100% satisfaction guarantee Immediately available after payment Both online and in PDF No strings attached
logo-home
The Th17 lineage: Answers to some immunological questions $13.49   Add to cart

Exam (elaborations)

The Th17 lineage: Answers to some immunological questions

 8 views  0 purchase
  • Course
  • Th17 lineage
  • Institution
  • Th17 Lineage

CLUES TO THE IDENTIFICATION OF A NEW T HELPER CELL LINEAGE PRODUCING IL-17 The first suggestion of a new T helper subset, distinct from Th1 and Th2, was provided by the finding of T CD4+ cells producing high levels of IL-17 without expression of IFN-γ or IL-4, the respective prototype cytokin...

[Show more]

Preview 2 out of 14  pages

  • August 6, 2024
  • 14
  • 2024/2025
  • Exam (elaborations)
  • Questions & answers
  • Th17 lineage
  • Th17 lineage
avatar-seller
TIFFACADEMICS
Revisión
Inmunología
Vol. 28 / Núm 1/ Enero-Marzo 2009: 32-45



The Th17 lineage:
Answers to some immunological questions
Coral González-García, Francisco M. Martín-Saavedra, Alicia Ballester, Sara Ballester
Unidad de Regulación Génica, Centro Nacional de Microbiología, Instituto de Salud Carlos III, Majadahonda, Madrid.

EL LINAJE TH17: RESPUESTAS A ALGUNAS CUESTIONES INMUNOLÓGICAS
Recibido: 1 Diciembre 2008
Aceptado: 26 Enero 2009




RESUMEN ABSTRACT
En los últimos años se han estudiado exhaustivamente las funciones y In recent years the function and developmental pathway for the T
las rutas de desarrollo del subtipo de células T helper especializado en la pro- helper subset specialized in IL-17 production (Th17) have been exhausti-
ducción de IL-17 (Th17). Este linaje celular de células efectoras desempeña vely studied. This lineage of effector cells plays a decisive role in the immu-
un papel decisivo tanto en la respuesta inmune a agentes infecciosos, como ne response to infectious agents, as well as in immunopathologies. Simi-
en inmunopatologías. Al igual que para los subtipos Th1 y Th2, la definición lar to the Th1 and Th2 subsets, the Th17 definition is orchestrated by spe-
de Th17 está dirigida por citocinas y factores de transcripción específicos. La cific cytokines and transcription factors. A combination of TGF-β plus IL-
combinación de TGF-β e IL-6, y los factores de transcripción RORγt, RORα 6, and the transcription factors RORγt, RORα and Stat3 are essential for
y Stat3 son esenciales para comprometer el subtipo Th17. IL-23 juega un papel Th17 commitment. IL-23 plays a key role in the stabilization of the phe-
clave en la estabilización del fenotipo y de la actividad patogénica de células notype and in the promotion of the pathogenic activity of IL-17-producer
productoras de IL-17. La citocina IL-21 producida por células Th17 participa cells. The IL-21 cytokine produced by Th17 cells participates in a feedback
en un mecanismo de retroalimentación para favorecer el desarrollo de célu- mechanism to favour this phenotype, while IL-27, IL-4, IFN-γ, IL-25 and
las productoras de IL-17, mientras que las citocinas IL-27, IL-4, IFN-γ, IL-25 IL-2 cytokines limit the Th17 response. CD4+CD25+Foxp3+ regulator cells
e IL-2 limitan el fenotipo Th17. Las células T reguladoras CD4+CD25+Foxp3+ (Treg) follow a development pathway divergent to Th17 establishment,
(Treg) siguen una ruta de desarrollo divergente al establecimiento de las célu- although both alternatives are governed by TGF-β that directs the fate
las IL-17, aunque ambas alternativas son gobernadas por TGF-β, el cual diri- of naïve CD4+ cells to each of these mutually exclusive T cell subsets depen-
ge el destino de células CD4+ naïve hacia uno u otro de estos subtipos celu- ding on the presence of IL-6. Furthermore, recent data indicate that pre-
lares mutuamente excluyentes dependiendo de la presencia de IL-6. Ade- established Treg cells can switch its genetic program to become IL-17-pro-
más, datos recientes indican que células Treg ya establecidas pueden modi- ducer cells. In this review we summarize and discuss the current availa-
ficar su programa genético para convertirse en células Th17. En esta revisión ble data about the biology of Th17 cells.
se resumen y analizan los datos disponibles actualmente acerca de la biolo-
gía de las células Th17. KEY WORDS: Th17 / TGF-β / IL-6 / IL-23 / RORγt.

