Duangrat Pruettivorawongse scite author profile

Duangrat Pruettivorawongse

3Publications

52Citation Statements Received

157Citation Statements Given

How they've been cited

How they cite others

147

Affiliations

Ramathibodi Hospital, Mahidol University

Publications

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A Prospective Randomized Controlled Study of Oral Tranexamic Acid for the Prevention of Postinflammatory Hyperpigmentation After Q‐Switched 532‐nm Nd:YAG Laser for Solar Lentigines

et al. 2019

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Background and Objectives Q‐switched (QS) 532‐nm Nd:YAG laser is one of the treatment options for solar lentigines (SLs). However, the high incidence of postinflammatory hyperpigmentation (PIH) is concerning, especially in dark‐complexioned skin. Tranexamic acid (TA) can decrease melanogenesis and has been used to treat melasma. The aim of this study is to evaluate the efficacy and safety of oral TA for PIH prevention and clearance in patients with SL treated with QS 532‐nm Nd:YAG laser. Study Design/Materials and Methods Forty patients with SL treated with QS 532‐nm Nd:YAG laser were enrolled in this randomized controlled trial. They were randomly assigned to be receive oral TA 1,500 mg daily or placebo for 6 weeks. Results were evaluated by blinded investigators using digital photographs, dermatoscopy, colorimetry, physician grading scores, and patient satisfaction scores at baseline, 2nd, 4th, 6th, and 12th weeks. Results The incidence of PIH, relative melanin value, lightness index, and clinical improvement scores were not significantly different between the two groups. However, the TA group had a significantly lower incidence of dermatoscopic finding of pigmented granules, which correspond to PIH at 6th and 12th weeks (P = 0.038 and 0.013, respectively). Homogenous light brown pigmentation under dermatoscopy was significantly associated with higher clinical improvement. Conclusions Oral TA therapy starting at the first day postlaser treatment is not effective for PIH prevention after QS 532‐nm Nd:YAG laser in SL. However, PIH clearance, as assessed dermatoscopically, is significantly improved by oral TA at 6th and 12th week. Lasers Surg. Med. © 2019 Wiley Periodicals, Inc.

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Clinical outcomes of topical bimatoprost for nonsegmental facial vitiligo: A preliminary study

Kanokrungsee

Pruettivorawongse

Rajatanavin

2020

J of Cosmetic Dermatology

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Vitiligo is a common acquired pigmentary disorder characterized by circumscribed white patches of depigmentation on the skin. It is caused by the destruction of melanocytes in certain areas. The prevalence of vitiligo is approximately 0.5-1% of worldwide population. 1 All races are affected, and the prevalence of vitiligo between male and female do not differ. It may appear at any age, but it presents earlier among females, and more than half of them present with symptoms of vitiligo before the age of 20. 2 Vitiligo is a multifactorial disease with complex pathogenesis, and both genetic and environmental factors play an important role

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Anti-BP180 and anti-BP230 enzyme-linked immunosorbent assays for diagnosis and disease activity tracking of bullous pemphigoid: A prospective cohort study

Chanprapaph

Ounsakul

Pruettivorawongse

et al. 2021

Asian Pac J Allergy Immunol

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Background: Autoantibodies against BP180 and BP230 play major roles in bullous pemphigoid (BP). We are the first to describe the values of serum anti-BP180 IgG and anti-BP230 IgG enzyme-linked immunosorbent assays (ELISA) for diagnosis and disease monitoring of BP among Thai patients. Objectives:We aimed to determine the diagnostic performance of anti-BP180 IgG and anti-BP230 IgG in BP, to correlate disease activity with autoantibody levels through follow-ups, and to relate BP comorbidities with disease activity and autoantibody levels.Methods: Consecutive patients suspected of having BP were included. Skin biopsy, direct immunofluorescence, and serum anti-BP180 IgG and anti-BP230 IgG tests were performed. BP disease area index (BPDAI) was evaluated at diagnosis and throughout follow-ups.Results: Of 131 patients, 68 were diagnosed with BP, and 63 were included as controls. Sensitivity and specificity of serum anti-BP180 IgG were 69.1% and 90.5%, respectively, while those of serum anti-BP230 IgG were 55.9% and 85.5%, respectively. Using anti-BP180 and anti-BP230 IgG antibodies resulted in a 7% increase in sensitivity compared with using anti-BP180 IgG antibody alone. Significant correlation with BPDAI was found for both autoantibodies at diagnosis but only for anti-BP180 IgG at follow-ups (p = 0.013). BP patients with positivity to anti-BP180 or anti-BP230 IgG had significantly higher BPDAI than did those without (p = 0.005). BP was associated with neurological diseases (p = 0.025), while patients with diabetes had higher disease activity (p = 0.010). Conclusions:While both serum autoantibodies are useful for diagnosing BP in patients with suspicious clinical features, only anti-BP180 IgG allowed prediction of disease activity over time.

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