Anthranilic acid-based inhibitors of phosphodiesterase: Design, synthesis, and bioactive evaluation

Cheng, Yih-Dih; Hwang, Tsong‐Long; Wang, Han-Hsiang; Pan, Tai‐Long; Wu, Chin Chung; Chang, Wen-Yi; Liu, Yiting; Chu, Tzu-Chi; Hsieh, Pei‐Wen

doi:10.1039/c1ob05714f

Cited by 13 publications

(13 citation statements)

References 45 publications

(96 reference statements)

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“…The drug HFP034, butyl 2-[2-(2-fluorophenyl) acetamido] benzoate, was derived from anthranilic acid derivatives and exhibited potent inhibitory activity on PDE4 enzyme (IC 50 = 4.2 μM) and fMLP-induced generation of

in human neutrophils in vitro (Cheng et al, 2011 ). The drug HFP034 was found to be well-absorbed into the skin and, meanwhile, causes negligible irritation on healthy skin.…”

Section: Pde4 Inhibitors Under Development For the Treatment Of Inflamentioning

confidence: 99%

Phosphodiesterase-4 Inhibitors for the Treatment of Inflammatory Diseases

2018

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Phosphodiesterase-4 (PDE4), mainly present in immune cells, epithelial cells, and brain cells, manifests as an intracellular non-receptor enzyme that modulates inflammation and epithelial integrity. Inhibition of PDE4 is predicted to have diverse effects via the elevation of the level of cyclic adenosine monophosphate (cAMP) and the subsequent regulation of a wide array of genes and proteins. It has been identified that PDE4 is a promising therapeutic target for the treatment of diverse pulmonary, dermatological, and severe neurological diseases. Over the past decades, numerous PDE4 inhibitors have been designed and synthesized, among which roflumilast, apremilast, and crisaborole were approved for the treatment of inflammatory airway diseases, psoriatic arthritis, and atopic dermatitis, respectively. It is regrettable that the dramatic efficacies of a drug are often accompanied by adverse effects, such as nausea, emesis, and gastrointestinal reactions. However, substantial advances have been made to mitigate the adverse effects and obtain better benefit-to-risk ratio. This review highlights the dialectical role of PDE4 in drug discovery and the disquisitive details of certain PDE4 inhibitors to provide an overview of the topics that still need to be addressed in the future.

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in human neutrophils in vitro (Cheng et al, 2011 ). The drug HFP034 was found to be well-absorbed into the skin and, meanwhile, causes negligible irritation on healthy skin.…”

Section: Pde4 Inhibitors Under Development For the Treatment Of Inflamentioning

confidence: 99%

Phosphodiesterase-4 Inhibitors for the Treatment of Inflammatory Diseases

2018

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“…HFP031 (in our previous study) showed dual inhibitory effects on human neutrophil elastase and proteinase 3 (19). HFP034 (in our previous study) exhibited a potent inhibitory effect on the N-formyl-Lmethionyl-L-leucyl-phenylalanine-induced release of O 2 ×2 and phosphodiesterase (PDE)4 activity by using human neutrophils as the inflammation cell models (20). PDE4 is a cAMP-metabolizing enzyme, exhibiting a major role in inflammatory regulation.…”

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confidence: 96%

Topical application of anthranilate derivatives ameliorates psoriatic inflammation in a mouse model by inhibiting keratinocyte‐derived chemokine expression and neutrophil infiltration

et al. 2018

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Psoriasis is an inflammatory autoimmune skin disorder possessing a complex etiology related to genetic and environmental triggers. Keratinocytes show a potential role for the origin of psoriasis. In this study, we estimated the efficiency of 2 anthranilate derivatives-(E)-4-( N-{2-[1-(hydroxyimino)ethyl]phenyl}sulfamoyl)phenyl pivalate (HFP031) and butyl 2-[2-(2-fluorophenyl)acetamido]benzoate (HFP034)-on psoriasis amelioration in a mouse model. The results showed that topical treatment with both compounds could attenuate epidermal thickness and scaling in an imiquimod (IMQ)-induced psoriasis mouse model via decreased expression of cytokines and chemokines [C-X-C chemokine ligand (CXCL)1 and CXCL2], leading to the reduction of neutrophilic abscess in the skin. The in vivo cutaneous absorption of HFP034 was 7.6-fold greater than that of HFP031. Both compounds caused negligible irritation on healthy mouse skin. In addition, we examined the effect of the anthranilate derivatives on chemokine expression in IMQ-treated HaCaT keratinocytes. Our results elucidated a mechanism for anti-inflammatory activity of HFP034 that involved the elevation of intracellular cAMP concentration, suppression of NF-κB activity, and attenuation of neutrophil chemoattractant expression. These results suggest that HFP034 could increase the cutaneous concentration of cAMP to suppress neutrophil infiltration into the skin. Topically applied HFP034 may demonstrate a potential for future clinical application as a novel therapy for psoriasis treatment.-Lin, Z.-C., Hsieh, P.-W., Hwang, T.-L., Chen, C.-Y., Sung, C. T., Fang, J.-Y. Topical application of anthranilate derivatives ameliorates psoriatic inflammation in a mouse model by inhibiting keratinocyte-derived chemokine expression and neutrophil infiltration.

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“…Since the side effects of selective PDE4 inhibitors limit their clinical use, compounds with dual PDE3–PDE4 inhibitory effects will provide a new approach for the development of PDE inhibitors . In our previous study, we identified two compounds, methyl 2‐(2‐fluorobenzamido)benzoate (DSM‐RX78) and ethyl 2‐(2‐fluorobenzamido)benzoate (EFB‐1) (Figure ), which potently inhibited O 2 − generation induced by formyl‐ l ‐methionyl‐ l ‐leucyl‐ l ‐phenylalanine (FMLP) in human neutrophils by inhibiting PDEs . Of these, EFB‐1 dually inhibited the enzymes of PDE4 and PDE3 with IC 50 values (concentration that reduces cell viability by 50%) of 3.61 and 23.3 μ m , respectively .…”

Section: Introductionmentioning

confidence: 99%

“…[10] In our previous study, we identified two compounds, methyl 2-(2-fluorobenzamido)benzoate (DSM-RX78) and ethyl 2-(2-fluorobenzamido)benzoate (EFB-1) (Figure 1), which potently inhibited O2generation induced by formyl-l-methionyl-l-leucyl-l-phenylalanine (FMLP) in human neutrophils by inhibiting PDEs. [1,11,12] Of these, EFB-1 dually inhibited the enzymes of PDE4 and PDE3 with IC50 values (concentration that reduces cell viability by 50%) of 3.61 and 23.3 mm, respectively. [1] DSM-RX78, an analogue of EFB-1, was also able to elevate cAMP levels by a similar pathway.…”

Section: Introductionmentioning

confidence: 99%