The findings are consistent with a low prevalence of PsA among patients with psoriasis in Asia and confirm a high percentage of undiagnosed cases with active arthritis among PsA patients in dermatologist's office. Dermatologists should screen for PsA in their patients, especially those with risk characteristics and early signs.
Simultaneous detection of large viruses has been a great
obstacle
in the field of molecular imprinting. In this work, for the first
time, a multifunctional molecularly imprinted sensor for single or
simultaneous determination of hepatitis A virus (HAV) and hepatitis
B virus (HBV) is provided. Visual detection was realized due to the
color of green and red quantum dots that varied with the concentration
of the target substance. The combination of hydrophilic monomers and
metal chelation reduced the nonspecific binding and enhanced the specificity
of adsorption. As a result, satisfactory selectivity and sensitivity
were obtained for the detection of the two viruses, with imprinting
factors of 3.70 and 3.35 for HAV and HBV, and limits of detection
of 3.4 and 5.3 pmol/L, respectively, that were achieved within 20
min. The excellent recoveries during simultaneous detection and single
detection modes indicate the prominent ability of the proposed sensor
to detect HAV and HBV in human serum and the potential ability to
simultaneously detect multiple viruses in real applications.
This study provides evidence for the involvement of ERAP1, IL28RA, GJB2 and PTTG1 loci in PsA susceptibility and confirmed the previously reported association with PsA and PsV. These results support the hypothesis that genetic aetiology of psoriasis is the same in both PsA and PsV and also support the higher genetic component of PsA than PsV.
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