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Current
Rheumatology Reviews
ISSN: 1573-3971
Current Rheumatology Reviews
Volume 1, Number 3, November 2005
Contents
Lipid Peroxidation End-Products as Modulators of
Catabolic and Inflammatory Responses in Arthritis: A Review
Pp.205
Barbara Morquette, Qin Shi, Patrick Lavigne,Julio C. Fernandes
and Mohamed Benderdour
[Abstract]
Update on the Molecular Genetic Studies of Behcet’s
Disease Pp.213
Hyun Kyu Chang
[Abstract]
HLA-B27 and B27-Subtypes in the Pathogenesis of Ankylosing
Spondylitis Pp.223
T.E.W. Feltkamp
[Abstract]
A Common Cause of Anemia in Inflammatory Disorders:
Anemia of Chronic Disease Pp.227
Cengiz Beyan and Esin Beyan
[Abstract]
Fibromyalgia Pp.231
Dina Dadabhoy and Daniel J. Clauw
[Abstract]
The Role of Ultrasonography of Peripheral Entheses
in the Diagnosis and Assessment of Spondyloarthropathies Pp.243
Paolo Falsetti, Bruno Frediani, Caterina Acciai, Georgios
Filippou, Mauro Galeazzi and Roberto Marcolongo
[Abstract]
MR-Based In Vivo Analysis of Joint Biomechanics
and its Relevance in the Pathogenesis of Osteoarthritis Pp.255
Heiko Graichen, Rüdiger von Eisenhart-Rothe, Steafan
Hinterwimmerand Felix Eckstein
[Abstract]
Autoantibodies in Systemic Lupus: Quite a Lot or Just
a Few? Pp.277
Paola Migliorini, Consuelo Anzilotti, Laura Caponi, Federico
Pratesiand Valeria Rocchi
[Abstract]
Etiologic Aspects of Paget’s Disease of Bone
Pp.283
Domenico Rendina, Gianpaolo De Filippo and Giuseppe Mossetti
[Abstract]
Intravenous Immunoglobulin (IVIG) in Rheumatologic
Diseases: A Review of its Mechanism of Action Pp.289
Martin N. Lee and Lavjay Butani
[Abstract]
Can 5-HT3 Receptor Antagonists Replace
Anesthetics and
Corticosteroids in the Local Treatment of Rheumatic Processes?
Pp.295
Thomas Stratz and Wolfgang Müller
[Abstract]
Abstracts
[Back to top]
Lipid Peroxidation End-Products as Modulators
of Catabolic and Inflammatory Responses in Arthritis: A Review
Barbara Morquette, Qin Shi, Patrick Lavigne, Julio C.
Fernandes and Mohamed Benderdour
Lipid peroxidation (LPO) is a free radical-related process
occurring in biologic systems under enzymatic or nonenzymatic
control, e.g. for the generation of lipid-derived aldehydes.
There is increasing evidence that these aldehydes are causally
involved in the pathogenesis of numerous diseases including
diabetes, heart failure, atherosclerosis, and neurodegenerative
process.
4-hydroxynonenal (HNE) is the most important aldehyde involved
in oxidant injury. Classically, HNE was described for a long
time as a marker of extensive oxidative stress in various
tissues. Recent studies, however, showed that HNE can modulate
cellular metabolism, inflammatory responses, as well as apoptosis
via its effects on signaling/transcription regulation
and protein modification. Interestingly, these pathological
processes are all implicated to various degrees in arthritis,
but no study has specifically reported the potential role
of these aldehydes in rheumatic diseases. Therefore, this
review focuses on the relevance of oxidative stress-induced
HNE production to the pathophysiology of arthritis at inflammatory
and catabolic levels.
[Back to top]
Update on the Molecular Genetic Studies of Behcet’s
Disease
Hyun Kyu Chang
Although the pathogenesis of Behcet’s disease (BD)
is not fully elucidated, a genetic susceptibility to the disease
appears to be affected by a polygenic inheritance, including
the major histocompatibility complex (MHC) and non-MHC genes.
