Antimelanogenic activity of a novel adamantyl benzylbenzamide derivative, AP736: a randomized, double-blind, vehicle-controlled comparative clinical trial performed in patients with hyperpigmentation during the summer

Jeong, Yeon Su MS
Kim, Jeong-Hwan MS
Choi, Joonho PhD
Baek, Heung Soo MS
Joo, Yung Hyup PhD
Lee, Chang Seok PhD
Shin, Hong-Ju MS
Park, Young-Ho PhD
Kim, Beom Joon MD,PhD
Shin, Song Seok PhD

¹AMOREPACIFIC Corporation R&D Center, Yongin-si, Korea
²Department of Medicine, Graduate School, Chung-Ang University, Seoul, Korea
³Department of Dermatology, Chung-Ang University College of Medicine, Seoul, Korea

Received 18 May 2015; Revised 28 June 2015; Accepted 10 July 2015

Correspondence

Beom Joon Kim, MD, PhD

Department of Dermatology

Chung-Ang University Hospital

224-1 Heukseok-dong

Dongjak-gu

Seoul 156-755

Korea

E-mail: [email protected]

Song Seok Shin, PhD

AMOREPACIFIC R&D Center

314-1Bora-dong

Giheung-gu

Yongin-si 446-729

Korea

E-mail: [email protected]

Grant sponsor: AMOREPACIFIC Co., Seoul, Korea.

Conflicts of interests: None.

International Journal of Dermatology 55(6):p e321-e326, June 2016. | DOI: 10.1111/ijd.13150

Abstract

Background/Purpose

AP736 is a novel compound with an adamantyl benzylbenzamide moiety that has shown antimelanogenic activity in melanocytes in vitro and in artificial skin equivalent through the inhibition of key melanogenic enzymes and suppression of the cAMP-phosphokinase A-cAMP response element-binding protein signaling pathway. To estimate the clinical effectiveness of AP736 for the treatment of facial hyperpigmentation, we examined the efficacy and safety of a topical formulation containing AP736 compared with a vehicle formulation in human facial skin. To evaluate the degree of whitening when used in a real-life situation, subjects with hyperpigmentation conditions were selected and the trial was performed from mid-May to the end of June, when there are strong UV rays in Korea.

Materials and Methods

Forty-eight healthy Korean women aged 20–60 years were enrolled in this study for 6 weeks. Women who were pregnant or undergoing any concurrent therapy were excluded. Subjects were instructed to apply a randomly assigned formulation containing 0.5% AP736 (test formulation; n = 24) or vehicle (vehicle control; n = 24) in addition to an assigned sunscreen with a twice-daily application protocol. The degree of facial pigmentation was measured objectively using a Mexameter MX18 and Chromameter CM700, in addition to assessment by physicians using clinical photographs.

Results

The AP736 formulation was significantly (P < 0.05) more effective than the vehicle control formation in reducing the appearance of pigmentation at 3- and 6-week follow-up visits.

Conclusion

A formulation containing a novel skin whitening ingredient, AP736, effectively reduced pigmentation and was well tolerated by study subjects in summer season.