measurement, cells were stimulated with 100 µg/mldenatured CII for 72 h and supernatants were assayed for IFN- ${gamma}$ and IL-4 by ELISA (R&D Systems).

ELISA Detection of CII-specific Antibodies.
Mice were bled and serum was prepared for determination of serumCII-specific Ab levels by ELISA. Samples were added to CII-coated96-well plates (Chondrex Inc.) and incubated overnight. Horseradishperoxidase–conjugated goat anti–mouse Ig (H + L;total Ig), IgG₁, or IgG_2a were applied to determine the isotypeof CII-specific antibodies. The quantity of CII-specific Abdetected is expressed as OD₄₉₀ readings minus the relevant blank.

Gene Expression Analysis.
RNA was extracted from hind paws of mice, cDNA was prepared,and mRNA levels were quantitated as described previously (16).

DLN Cultures for Intracellular IL-17 and IFN- ${gamma}$ Detection.
DLNs were harvested from WT, p19^-/-, p35^-/-, and p40^-/- mice(all on C57BL/6 background). For intracellular staining, DLNcells were initially stimulated with 50 ng/ml PMA and 500 ng/mlionomycin (Sigma-Aldrich) in the presence of GolgiPlug^TM for3 h and stained with FITC-conjugated anti-CD4. Samples werewashed, fixed, permeabilized with Cytofix/Cytoperm^TM buffer,and stained with PE- or allophycocyanin-conjugated anti–IL-17and anti–IFN- ${gamma}$ . All antibodies and buffers unless otherwisestated were purchased from BD Biosciences.

Results and Discussion

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Abstract
Introduction
Materials and Methods
Results and Discussion
References

IL-23 Rather Than IL-12 Is Essential for Development of Joint Autoimmune Inflammation.
To study the differential functions of IL-12 and IL-23 in jointautoimmune inflammation, we compared susceptibility of micelacking only IL-23 (p19^-/-), only IL-12 (p35^-/-), or both cytokines(p40^-/-) to CIA. Overall incidence of disease was similar inWT C57BL/6 and B6 x 129 F2 mice (Fig. 1, A and B , $~$ 50%) asreported previously (17). In contrast, mice specifically lackingIL-23 (p19^-/-) and those animals lacking both IL-12 and IL-23(p40^-/-) were resistant to CIA induction (Fig. 1, A and B).Histological examination of joints revealed no pathology inp40^-/- (reference 18; not depicted) and p19^-/- mice (Fig. 1C). Unexpectedly, mice specifically lacking only IL-12 (p35^-/-)were highly susceptible to CIA with 80% of mice developing clinicalsigns of disease (Fig. 1, A and B). Histologically, diseasewas indistinguishable from that of similarly affected WT animals(Fig. 1 C). However, disease severity (Fig. 1 B) appeared tobe more intense in p35^-/- mice (median clinical score of micewith disease = 6; 12 out of 15 mice developed disease) comparedwith WT C57BL/6 mice (median clinical score of mice with disease= 4; 10 out of 18 mice developed disease). Disease recoverywas also delayed in mice lacking only IL-12 (Fig. 1 A). Thus,IL-23, but not IL-12, is necessary for the development of jointautoimmune inflammation, and the absence of IL-12 may resultin a more severe disease.

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Figure 1. IL-23, and not IL-12, is required for induction of CIA. (A) Cumulative incidence and the mean clinical score of mice that developed clinical disease are plotted against days after primary immunization with CII/CFA. (B) Disease incidence (number of diseased mice/total mice in group), disease severity (median maximum disease score attained and range of clinical scores), and mean day of onset of clinical disease are shown for mice of all genotypes. ^a, Only mice that developed clinical signs of disease were analyzed. N/A, not applicable. (C) Histopathology of decalcified paws at day 42 after primary CII immunization from WT, p35^-/-, and p19^-/- mice. Hematoxylin and eosin staining of tarsal joints from both WT and p35^-/- mice frequently showed severe pathology with articular cartilage erosion ( ${blacktriangleup}$ ), synovial inflammation (S), and pannus (P) formation. p19^-/- joints showed no pathology, characterized by smooth, intact articular cartilage ( ${triangleup}$ ) and no cellular infiltrate in the joint space (J). Original magnification, 100.

