Version Changes
Revised. Amendments from Version 1
The title has been amended. Therapeutic applications of bakuchiol are added to the latest version as a table. A table on experimental data on the toxicity of bakuchiol is added. Finally, the conclusion is revised with future research.
Abstract
Background and aims
Natural compounds extracted from medicinal plants have recently gained attention in therapeutics as they are considered to have lower Toxicity and higher tolerability relative to chemically synthesized compounds. Bakuchiol from Psoralea corylifolia L. is one such compound; it is a type of meroterpene derived from the leaves and seeds of Psoralea corylifolia plants. Natural sources of bakuchiol have been used in traditional Chinese and Indian medicine for centuries due to its preventive benefits against tumors and inflammation. It plays a strong potential role as an antioxidant with impressive abilities to remove Reactive Oxygen Species (ROS). This review has focused on bakuchiol’s extraction, therapeutic applications, and pharmacological benefits.
Methods
A search strategy has been followed to retrieve the relevant newly published literature on the pharmacological benefits of bakuchiol. After an extensive study of the retrieved articles and maintaining the inclusion and exclusion criteria, 110 articles were finally selected for this review.
Results
Strong support of primary research on the protective effects via antitumorigenic, anti-inflammatory, antioxidative, antimicrobial, and antiviral activities are delineated.
Conclusions
From ancient to modern life, medicinal plants have always been drawing the attention of human beings to alleviate ailments for a healthy and balanced lifestyle. This review is a comprehensive approach to highlighting bona fide essential pharmacological benefits and mechanisms underlying their therapeutic applications.
Keywords: Bakuchiol, Psoralea corylifolia, medicinal plants, health benefits
List of abbreviations
- 3-NT
3 Nitrotyrosine
- 4HNE
4-Hydroxynonenal
- AKT
Protein kinase B
- ALT
Alanine Transaminase
- AMPK
AMP-activated protein kinase
- AR
Androgen receptor
- AST
Aspartate Aminotransferase
- ATM
Ataxia-Telangiectasia Mutated Kinase
- ATM
ATM serine/threonine kinase
- BAK
Bakuchiol
- Bax
Bcl-2-associated X protein
- Bcl2
B-cell lymphoma 2
- BUN
Blood Urea Nitrogen
- Cdc2
Cell division control 2
- Col I
Collagen type I
- Col III
Collagen type III
- COX2
Cyclooxygenase2
- Cr
Creatinine
- ER-alpha
Estrogen Receptor alpha
- ER-beta
Estrogen Receptor beta
- GSH-Pxi
Inducible Glutathione peroxidase
- GSTA3
Glutathione S-Transferase Alpha 3
- HIF-1
Hypoxia-inducible factor 1
- H1N1
Hemagglutinin 1 neuraminidase 1
- HPLC-UV
High Performance Liquid Chromatography – Ultra Violet
- HNO 3
Nitric acid
- IL6
Interleukin 6
- iNOS
Inducible Nitric Oxide Synthase
- KIM-1
Kidney Injury Molecules - 1
- LDH
Lactate Dehydrogenase
- LTB4
Leukotriene B4
- LPS
Lipopolysaccharide
- MDA
Malondialdehyde
- MAPK
Mitogen-activated protein kinases
- MMP-1
Matrix metalloproteinase-1
- Myt1
Myelin Transcription Factor 1
- NAG
N-Acetyl-Glucoseamindase
- NFkB
Nuclear Factor kappa-light-chain-enhancer of activated B cells
- NQ01
NAD(P)H Quinone Dehydrogenase 1
- NSCLC
Non-small cell lung cancer
- Nrf1
Nuclear Respiratory Factor 1
- p38
Tumor protein p53
- PGC-1α
Proliferator-activated receptor gamma coactivator 1-alpha
- PGE2
Prostaglandin E2
- P-Cdc2
Phosphorylated cell division cycle protein 2
- Rac
Ras-related C3 botulinum toxin
- ROS
Reactive Oxygen Species
- SARS-CoV-2
Severe Acute Respiratory Syndrome-CoronaVirus-2
- Sirt1
NAD-dependent deacetylase sirtuin-1
- STAT3
Signal transducer and activator of transcription 3
- SOD
Superoxide Dismutase
- TIMP-1
Tissue inhibitors of metalloproteinases-1
- TIMP-2
Tissue inhibitors of metalloproteinases-2
- TNFα
Tumour Necrosis Factor alpha
- Trx1
Thioredoxin 1
- TXNIP
Thioredoxin-interacting protein
Introduction
Plants have been used in traditional Indian and Oriental medicine for centuries. Despite improved access to essential medicines as supported by World Health Organization (WHO), 1 a large population, especially in less developed countries, still relies on plant-based medications for primary health care needs due to ease of availability and high benefit to cost ratio. 2 There is an increase in global demand for medicinal plants due to improved quality of life. Some compounds have been extracted from these beneficial plants to study their mechanisms of action that facilitate their beneficial effects.