PALABRAS CLAVE: Th17 / TGF-β / IL-6 / IL-23 / RORγt.




32

, INMUNOLOGÍA CORAL GONZÁLEZ-GARCÍA, FRANCISCO M. MARTÍN-SAAVEDRA, ALICIA BALLESTER AND SARA BALLESTER




THE IL-17 FAMILY TRAF6 was shown to be involved in the activation of NFκB
Since Mossman et al. proposed the model wherein CD4+ by IL-17(17). On the other hand, IL-17 can increase expression
T helper cells were classified in Th1 and Th2 subtypes with of some of its target genes through mRNA stabilization(18).
different functions in immune responses according to the IL-17B and IL-17C are members of the family whose
profile of cytokines produced(1), the Th1/Th2 paradigm cellular sources are unknown yet, and whose biology seems
provided a valuable tool to understand the interplay of unrelated to IL-17A. In this review, we will refer to IL-17A
innate and adaptive immunity and CD4+ T cell function. as IL-17.
However, some discrepancies have arisen related to results
that did not fit in the Th1/Th2 hypothesis. During the
past years new studies have identified a distinct subset of CLUES TO THE IDENTIFICATION OF A NEW T
CD4+ T cells that secrete IL-17 and the closely related cytokine HELPER CELL LINEAGE PRODUCING IL-17
IL-17F as well as other inflammatory cytokines such as IL- The first suggestion of a new T helper subset, distinct
6 and IL-22(2,3). from Th1 and Th2, was provided by the finding of T CD4+
Murine IL-17 was described as CTLA-8(4), and a 63% cells producing high levels of IL-17 without expression of
homologous human cytokine was soon found(5). Currently, IFN-γ or IL-4, the respective prototype cytokines produced
the IL-17 cytokines include a family of six members (IL-17A- by Th1 and Th2(19). Other important clues were supplied
F), with at least two of them having potent proinflammatory by studies on animal models of autoimmunity. Pathologies
properties: IL-17A or CTLA-8 (the founder member of the such as experimental autoimmune encephalomyelitis (EAE)
family also named IL-17), and IL17-F. Both are produced and collagen-induced arthritis (CIA), or mouse models
by the recently described Th17 cell subset, are localized at for human multiple sclerosis (MS) and rheumatoid arthritis
the same chromosomal locus (1A4), share a 55% of homology (RA), have been traditionally considered as Th1-mediated
at the protein level, and seem to have similar functions. IL- diseases. However, over the years, a number of experimental
17A and IL-17F work mostly as homodimers, but IL-17A/F results showed inconsistencies with the Th1/Th2 hypothesis.
heterodimers have been recently described in several For example, depletion of the Th1 cytokine IFN-γ, its
independent reports(6-8), suggesting a role in inflammatory receptor IFN-γR, or the IL-12 receptor (IL-12Rβ2), the master
response regulation for such IL-17 complexes. IL-17D and inductor of the Th1 phenotype, increased the susceptibility
IL-17E (alternative names: IL-27 and IL-25) are the two to EAE(20-26).
members of the IL-17 family with lowest homology (16% With the discovery of IL-23 as an heterodimeric cytokine
at protein level) to IL-17A. None of them is produced by sharing its p40 subunit with IL-12(27), the relative contribution
Th17 cells, and both of them, as discussed later, exert a of IL-12 and IL-23 to chronic inflammation could be analyzed.
negative control on the Th17 subset development. The IL-12 heterodimer is composed by the p40 and p35
IL-17 receptors are a family of five members of membrane subunits, while IL-23 comprises p40 and a different p19
proteins, IL-17RA-F(9). Except for IL-17RA, each of these protein. By using mice lacking IL-23 (p19-/-), IL-12 (p35-/-) or
receptors has alternative splicing variants, and, for IL-17RB both cytokines (p40-/-), it could be demonstrated that IL-23,
and IL-17RC, result in secreted soluble proteins which could and not IL-12, is the critical cytokine for autoimmune
serve to antagonize their ligands(10). IL-17A and IL-17F bind inflammation of the central nervous system (CNS) during
to IL-17RA, although IL-17A binds with much higher EAE(28). This study was followed by many other showing
affinity(11), which correlates with its greater potency in the role of IL-23 in inflammation(29-31). In parallel with these
functions like induction of chemokine expression(8). In findings, it was reported that IL-17-producer cells could be
addition to IL-17RA, IL-17F can also bind to IL-17RC. By generated independently of the cytokines and transcription
signalling through IL-17RA, which is ubiquitously expressed, factors required for Th1 or Th2 differentiation. The development
IL-17 can induce the production of different kinds of proteins, of Th17 from naïve cells was potently inhibited by IFN-γ and
many of them related to inflammation, including chemokines IL-4, whereas memory Th17 cells were resistant to suppression
(CXCL-1, CXCL-2, CXCL-8-10, CCL-2, CCL-20), cytokines by Th1 or Th2 cytokines, indicating that these cells had a
(IL-6, TNFα, G-CSF, GM-CSF), proteins of the acute phase permanent commitment. All these data together indicated
response, tissue remodelling factors (MMP1, MMP3, MMP9, that a T helper lineage distinct from Th1 and Th2 can
MMP13, TIMP2), and anti-microbial products (β-defensins, differentiate from naïve CD4+ cells to produce IL-17(2, 3).
mucins, calgranulins)(12). The signal transduction of IL-17 is In 2006, three independent reports provided the basis
mainly mediated by NFκB and C/EBP transcription factors, for understanding the process of Th17 cell promotion(32-34).
with the involvement of MAP kinase pathways(13-16). Moreover, All of them found that transforming growth factor β (TGF-