As is true for the well-known regional differences in the
disease expression of BD, a genetic susceptibility to BD appears
to be different in various ethnic groups. Although HLA-B51
is a genetic factor with the strongest association in most
ethnic populations who reside in countries adjacent to the
ancient Silk Road, it is still uncertain whether this HLA
molecule is directly involved in the pathogenesis of BD. In
addition to HLA-B51, the association of BD with the MICA gene
has been reported to be the consequence of linkage disequilibrium
with HLA-B51, whereas the TNF-1031C allele among TNF gene
polymorphisms has been observed to be another risk factor
independent of the presence of HLA-B51 in UK Caucasoid patients
with BD. Recently, intensive investigations on non-MHC genes,
some of which are noted to be associated with a susceptibility
to BD in several ethnic groups, are under way.
[Back to top]
HLA-B27 and B27-Subtypes in the Pathogenesis of Ankylosing
Spondylitis
T.E.W. Feltkamp
Ankylosing spondylitis (AS) is so strongly associated with
the genetical marker HLA-B27 that the molecule is supposed
to play a central role in the pathogenesis of the disease.
If this is true, it has to be explained why there is such
a difference in pathogenic consequences between certain subtypes
of HLA-B27. The subtypes B*2706 and B*2709 play probably no
pathogenic role, this in contrast to other subtypes like B*2704
and B*2705 for which such a role is evident.
The difference between pathogenic and non-pathogenic subtypes
is small and limited to the amino acid residues 114 and 116
on the antigen presenting groove of the molecule. The non-pathogenic
molecule HLA-B*2706 has, in contrast to all HLA-B27 molecules
associated with the disease, aspartic acid on position 114.
This amino acid residue is situated on the rim between the
D and the F pocket. The molecule B*2709 has histidine on position
116 on the bottom of the F pocket, which is unique.
These small but significant differences were the subject
of studies by Ringrose and Lopez de Castro. Ringrose studied
the bacterial antigen presenting capacity of HLA-B*2704, but
was not already able to compare it with that of B*2706 [1].
Lopez de Castro and his co-workers compared B*2704 and B*2706.
They showed that arginine at position 3 of peptides is better
presented by B*2706 than by B*2704, whereas alanine and tyrosine
at this position show the opposite [2].
These studies have to proceed and will help to reveal how
these small differences can be responsible for the difference
between health and disease.
[Back to top]
A Common Cause of Anemia in Inflammatory Disorders:
Anemia of Chronic Disease
Cengiz Beyan and Esin Beyan
Anemia of chronic disease (ACD), one of the most common
syndromes in medicine, is observed in patients with chronic
infections, inflammatory and neoplastic disorders. All of
the factors involved in the development of ACD can be attributed
to effects of cytokines, including shortened red cell survival,
blunted erythropoietin response to anemia, impaired erythroid
colony formation in response to erythropoietin and abnormal
mobilization of reticuloendothelial iron stores. Tumor Necrosis
Factor-alpha (TNFα),
which is important for the pathophysiology of ACD, may act
directly on bone marrow erythroid precursors. Hepcidin is
a liver-made peptide, and its synthesis is greatly stimulated
by inflammation. The plasma level of erythropoietin (EPO)
in anemic patients suffering from inflammation is often low
in relation to the blood hemoglobin concentration. Interleukin
1 and TNFα
suppress EPO gene expression. ACD is most effectively treated
via approaches directed against the underlying cause.
There are also some reports addressing that iron supplementation
and iron chelation therapy may be useful. If this is not possible,
supportive care is given through red cell transfusions or
use of recombinant human EPO. Patients with inflammatory
disorders showed remarkable hematologic responses to recombinant
EPO, although a significant change in rheumatologic picture
was not seen.