Bakuchiol, extracted predominantly and traditionally from the Psoralea corylifolia L. plant, is one such compound. It is a meroterpene that has shown potent antimicrobial, anti-inflammatory, anti-osteoporotic, and antitumorigenic activities and exhibited other beneficial uses. 3 It has also gained huge popularity in the beauty industry as a tolerable analogue of retinol in skin therapeutics. 4 Studies have also shown bakuchiol’s protective effect on the liver, heart, bones, and other organs. 5 Recent studies have focused on bakuchiol and its therapeutic effects, showing promise as a multi-targeting therapeutic agent. 6 – 13
Bakuchiol is a naturally occurring prenylated phenolic isoprenoid ( Figure 1). It is a type of meroterpene with a chiral tetra-alkylated (all-carbon) quaternary center. 15 It was first extracted from the seeds of Psoralea corylifolia in 1966 when its plane structure was also determined, while its configuration of the quaternary center was determined in 1973. 16 The formal chemical name of bakuchiol is 4-[(1E,3S)-3-ethenyl-3,7-dimethyl-1,6-octadien-1-yl]-phenol. Its naturally occurring form (S)-(+)-Bakuchiol has an enantiomer (R)-(-)-Bakuchiol, and its chirality influences their actions and effectiveness.
The source of bakuchiol varies between regions; it is commonly extracted from the seeds and leaves of Psoralea corylifolia (Babchi plant) in India, which belongs to the Leguminosae plant family, and is a major phytochemical present in the root and stem of Ulmus davidiana var. 17 Japonica (Japanese Elm) is widely distributed in China, Japan, and Korea. 6 These plants have been used in their regions of wide distribution in traditional medicine to treat inflammatory disorders and cancer. Piper longum (Long pepper) , Psoralea glandulosa L, Otholobium pubescens, Prosopis glandulosa, Aerva sanguinolenta, Psoralidium tenuiflorum, Pimelea drupacea, Bridelia retusa, Spiraea formosana, Elaeagnus bockii and other sources of bakuchiol have been discovered in recent times. 17 – 20
Medicinal plants e.g.: Psoralea corylifolia where bakuchiol is derived have been used directly as traditional medication or via pharmaceutical preparations in modern medicine. Recent times have shown collective evidence highlighting the immense potential of traditionally used medicinal plants and their derived compounds. 21 An increase in international demand and trade has also been observed, appreciating its low costs and tolerability. In addition, an increasing trend of antimicrobial resistance has been observed due to inappropriate dosage and lack of regulation of prescriptions. It is thus imperative to find new sources of antiviral and antimicrobial therapy to account for the increased resistance observed. Plants and phytochemicals are generally considered sources of tolerable, less toxic treatments. 21 Bakuchiol has recently been studied in detail in research settings while being used in traditional medicine for centuries. 22
This review article focuses on the potential pharmacological benefits of bakuchiol, focusing on its promising protective effects in controlling activities that lead to the amelioration of non-communicable diseases, as well as verifying its function as an antimicrobial and antiviral agent. The workflow of this review is illustrated in Figure 2. The knowledge gained from this review will shed light on the published research to pave the path for future research perspectives and considerations.
Methods
Retrieval of the published articles
This review evaluates the pharmacological uses of bakuchiol, focusing on its promising protective effects on controlling both communicable and non-communicable diseases. Data for this study have been amalgamated from both primary and secondary data resources, including clinical trials (both randomized and non-randomized), as well as in vitro and in vivo studies, which have evaluated the use of bakuchiol as a potential pharmacological agent in controlling multiple disease conditions.