33

The benefits of buying summaries with Stuvia:

Guaranteed quality through customer reviews

Guaranteed quality through customer reviews

Stuvia customers have reviewed more than 700,000 summaries. This how you know that you are buying the best documents.

Quick and easy check-out

Quick and easy check-out

You can quickly pay through credit card or Stuvia-credit for the summaries. There is no membership needed.

Focus on what matters

Focus on what matters

Your fellow students write the study notes themselves, which is why the documents are always reliable and up-to-date. This ensures you quickly get to the core!

Frequently asked questions

What do I get when I buy this document?

You get a PDF, available immediately after your purchase. The purchased document is accessible anytime, anywhere and indefinitely through your profile.

Satisfaction guarantee: how does it work?

Our satisfaction guarantee ensures that you always find a study document that suits you well. You fill out a form, and our customer service team takes care of the rest.

Who am I buying these notes from?

Stuvia is a marketplace, so you are not buying this document from us, but from seller TIFFACADEMICS. Stuvia facilitates payment to the seller.

Will I be stuck with a subscription?

No, you only buy these notes for $13.49. You're not tied to anything after your purchase.

Can Stuvia be trusted?

4.6 stars on Google & Trustpilot (+1000 reviews)

75323 documents were sold in the last 30 days

Founded in 2010, the go-to place to buy study notes for 14 years now

Start selling
$13.49
  • (0)
  Add to cart