Psoriasis Clinical Trial
Official title:
Methotrexate-related Liver Toxicity in Psoriasis Patients, Using Ultrasound-based Techniques as a Diagnostic Tool
Methotrexate is one of the commonly used conventional systemic treatment for moderate to
severe psoriasis as well as psoriatic arthritis. It is also used as co-therapy with
TNF-antagonists to improve efficacy and reduce neutralizing drug antibodies formation. Apart
from the bone marrow suppression, which can largely be avoided with careful dosing,
monitoring and avoidance of certain drug interaction, hepatotoxicity is one of the major
side-effects. The prevalence of significant liver fibrosis in patients taking methotrexate is
estimated to be 5% and cirrhosis 1-2%.
The British Association of Dermatologist's guideline (2016) discussed a few non-invasive
tests such as the amino-terminal peptide of procollagen III (PIIINP), Fibrotest and transient
elastography. While PIIINP was recommended to be used in baseline and serial assessment,
liver stiffness measurement by transient elastography is not yet widely used owing to lack of
high-quality data. Transient elastography (TE) has been shown to correlate well with liver
fibrosis and has been widely adopted as a non-invasive method to assess liver fibrosis in
various chronic liver disease.
Two-dimensional shear wave elastrography (2D SWE) is a novel ultrasound technique that
combines shear wave elastography with traditional ultrasound imaging. Liver stiffness
measurement can be performed under the guidance of high rate B-mode image, allowing real-time
visualization of liver parenchyma and avoidance of non-target structures such as vessels or
focal liver lesions.
In view of the demand of a safer and reliable non-invasive test to detect advanced liver
fibrosis in psoriasis patients receiving methotrexate, we propose to recruit at-risk patients
for a paired TE and 2D SWE assessment and liver biopsy.
Methotrexate is one of the commonly used conventional systemic treatment for moderate to
severe psoriasis as well as psoriatic arthritis. It is also used as co-therapy with
TNF-antagonists to improve efficacy and reduce neutralizing drug antibodies formation. Apart
from the bone marrow suppression, which can largely be avoided with careful dosing,
monitoring and avoidance of certain drug interaction, hepatotoxicity is one of the major
side-effects. Short term rises in hepatic transaminases are well recognized with
methotrexate, which is largely reversible. However, the insidious development of liver
fibrosis and ultimately cirrhosis is of greater clinical concern given this may be
irreversible with significant impact. Methotrexate-induced liver fibrosis is still a concern
especially in patients who received high cumulative dose and those with comorbid risk factors
such as diabetes and obesity. The prevalence of significant fibrosis and cirrhosis were
reported to be 4.5 - 33.3% and 0 - 25.6%, respectively, in liver biopsy series of psoriasis
patients on methotrexate. The results were so variable owing to the facts that many studies
were old with poor reporting and variable histological scoring system making interpretation
difficult.
According to the NICE guideline and British Association of Dermatologist's guideline ( 2016),
liver biopsy remains the gold standard in the assessment of liver fibrosis, however, it is a
relatively invasive procedure, with potential sampling error and inter-observer variability,
leading to decreasing use of liver biopsy as routine for monitoring methotrexate
hepatotoxicity . Non-invasive methods to assess liver fibrosis are therefore advocated,
including serum indices as well as transient elastography.
Transient elastography has been shown to correlate well with liver fibrosis in chronic
hepatitis and has been widely adopted as a noninvasive method to assess liver fibrosis in
various chronic liver disease, but not yet in this specific Psoriasis patients on
methotrexate. There is increasing trend to use transient elastography for detection of
methotrexate-associated liver fibrosis. However, only few studies included adequate number of
patients with concomitant liver biopsy and transient elastography. Data from a study
including a relatively high number of patients with liver biopsy (24 psoriasis patients)
reported successful scan rate of 83.3% and high negative predictive value of 88% for
significant fibrosis. Alternative, Serum procollagen III level (PIIINP) for liver fibrosis is
only available in selected specialist centres oversea but not in HK and is costly. Currently,
psoriasis patients on methotrexate with cumulative dose of 3000mg of above are advised to
have USG guided Fine-needle aspiration (FNA) liver biopsy to assess the presence of liver
fibrosis with severity grading , according to American Academy of Dermatology Guideline in
Methotrexate dosing. For patient with liver fibrosis grading of 3 a or above ( Roenigfk
classification) , they are advised to stop methotrexate and switch to alternative medication.
In view of the demand of a safer and reliable non-invasive test to detect advanced liver
fibrosis in psoriasis patients receiving methotrexate, we propose to recruit these patients
for a paired transient elastography assessment and liver biopsy.
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