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Current Immunology
Reviews
ISSN: 1573-3955
Current Immunology Reviews
Volume 3, Number 1, February 2007
Contents
Editorial Pp. 1
Regulation of Protective and Pathogenic Th17 Responses
Pp. 3-16
Gottfried Alber and Thomas Kamradt
[Abstract] [Full
text article]
Dendritic Cells: More Than Just Adaptive Immunity
Inducers? Pp. 17-22
Nathalie Jacobs, Jacques Boniver, Pascale Hubert and Philippe
Delvenne
[Abstract] [Full
text article]
Signal Transduction of the Aging Innate Immune System
Pp. 23-30
Christian R. Gomez, Vanessa Nomellini, Eric D. Boehmer
and Elizabeth J. Kovacs
[Abstract] [Full
text article]
Host-Cell Survival and Death During Chlamydia
Infection Pp. 31-40
Songmin Ying, Matthew Pettengill, David M. Ojcius and
Georg Häcker
[Abstract] [Full
text article]
Myeloma Cells and Their Interactions With the Bone
Marrow Endothelial Cells Pp. 41-55
Elke De Bruyne, Eline Menu, Els Van Valckenborgh, Hendrik
De Raeve, Ben Van Camp, Ivan Van Riet and Karin Vanderkerken
[Abstract] [Full
text article]
In Vitro Models of Human
T Cell Development: Dishing Out Progenitor T Cells
Pp. 57-75
Ross N. La Motte-Mohs, Génève Awong and
Juan Carlos Zúñiga Pflücker
[Abstract] [Full
text article]
Current Understanding of the Role of Dendritic Cells
and Their Co-Stimulatory Molecules in Generating Efficient
T Cell Responses in Lepromatous Leprosy Pp. 77-85
Dilvani O. Santos, Alice Miranda, Philip Suffys, Carlos
R. Rodrigues, Saulo C. Bourguignon and Helena C. Castro
[Abstract] [Full
text article]
Abstracts
[Back to top]
Editorial
We begin another year much as the last, but with continued
momentum. As we noted in last year’s comments, our goal
is to provide review articles that furnish new perspectives
to bridge the gap between basic immunology and clinical application.
Our particular focus is to arrange reviews covering specific
application of research in basic mechanisms to the understanding
of complex clinical diseases, and to highlight areas in which
studies in other biomedical topics have major significance
to basic and clinical immunology mechanisms. The article in
this first issue of our third year illustrates these goals
emphatically!
I will begin by highlighting two articles that start with
the cutting edge research in basic immune mechanisms and then
go all the way to bridging the gap toward direct application
to clinical medicine. The article by Alber and Kamradt on
the most recently described Th17 subset shows how new discoveries
in basic cellular immunology have direct application in elucidating
clinical disease mechanisms. Similarly, the article by La
Motte-Mohs, Awong and Zuniga-Pflucker shows the development
of a model of the most fundamental lymphocyte developmental
pathway – T lymphocyte differentiation – might
be exploited for the production of lymphocytes in vitro for
clinical applications.
Also in this issue are the articles that impart essential
mechanistic information on host response and disease pathogenesis.
Gomez et al. provide us with new information on how
the signal transduction mechanism changes become evident in
aging immune systems. Santos et al. give us some
interesting insights into how the different roles of dendritic
cells can have a profound impact on the nature of immune responses
in response to mycobacterium, and subsequent clinical disease.
Jacobs et al. also provide us with important information
on various mechanisms associated with dendritic cells in both
innate and adaptive immunity.
Finally, molecular mechanisms of pathogenesis are elucidated
in articles by De Bruyne et al., who summarizes some
important interactions between myeloma cells and stromal cells
in the bone marrow, and Ying et al., who presents
interesting details on how Chlamydia has been able
to override basic cell mechanisms in the regulation of cell
survival and death during infection.
Thus, our journal is in full stride, providing an important
forum for articles presenting critical information on molecular
mechanisms of pathogenesis in immune mediated diseases and
host response. We are grateful for the impressive contributions
from our authors, and we encourage continued support from
our readers and contributors.