Reduced IFN- ${gamma}$ and Elevated CII-specific Antibodies in IL-12–deficient Mice.
CIA development is dependent on both T and B cell responses(14, 19), and the nature of the T cell response can have animportant impact in initiating CIA (20). T cell developmentwas first examined by CII-specific proliferation, and cytokineproduction in DLN cells was taken from mice 10 d after immunizationwith CII/CFA. WT C57BL/6, WT B6 x 129 F2, p19^-/-, p35^-/-, andp40^-/- mice had similar CII-specific proliferative responses,regardless of susceptibility to CIA (Fig. 2 A), indicatingthat induction of CII-reactive T cells did not depend on eitherIL-12 or IL-23. DLN cells from p19^-/- mice secreted WT levelsof IFN- ${gamma}$ , but undetectable levels of IL-4, in response to CIIstimulation, indicating that classical Th1 cells were inducedin these mice (Fig. 2 B). In contrast, DLN cells from p40^-/-mice exhibited a Th2 phenotype with low IFN- ${gamma}$ and high IL-4 levels.DLN cells from highly CIA susceptible p35^-/- mice produced lowlevels of IFN- ${gamma}$ (Fig. 2 B) in accordance with the known rolefor IL-12 in driving this cytokine (2, 21), yet did not produceIL-4, consistent with small amounts of IFN- ${gamma}$ seen in these cultures(Fig. 2 B). Our ongoing studies, as well as recent publishedwork (22), indicate that mouse IL-23 does not induce IFN- ${gamma}$ productionin T cells, but rather induces TNF and IL-17 (see the IL-23Promotes the Development...section).

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Figure 2. Type II collagen (CII)–specific T and B cell responses in IL-23– and IL-12–deficient mice. (A) Normal CII-specific T cell proliferation for both IL-23– and IL-12–deficient mice from DLN cells taken day 10 after CII/CFA immunization (n = 3–4/group) were cultured individually in triplicate. Data show the mean proliferative response of DLN cells for each genotype ± SEM. (B) DLN cells (day 10 after CII immunization) from individual mice were cultured and assayed as described in Materials and Methods. Data represent the mean response of 3–4 mice ± SEM. (C) Divergent humoral responses by p19^-/- mice versus p35^-/- and p40^-/- mice. Sera levels of CII-specific total Ig and IgG₁ at day 42 after primary CII immunization (n = 5/group) were determined by ELISA. Differences in Ig levels between relevant groups are indicated by p-values as determined by the unpaired Student's t test. Data represent the mean ± SEM.

p19^-/- mice generated a lower CII-specific antibody responsecompared with WT B6 x 129 F2 controls, suggesting that theirresistance to CIA may be due in part to impaired humoral responses(Fig. 2 C). Thus, even though p19^-/- mice have normal T cellresponse with normal capacity to produce IL-12 and IFN- ${gamma}$ (Fig. 2B; reference 12), their ability to elicit collagen-specificautoantibodies is impaired. By contrast, p35^-/- mice had increasedCII-specific total Ig and IgG₁ levels (Fig. 2 C) compared withWT C57BL/6 mice, suggesting that specific absence of IL-12 leadsto increased autoantibody production. At this stage, it is notknown whether this has a causative role in contributing to increaseddisease severity in p35^-/- mice. Low and comparable levels ofCII-specific IgG_2a were detected in WT C57BL/6, WT B6 x 129F2, p19^-/-, p35^-/-, and p40^-/- mice (unpublished data). p40^-/-mice also exhibited increased CII-specific total Ig and IgG₁,even though these mice were completely resistant to CIA. Thisresult is in contrast to others that have reported reduced CII-specificantibody responses in p40^-/- mice backcrossed onto the DBA/1background (18), and in anti–IL-12p40–treated DBA/1mice immunized to induce CIA (23). This may be due to differencesin mouse strains used in the studies. It has also been shownin several infectious disease models that p40^-/- mice on a C57BL/6background produce dramatically elevated levels of IgG₁ (24)and IgE (25). Overall, the results suggest that IL-12 may bean important regulator of autoantibody responses, especiallyof those isotypes commonly associated with a Th2 or allergicphenotype. Significantly, the presence of high CII-specificantibody levels in p40^-/- mice was not sufficient to inducearthritis in the absence of IL-23 and IL-12.

