Inflammation Clinical Trial
Official title:
Effects of Allopurinol on Inflammatory Markers and Morphostructural Changes Evidenced by Musculoskeletal Ultrasound in Individuals With Asymptomatic Hyperuricemia. A Proof of Concept
Hyperuricemia is a metabolic alteration defined as the presence of serum urate levels higher
than 7 mg/dL. This has proven to be the maximum limit of solubility of urate in serum, any
higher concentration leads to precipitation and eventually to the formation of monosodium
urate (MSU) crystals. The accumulation of said crystals can manifest as gouty arthritis, uric
acid nephropathy, urolithiasis or chronic tophaceous gout.
A strong relation between hyperuricemia and other chronic degenerative diseases, including
diabetes mellitus, systemic arterial hypertension, obesity and metabolic syndrome, has been
consistently proven.
Hypouricemic pharmacological agents have shown a decrease in cardiovascular complications and
death in patients with gout.
A series of studies conducted on individuals with asymptomatic hyperuricemia using
musculoskeletal ultrasound (MSUS) have shown the presence of morphostructural changes
suggestive of MSU crystal deposits, combined with an elevation in a series of inflammation
markers to a degree similar to those found in patients with chronic gout.
Even though, there is evidence of morphostructural damage in individuals with asymptomatic
hyperuricemia, there are no clinical, laboratorial or imaging parameters that indicate when
hypouricemic treatment should be started.
This clinical trial is proposed as a proof of concept which is looking to evaluate if
treatment with allopurinol induces changes in levels of inflammatory markers in individuals
with asymptomatic hyperuricemia and morphostructural changes suggestive of MSU crystal
deposits. this proof of concept is not looking to measure the efficiency, effectiveness or
security of the treatment.
Our Hypothesis is that Individuals with asymptomatic hyperuricemia and morphostructural
changes evidenced by MSUS (double contour sing, tophi, aggregates) will show a decent in
inflammatory markers and their morphostructural changes will diminish or revert after
treatment with allopurinol.
Gout is the most prevalent inflammatory rheumatological disease among young men, affecting
about 4% of the general population. Caused by the deposit of monosodium urate (MSU) crystals
which form because of high urate concentrations in serum. Currently, there is no universal
definition for hyperuricemia but The Gout, Hyperuricemia, and Crystal-Associated Disease
Network (G-CAN) define hyperuricemia as a blood urate concentration above the saturation
threshold which is usually understood to be urate levels over 7 mg/dL. For this study, the
term urate will be used as the final circulating product of the enzyme xanthine oxidase in
the purine metabolism which favors the precipitation and formation of MSU crystals. Even
tough, hyperuricemia is often asymptomatic, the clinical presentation can be that of gouty
arthritis, uric acid nephropathy, urolithiasis and/or chronic tophaceous gout.
The relevance of asymptomatic hyperuricemia lays in the relation to other chronic
degenerative diseases, including atherosclerotic disease, systemic arterial hypertension,
coronary artery disease and chronic kidney disease.
A logistic regression analysis made by Zhu et al, looking specifically at the demographics of
gout and asymptomatic hyperuricemia based on the data from The National Health and Nutrition
Examination Survey (NHANES) showed a general hyperuricemia prevalence of 13.2%, which
corresponds to about 26.6 million individuals. Additionally, it was observed that
hyperuricemia increases with age, it being more common in individuals over 65 years,
prevalence of 31%, corresponding to approximately 10.7 million American adults. Other
epidemiological studies have evidenced the relationship between asymptomatic hyperuricemia y
different comorbidities for example atherosclerotic disease, systemic arterial hypertension,
coronary artery disease and metabolic syndrome. Those studies suggest that elevated urate
levels are an independent cardiovascular risk factor. Their findings also suggest that
lowering serum urate levels is associated with a descend in the risk of cardiovascular
complications. In spite of this, there is currently no indication for hypouricemic
pharmacological treatment for individuals with hyperuricemia that don´t have a diagnosis of
gout, urolithiasis, uric acid nephropathy or as prophylaxis for tumoral lysis syndrome. The
I-Lan Longitudinal Aging Study (ILAS), a cohort study from Taiwan, showed a higher
cardiovascular risk in individuals without diabetes or previous cardiovascular disease but
with serum urate levels above 6.1 mg/dL. Lastly, our group has shown that the presence of
hyperuricemia at admission in the emergency room doubles the short-term risk of death (30
days) in patients with coronary heart disease.
Hyperuricemia increases the risk of atherosclerosis by up to 60%. It is believed that the
cause for this lay in the activation of the inflammasome´s cryopyrin (NLRP3) protein complex
by the MSU crystals . This promotes the release of pro-inflammatory cytokines and chemokines,
particularly the mature forms of interleukin (IL)-1β and IL-18. In addition, the phagocytosis
of MSU crystals executed by neutrophils and macrophages, induces production of reactive
oxygen and nitrogen species all of which lead to oxidative stress and consequently to
endothelial dysfunction. When kept chronically, it is probable that these mechanisms result
in atherosclerosis. Solid evidence has shown that pharmacological treatment aimed at reducing
urate levels is beneficial in patients with gout since it lowers the occurrence of adverse
cardiovascular events and all-cause mortality. There is still a group of individuals with
chronically elevated urate levels without clinical manifestations for which pharmacological
treatment remains a topic of debate and controversy. Even though, some of these individuals
could benefit from hypouricemic pharmacological therapy, there is currently no criteria for
determining when it should be started. The first line of treatment are xanthine oxidase
inhibitors like allopurinol and febuxostat. Both lower serum urate in comparable
concentrations but a study done comparing the two agents showed that allopurinol induces a
more significant global survival rate than febuxostat therefore treatment with allopurinol is
preferred.