[Back to top]
Fibromyalgia
Dina Dadabhoy and Daniel J. Clauw
Fibromyalgia syndrome is a frequent cause of chronic, widespread
pain and affects up to 5% of the general population in industrial
nations. Both genetics and the environment have been implicated
in the development of fibromyalgia, and current research focuses
on evaluating neurobiological, psychological, and behavioral
factors that play a part in the disease pathogenesis. As we
better understand how these factors interact to cause symptoms
in groups of individuals, we can design treatment programs
that are more effective in individual patients. For example,
classes of drugs such as non-steroidal anti-inflammatory drugs
(NSAIDs) and opioids which are quite effective for “peripheral”
pain are typically ineffective for the “central”
pain seen in fibromyalgia. Instead, tricyclic antidepressants
(TCA) and other classes of antidepressants, antiseizure drugs,
and a number of other neuroactive compounds seem to be more
effective. In addition, non-pharmacological therapies such
as aerobic exercise and cognitive behavioral therapy are reasonably
effective, and frequently underutilized in clinical practice.
[Back to top]
The Role of Ultrasonography of Peripheral Entheses
in the Diagnosis and Assessment of Spondyloarthropathies
Paolo Falsetti, Bruno Frediani, Caterina Acciai, Georgios
Filippou,Mauro Galeazzi and Roberto Marcolongo
Enthesitis is the inflammatory process marked by the insertion
of tendons, ligaments and joint capsules on the bone and it
is a cardinal feature (and diagnostic criteria) of spondyloarthropathies
(SpA). Although it is usually revealed by clinical examination,
recent studies using magnetic resonance imaging (MRI) and
ultrasonography (US) have confirmed that enthesitis (as well
as synovitis) can often be asymptomatic, both in the axial
and peripheral skeleta. Therefore, a systematic US study of
peripheral entheses could be useful in the diagnostic process
of patients suspected with SpA, and peripheral enthesitis
scoring systems have been proposed. Recently, power Doppler
US (PDUS) has been proved to be useful for differentiating
mechanical and inflammatory enthesitis and for monitoring
the efficacy of therapy. This article reviews the main anatomical
and histopathological aspects of enthesitis and describes
the general US features of enthesis and the basic US features
of enthesitis, in its various stages. The usefulness of US
and PDUS in the diagnosis and assessment of SpA is discussed
on the basis of the available literature and our experience.
[Back to top]
MR-Based In Vivo Analysis of Joint Biomechanics
and its Relevance in the Pathogenesis of Osteoarthritis
Heiko Graichen,Rüdiger von Eisenhart-Rothe, Steafan
Hinterwimmer and Felix Eckstein
Alterations of joint biomechanics are known to play a pivotal
role in the pathogenesis of osteoarthritis. Open MRI now allows
one to assess important biomechanical parameters of diarthrodial
joints in vivo during the entire range of joint motion, encompassing
all clinically relevant joint positions, and to analyze in
particular the influence of muscle activity and neuromuscular
control.
The current article reviews data of the authors on quantitative,
open, functional MR imaging of in vivo joint biomechanics,
with focus on the shoulder and knee and gives an overview
of the literature on these topics. Further, the article summarizes
technical descriptions of the methods used as well as studies
on accuracy and reproducibility of the technique. We present
normative data on subacromial space width, glenohumeral translation
and scapulothoracic motion patterns in the human shoulder
joint of young healthy volunteers, and describe their association
with gender and body dimensions. Also, alterations of these
parameters are reported in different disease entities of the
shoulder. We present ongoing work on the functional changes
of cartilage contact areas in healthy and pathologic knee
joints and we describe how these biomechanical changes are
related to alterations of cartilage morphology. Future perspectives
of these methods are mentioned in which a combination of open
MRI and qMRI of cartilage morphology should give a more detailed
insight into the pathogenesis, progression and treatment of
osteoarthritis in different joint pathologies.
[Back to top]
Autoantibodies in Systemic Lupus: Quite a Lot or Just
a Few?