David D. Lo
(Editor-in-Chief)
Division of Biomedical Sciences
University of California, Riverside
2146 Webber Hall
Riverside, CA 92521-0121
USA
E-mail: david.lo@ucr.edu
[Back to top]
Regulation of Protective and Pathogenic Th17 Responses
Gottfried Alber and Thomas Kamradt
[Full
text article]
The recent description of a T helper lymphocyte subset (Th17)
that is characterized by the production of IL 17, TNF α,
IL 6, IL 22, and GM-CSF has substantially influenced current
concepts of the pathogenesis of inflammatory diseases such
as arthritis or encephalitis. Contrasting with the prevailing
dogma that held IFN γ
producing Th1 cells responsible for the pathogenesis of most
organ-specific autoimmune diseases it had been noted for some
time that IFN γ-/-
mice were more susceptible to arthritis and encephalitis than
their wild-type, littermates and that IL 12 was dispensable
for disease induction. Recently it has become clear, that
Th17 cells are of central importance for the pathogenesis
of inflammatory diseases. The differentiation of naive Th
cells into Th17 is triggered by antigen recognition in the
presence of both IL 6 and TGF β.
IL 23, a heterodimeric cytokine which shares the p40 chain
with IL 12 is an important survival factor for Th17 whereas
IL 27, another member of the IL 12 family strongly inhibits
Th17 production. Here we review the protective and pathogenic
functions of Th17 in host defense and inflammatory diseases.
[Back to top]
Dendritic Cells: More Than Just Adaptive Immunity
Inducers?
Nathalie Jacobs, Jacques Boniver, Pascale Hubert and Philippe
Delvenne
[Full
text article]
Dendritic cells (DC) are well known for their capacity to
induce immune responses and there is also accumulating evidence
of their ability to interact with various cell types of the
innate system, such as NK, NKT or TCRγδ
cells. These interactions are bi-directional, mediated by
soluble or cell surface molecules and have been mainly described
in the context of immune responses to infectious agents and
tumors.
NK, NKT or TCRγδ
cells induce the maturation of DC, as shown by the increased
expression of CD86, IL12 production and priming of T cell
responses. On the other hand, mature DC have the ability to
activate NK, NKT or TCRγδ
cells for sustained innate immune responses and activated
NK cells may kill immature DC. In addition, DC and NK or TCRγδ
cells share similar functions such as cytotoxic and antitumor
activity, interferon production and antigen presentation capacity.
[Back to top]
Signal Transduction of the Aging Innate Immune System
Christian R. Gomez, Vanessa Nomellini, Eric D. Boehmer
and Elizabeth J. Kovacs
[Full
text article]
Aging is associated with defects in the cells of the innate
immune system, in both their function and number. During the
last decade, new evidence has revealed impairment in the early
stages of the activation processes that trigger innate immune
cells. In this review, the impact of aging on signal transduction
in macrophages (MΦs),
as pivotal representatives of innate immunity, is presented.
Emphasis is put on the classical intracellular pathways of
MΦ
activation in response to lipopolysaccharide (LPS) and interferon-gamma
(IFN-γ).
The critical analysis of the literature reveals that, when
intracellular signaling defects occur, the ability of MΦs
to respond appropriately is significantly compromised. Taken
together, these observations may help explain why aged individuals
have inflammatory and immune defects that range from decreased
capacity to fight infections to delayed healing of dermal
wounds. Gaining an understanding of the nature of the defects
in innate immune cells, such as MΦs,
may shed light on the development of therapeutic strategies
aimed at restoring innate immune function in aged individuals
so they can better combat infectious challenges.
[Back to top]
Host-Cell Survival and Death During Chlamydia
Infection
Songmin Ying, Matthew Pettengill, David M. Ojcius and
Georg Häcker
[Full
text article]
Different Chlamydia trachomatis strains are responsible
for prevalent bacterial sexually-transmitted disease and represent
the leading cause of preventable blindness worldwide. Factors
that predispose individuals to disease and mechanisms by which
chlamydiae cause inflammation and tissue damage remain unclear.
Results from recent studies indicate that prolonged survival
and subsequent death of infected cells and their effect on
immune effector cells during chlamydial infection may be important
in determining the outcome. Survival of infected cells is
favored at early times of infection through inhibition of
the mitochondrial pathway of apoptosis. Death at later times
displays features of both apoptosis and necrosis, but pro-apoptotic
caspases are not involved. Most studies on chlamydial modulation
of host-cell death until now have been performed in cell lines.