IL-23 Is Required for Induction of Joint Inflammatory Mediators, Including IL-17 and TNF.
To further analyze the means through which IL-23 deficiencymediates its protection in CIA, and in contrast, how the absenceof IL-12 results in more severe disease, we adopted a gene expressionstrategy. At day 42 after primary immunization with CII/CFA( $~$ 1 wk after peak of disease in WT mice), IFN- ${gamma}$ mRNA levels wereelevated above naive levels only in WT paws (Fig. 3 A) andin accordance with this, the IFN- ${gamma}$ –inducible chemokines,monokine induced by IFN- ${gamma}$ (Mig) and IFN- ${gamma}$ –inducible protein10 (IP-10; reference 26) were also elevated only in WT samples(Fig. 3 A). Notably, these factors were not elevated in p35^-/-samples. Also, although IL-23–deficient mice generatea normal antigen-specific Th1 response characterized by IFN- ${gamma}$ production by DLN cells (Fig. 2 B), this response does not developin the joints, as indicated by the absence of mRNA encodingboth IFN- ${gamma}$ and chemokines induced by IFN- ${gamma}$ (Fig. 3 A).

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Figure 3. Reduced IFN- ${gamma}$ , but elevated inflammatory cytokine and chemokine expression by p35^-/- mice. Cytokine and chemokine mRNA levels in hind paws day 42 after primary CII/CFA immunization were determined by quantitative real-time PCR and expressed in units relative to ubiquitin mRNA levels. (A) mRNA expression levels for IFN- ${gamma}$ and the IFN- ${gamma}$ –inducible chemokines IP-10 and Mig. (B) mRNA expression of genes encoding proinflammatory factors. RNA from 3 to 5 individual paw samples for each genotype were pooled for analysis, except for IFN- ${gamma}$ and IL-17, where the data represent the mean ± SEM; n = 3. The abundance of mRNA encoding IFN- ${gamma}$ and IL-17 were very low and, hence, were confirmed using expression data from individual mice. (Naive) Paws from unimmunized mice. WT samples, both inflamed and naive, consist of pooled RNA from both C57BL/6 and B6 x 129 F2 mice.

mRNA levels for the proinflammatory cytokines IL-1ß,IL-6, TNF, and IL-17, as well as a range of chemokines includingMIP-1ß (Fig. 3 B), MIP-1 ${alpha}$ , and MCP-6 (not depicted)remained elevated in WT and p35^-/- paws at day 42, but werenot elevated above unimmunized WT (naive) levels in p19^-/- andp40^-/- paws (Fig. 3 B). These factors, levels of IL-1ßand IL-6 in particular, were substantially higher in paws ofp35^-/- mice, which is indicative of the more chronic diseasein these animals relative to arthritic WT controls (Fig. 3 B).Nitric oxide synthase 2 gene expression, which is associatedwith activated macrophages (a major component of the synovialcellular infiltrate), was also elevated in p35^-/- mice relativeto arthritic WT animals (Fig. 3 B). These results suggest thatthe specific absence of IL-12, associated with reduced levelsof IFN- ${gamma}$ and increased expression of IL-1ß, IL-6, IL-17,TNF, and nitric oxide synthase 2, exacerbates autoimmune jointinflammation.