Paola Migliorini, Consuelo Anzilotti, Laura Caponi, Federico
Pratesi and Valeria Rocchi
Systemic lupus erythematosus (SLE) is characterized by the
presence of a wide variety of autoantibodies directed against
nuclear, cytoplasmic and cell membrane autoantigens. Several
lines of evidence, however, suggest that the variety of autoantibodies
in SLE may be more limited than was previously thought; different
studies clearly suggest that lupus autoantibodies are able
to bind multiple antigens. Cross-reactivity, i.e. the ability
to bind multiple antigens with high affinity, is not limited
to a single autoantibody specificity, but instead seems to
be a general property of lupus autoantibodies, distinguishing
them from immunization-induced antibodies.
Many studies on cross-reactivity have focused on the autoantibodies
present exclusively in SLE, and which are therefore considered
to be markers of the disease, such as anti-dsDNA, anti-Sm
and anti-ribosomal P protein antibodies. However, cross-reactivity
has also been shown to be a feature of SLE autoantibodies
that are not strictly disease-specific.
The structural basis of cross-reactivity is not always clear.
It may be due to the presence of common epitopes on different
antigens, or to the specific structure of the antigen binding
site that can then accommodate different epitopes. Whether
one or more mechanisms of cross-reactivity are involved, the
ability of an antibody to bind different antigens directly
affects its pathogenic potential.
[Back to top]
Etiologic Aspects of Paget’s Disease of Bone
Domenico Rendina, Gianpaolo De Filippo and Giuseppe Mossetti
Paget’s bone disease (PDB) is a focal metabolic disorder
that affects 2-3% of the population older than 60 years and
is characterized by increased and grossly distorted bone remodeling,
bone hypertrophy, and abnormal bone structure. The disease
affects one or several bone pieces and its aetiology remains
unclear. The primary cell abnormality in PDB could involve
the osteoclasts that are markedly increased in number and
size, can have 100 nuclei per cell, and contain paramyxoviral-like
nuclear and cytoplasmatic inclusions. Thirty years ago the
observation of these inclusions suggested the involvement
of paramyxovirus in the PDB pathogenesis. Nevertheless, the
paramyxoviral theory is a very controversial one. On the other
hand, familial aggregation studies indicate that 40% of affected
subjects show a PDB familial history and recent advances in
our understanding of the disease come from genetic studies.
PDB is genetically heterogeneous, with seven loci (PBD 1-7)
reported at this time. Most likely, an interaction between
environmental and genetic factors is required for patients
to develop PDB and could explain the geographic distribution
of the disease as well as its peculiar variable phenotypic
presentation.
[Back to top]
Intravenous Immunoglobulin (IVIG) in Rheumatologic
Diseases: A Review of its Mechanism of Action
Martin N. Lee and Lavjay Butani
Intravenous Immunoglobulin (IVIG) has been used since the
1970’s for the treatment of a variety of different rheumatologic
and infectious diseases. While the therapeutic efficacy of
IVIG has been definitively demonstrated in many different
disorders, its mechanism(s) of action have remained poorly
explained. This is complicated, in part by the difference
in pathophysiology of the many diseases it has been used in
the treatment of. Regardless of the types of diseases, understanding
why transfusing pooled donor antibodies to unscreened patients
fails to elicit a detrimental immunologic response, let alone
benefit these patients, needs explanation. This review aims
to explain how IVIG works by reviewing the medical literature
and the relevant basic immunology involved.
[Back to top]
Can 5-HT3 Receptor Antagonists Replace Anesthetics
and Corticosteroids in the Local Treatment of Rheumatic Processes?
Thomas Stratz and Wolfgang Müller
A local injection of the 5-HT3 receptor antagonist tropisetron
has a distinct analgesic effect on various local diseases
of the locomotor system, such as tendinopathy, periarthropathy,
trigger points and inflammatory articular processes. The effect
of tropisetron matches that of commonly used local anesthetics
like lidocaine, prilocaine and others, lasts much longer.
Animal experimental and clinical findings seem to indicate
that this prolonged action is most likely due to a concomitant
antiinflammatory effect of the 5-HT3 receptor antagonist.
It may therefore be assumed that this substance will at least
partly be able to replace the administration of anesthetics
and corticosteroids in the local treatment of rheumatic processes.
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