The consequences for pathogenesis and the immune response
will require animal models of chlamydial infection, preferably
mice with targeted deletions of genes that play a role in
cell survival and death.
[Back to top]
Myeloma Cells and Their Interactions With the Bone
Marrow Endothelial Cells
Elke De Bruyne, Eline Menu, Els Van Valckenborgh, Hendrik
De Raeve, Ben Van Camp, Ivan Van Riet and Karin Vanderkerken
[Full
text article]
Multiple myeloma (MM) is an incurable plasma cell malignancy
characterized by a monoclonal proliferation of plasma cells
in the bone marrow (BM), secretion of paraprotein in serum,
development of osteolytic bone lesions and angiogenesis in
the BM. In the BM, MM cells receive signals to survive and
proliferate due to the existence of functional, mutual interactions
between the MM cells and the BM stromal cells. This stroma
not only offers protection against apoptosis and leads to
growth stimulation, but also has a role in the clinical very
relevant drug resistance. As such, it became clear that the
BM stroma can also become a therapeutical target in addition
to the MM cells. In the past, the BM fibroblasts were considered
to be the main stromal cells that interact with the MM cells.
However, since the observation of a myeloma associated angiogenesis
in patients and in the 5TMM mouse model, it became clear that
the endothelial cells (EC) are also an important participant
of the BM stromal cells. BMEC are involved in the specific
homing of MM cells and are a source of paracrine growth factors.
In this review, the interaction between BMEC and MM cells
will be discussed.
[Back to top]
In Vitro Models of Human
T Cell Development: Dishing Out Progenitor T Cells
Ross N. La Motte-Mohs, Génève Awong and
Juan Carlos Zúñiga Pflücker
[Full
text article]
T cells develop within the unique microenvironment provided
by the thymus. T cell differentiation involves a series of
commitment events and developmental checkpoints including
T cell receptor (TCR) gene recombination and positive/negative
selection of developing thymocytes to yield functionally mature
T cells. These events occur in a sequential, temporal and
spatial fashion, as developing thymocytes migrate through
the thymus. In vitro studies to yield insights into
human T cell development have classically employed the fetal
thymic organ culture (FTOC) model system. This approach relies
on the seeding of human hematopoietic stem cells (HSCs) and/or
their progeny into host thymic lobes or thymic fragments,
typically of mouse origin. Recently, a novel in vitro
approach that makes use of the OP9 bone marrow stromal cell
line expressing the Notch receptor ligand Delta-like-1 (OP9-DL1)
effectively supported the generation of large numbers of human
progenitor T cells from HSCs. In this review, we outline several
in vitro systems employed for the generation and
study of human T cells. Particular emphasis is dedicated to
the OP9-DL1 coculture system. Finally, given the number of
progenitor T cells that can be generated in vitro,
we discuss the potential implications for the treatment of
immune-related diseases such as cancer, immunedeficiency,
and autoimmunity.
[Back to top]
Current Understanding of the Role of Dendritic Cells
and Their Co-Stimulatory Molecules in Generating Efficient
T Cell Responses in Lepromatous Leprosy
Dilvani O. Santos, Alice Miranda, Philip Suffys, Carlos
R. Rodrigues, Saulo C. Bourguignon and Helena C. Castro
[Full
text article]
Leprosy is a chronic infectious disease caused by Mycobacterium
leprae that needs continued vigilance, particularly for
detection and treatment of hidden and undiagnosed cases. Cell-mediated
immunity in leprosy has been identified as a key mechanism
for the understanding of this disease. The dendritic cell
(DC) is the most potent professional antigen-presenting cell
and recently has been the focus of much interest as the main
initiator of naive T-cell responses to several antigens. For
rational use of DCs in adjuvant therapy of lepromatous leprosy,
the patterns of synthesis and secretion of cytokines by DCs
during some mycobacterial infections must be better understood.
Therefore, the aim of this review is to illustrate some of
the cellular events involved in the immune recognition of
the antigens during leprosy and the role of antigen-presenting
cell (DC) and their co-stimulatory molecules, such as DC-SIGN,
CD-40, B7-1 and B7-2, in generating efficient T-cell responses.
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