IL-23 Promotes the Development of IL-17–producing T Cells.
IL-17 is a potent proinflammatory cytokine produced by PBMCs/Tcells and by cells isolated from synovial fluid of rheumatoidarthritis patients (27). To determine whether there is a correlationbetween IL-23 and the development of IL-17–producing cells,we analyzed DLN cell cultures derived from mice inoculated s.c.with CFA (Fig. 4) . Ex vivo analysis of DLN cells from WT C57BL/6mice showed two relatively discrete populations of IFN- ${gamma}$ andIL-17–producing CD4⁺ T cells. In contrast, p19^-/- mice(C57BL/6 background) showed an absence of IL-17–producingCD4⁺ cells, as did p40^-/- mice, which also lack IL-23 (Fig. 4).Identical results were observed with p19^-/- versus WT miceon the B6 x 129 F2 background (unpublished data). IL-12–deficient(p35^-/-) mice showed elevated numbers of IL-17–producingT cells relative to WT controls. DLN cells from WT and p19^-/-mice both produced IFN- ${gamma}$ (Fig. 4), which is consistent with theirability to produce CII-specific IFN- ${gamma}$ (Fig. 2 B). Culture ofDLN cells for 5 d in the presence of IL-12 caused skewing ofCD4⁺ T cells toward IFN- ${gamma}$ production. Conversely, culture withIL-23 skewed toward IL-17 production, and this effect was especiallydramatic in p35^-/- and p40^-/- animals in which IFN- ${gamma}$ productionis minimal (Fig. 4). Preliminary studies indicate that IFN- ${gamma}$ neutralization in vitro enables outgrowth of IL-17–producingCD4⁺ T cells (unpublished data). These results indicate thatIL-23 promotes the development of IL-17–producing cells,whereas IL-12 drives IFN- ${gamma}$ production.

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Figure 4. IL-23 promotes the production of IL-17, which is regulated by the IL-12 pathway. Intracellular detection of IFN- ${gamma}$ and IL-17 protein by CD4⁺ T cells from DLN cells at day 10 after CFA immunization. Cells were either analyzed immediately after isolation (ex vivo) or after 5 d of culture in the presence of rIL-12 or rIL-23, both at 10 ng/ml. All plots are gated on live CD4⁺ T cells and are representative of four separate experiments.

We have shown previously that IL-23 is required for CNS autoimmunity(12), and here we show that IL-23 is also essential in jointautoimmune inflammation and, therefore, possibly other organ-specificautoimmune diseases. Thus, IL-23, but not IL-12, is necessaryfor disease development. Moreover, the absence of IL-12 resultsin more severe disease, reflected in elevated and prolongedexpression of proinflammatory cytokines such as IL-1ß,IL-6, IL-17, and TNF (Fig. 3 B). These results are in agreementwith other papers (10–12) demonstrating that mice selectivelylacking only IL-12 (p35^-/- mice) or IL-12Rß, the specificIL-12 signaling chain (28), exhibit increased severity of experimentalautoimmune encephalomyelitis compared with WT animals.

Together, these studies are consistent with the view that IL-12,on the one hand, is a key factor driving Th1 responses and IFN- ${gamma}$ production in the initial phases of an immune response; on theother hand, IL-12 may play a subsequent immunoregulatory rolein late-stage inflammation at a point when IL-23 strongly supportsthe inflammatory process (Fig. 5) . Interplay between IL-23and IL-17 production may be a critical immune pathway, potentiallyregulated via an IL-12–induced IFN- ${gamma}$ pathway (Figs. 4 and5; reference 22). Therefore, specific therapeutic blockade ofIL-23 (rather than IL-12 neutralization) may provide a preferredapproach for the treatment of a range of inflammatory autoimmunediseases.

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Figure 5. A model proposing the respective roles of IL-12/IFN- ${gamma}$ and IL-23 in T cell-priming events versus end-stage autoimmune inflammation. The precise mechanism through which IL-12/IFN- ${gamma}$ may down-regulate the magnitude of the inflammatory response (i.e., reducing IL-17 production) remains to be defined. It is recognized that IFN- ${gamma}$ may have dual roles during late-stage inflammation (i.e., antiinflammatory actions through termination of activated T cell responses [references 9, 29] while also stimulating macrophage function [reference 5]). ^a, The IL-23R is present on CD4⁺ CD45RB^lo "memory" T cells (30), but this cell phenotype may also include activated CD4⁺ T cells that are not strictly memory T cells.

	Acknowledgments

We thank C. Ollinger for histology assistance.

DNAX Research Inc. is supported by the Schering-Plough Corporation.

Submitted: June 4, 2003
Accepted: October 31, 2003

Footnotes

C.A. Murphy and C.L. Langrish contributed equally to this work.

References

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Introduction
Materials and Methods
Results and Discussion
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