Musculoskeletal ultrasound (MSUS) has proven to be an excellent, noninvasive, diagnostic tool
for different articular and rheumatological diseases. Its value lays in the evaluation of
tendons, ligaments, joints and periarticular soft tissue. MSUS is useful in early stages of a
disease, when no symptoms are present, and also at the chronic stages with established
morphostructural damage. It has proven to be sensible to change, so it can be used to follow
up on morphostructural changes during the course of treatment. Additionally, having color
doppler and power doppler (PD) technology allows for the visualization of the degree of
vascularization and angiogenesis in the affected tissue. These are the reasons MSUS is
considered an innocuous imaging method which works without radiation, that is less costly and
more accessible than most other imaging technologies. A series of studies show the relevance
of MSUS for the detection of morphostructural changes suggestive of MSU deposits
characteristically found in gout. The ultrasonographic signs related to said deposits are
hyperechoic enhancement of the superficial margin of the hyaline cartilage, better known as
the double contour sign, widening of the joint cavity, aggregates, tophi, and erosions.
Wright et al compared MSUS´ and conventional radiography's capacity to detect erosions
secondary to gout on the first metatarsophalangeal joint of 78 patients. MSUS proved to be
superior in that study.
In previous studies, our group has observed the presence of morphostructural changes
suggestive of MSU deposits in individuals with asymptomatic hyperuricemia using MSUS. The
change observed in the joints was similar to that of patients with a gout diagnosis. The main
findings were hyperechoic enhancement of the superficial margin of the hyaline cartilage
(double contour sign) on the femoral cartilage and first metatarsophalangeal joint,
intraarticular tophi, as well as patellar and Achilles enthesopathy. These results have since
been replicated even in animal models, supporting that asymptomatic hyperuricemia induces
morphostructural changes in different tissues (hyaline cartilage, entheses, tendons and
subchondral bone) before leading to an acute gout attack or an episode of urolithiasis.
Recently, our group investigated a possible association between morphostructural changes
suggestive of MSU deposits and the elevation of inflammation markers in individuals with
asymptomatic hyperuricemia. For this purpose, three groups were studied: the first made up of
individuals with asymptomatic hyperuricemia, the second formed by patients with chronic gout,
and the third comprised of normouricemic individuals as a control group. All participants got
an MSUS of the knee, ankle and first metatarsophalangeal joint in search for morphostructural
changes suggestive of MSU deposits. The serum concentrations of IL-1β, IL-2, IL-4, IL-5,
IL-6, IL- 10, IL-12, IL-13, interferon -γ(INF) and tumoral necrosis factor (TNF) were
measured in all the participants. The levels of the following chemokines IL-8 also known as
C-X-C Motif chemokine ligand 8 (CXCL8), monocyte chemoattractant protein 1 (MCP-1) also known
as C-C Motif Chemokine Ligand 2 (CCL2) and epithelial-derived neutrophil-activating peptide
78 (ENA-78) also known as C-X-C Motif chemokine ligand 5 (CXCL5), and microRNA(miR) miR-146a,
miR-155 y miR-223 were also quantified.
In this study, the investigators found that individuals with asymptomatic hyperuricemia
present similar levels of cytokines and chemokines as those observed in patients with gout;
more notably the serum concentration of IL-6, IL-8 and miR-155 were significantly higher in
both groups when compared to the normouricemic controls. Also, a significant relation between
presence of MSU crystals (independent of urate acid levels) and higher levels of IL-6, IL-8
and miR-155 was found. This is the first study to suggest that the presence of MSU deposits
(detected by MSUS) are a marker of inflammatory activity independent of the existence or lack
of previous gouty arthritis episodes.
The elevated levels of inflammatory cytokines, chemokines and microRNA in individuals with
asymptomatic hyperuricemia makes questioning the need for pharmacological treatment in this
group even more relevant.
The more knowledge is gained on the beginning and progression of atherosclerotic heart
disease, the more evident it becomes that local and systemic inflammatory processes are
associated.
Chronic, systemic inflammation can be evidenced by different premature immunosenescence
phenomena, among them the loss of expression of the co-signalizing Cluster of Differentiation
28(CD 28) molecule from T CD4 + lymphocytes is of particular interest. The percentage of
Cluster of Differentiation 4 that lack the expression of Cluster of Differentiation 28 (CD4+
CD28null) is a relievable marker that is sensible to change of chronic inflammation and
atherosclerotic damage.
As a matter of fact, the presence of activated systemic inflammatory pathways could be the
etiopathogenic bond that unites a persistent elevation of urate serum concentration with the
development of accelerated atherosclerosis and adverse cardiovascular events including
coronary artery disease. By this logic, individuals with asymptomatic hyperuricemia with
evidence of MSU articular deposits are the ones that could benefit from hypouricemic
treatment since this would lower local and systemic inflammation.
A score which can be used to predict the risk of myocardial infarction or stroke (QRISK3).
The variables it uses are age, gender, ethnicity, tobacco consumption, previous diagnostic of
diabetes, chronic kidney disease, rheumatoid arthritis, systemic lupus erythematosus or
severe psychiatric disease; family history of angina or myocardial infarction before 60 years
of age, use of drugs for erectile disfunction, antihypertensives, atypical antipsychotics or
regular use of steroids, and body mass index. Its algorithm provides four results: 10-year
risk given as a percentage, the result a healthy person of the same age, gender and ethnicity
would get, relative risk, and the age at which a healthy individual would have the same risk
as the patient.
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