Several inclusion and exclusion criteria were fixed while selecting articles for this review. The works done from 1990 to 2022 have been studied rigorously. Literature searches were done using keywords such as “ Psoralea corylifolia AND/OR Babchi AND/OR Bakuchiol” in various available online scientific databases. Articles that represent phytochemistry AND/OR pharmacological activity AND/OR health benefits of Bakuchiol published in PubMed, Web of Science, PMC, Google Scholar, ScienceDirect, and ResearchGate were incorporated in this review. From the evaluation of 110 articles, the effect of bakuchiol as a potential antitumorigenic, anti-inflammatory, antioxidative, antimicrobial, and antiviral agents, as characterized in several studies, was finally assessed for this review. In addition, clinical trial databases were also searched to find current registered clinical trials of the use of bakuchiol in multiple disorders, including diabetes, inflammatory disorders of the skin and other organs, oral disorders, cancer, and coronavirus disease 2019 (COVID-19). Only articles published in English were considered for this review. The databases were searched in a timeline from 2010 to date, except for articles related to its initial discovery and extraction, and only approved and published data were considered for this review unless otherwise mentioned. In most studies, the outcomes measured and considered for this review include the severity and comparative assessment of disease progression in bakuchiol-treated and untreated groups.
Results
Extraction and solubility of bakuchiol
Traditional plant-based medications work by grinding the interest portion and then extracting it into carrier oils or spirits. 24 However, specific compounds cannot be distilled this way and there may also be the presence of potentially cytotoxic compounds in an extract made in traditional methods. 25 , 26 While beneficial, the number of bioactive ingredients present in natural sources is generally meager, and extraction processes are time-consuming and lab-intensive, hindering the mass-scale use of natural products in drug selection and development. Current extraction methods include distillation, cold pressing for oils, and solvent extraction, the most commonly used method. 27
Factors that affect the ease of solubility and diffusivity are considered during extraction processes, including consideration of the properties of the solvent being used, such as the laws of inter miscibility as well as cost and safety, the size of the raw substances material being used, temperature and time duration. 27 Generally, methanol and ethanol are used in solvent extraction for phytochemicals. Smaller particle sizes of raw substances are preferred for better extraction efficiency. 28 Temperature is also an essential factor in controlling the extraction rate, as higher temperatures increase solubility and diffusion, but this is not ideal for highly volatile compounds as higher temperatures can cause the decomposition of thermolabile compounds. 29
Bakuchiol is soluble in organic solvents such as ethanol and dimethyl sulfoxide (DMSO) and sparingly soluble in aqueous solutions. 6 Its solubility can be increased by first making a stock solution with ethanol and then diluting it with aqueous buffers for experimental purposes. The most commonly reported method is extraction with 80% ethanol, followed by silica column chromatography. 6 This method is also suitable for deriving other phenolic phytochemicals present in the sources of bakuchiol.
The first synthesis of the naturally occurring form of bakuchiol was done by Carnduff and Miller in 1967, with a Claisen rearrangement being a crucial part of the synthesis process; however, this was not enantioselective. 20 Other variations in chemical synthesis methods have also been developed over the years, but current methods focus on concisely synthesizing enantioselective (S)-(+)-Bakuchiol. It is also synthesized chemically in four steps from (E)-geranic acid under aldol reaction conditions, with an overall yield of 53%, increasing commercial availability. 30 Stock solutions of (S)-(+)-Bakuchiol synthesized from (E)-geranic acid can be made by dissolving the compound in DMSO.
However, conventional extraction methods require a large solvent volume and longer durations. Separation techniques have developed and come a long way. More sophisticated techniques, including various forms of chromatography, have been developed to extract specific compounds from the plant source. 14 Other methods (supercritical fluid extraction, pressurized liquid extraction, and microwave-assisted extraction) with much shorter extraction time and lower solvent consumption may be considered for mass extraction of bakuchiol. 14 They may be used on a large scale for cheaper drug development. These methods have also been used to extract natural products, so their efficiency in the extraction of bakuchiol needs to be evaluated. 31
Methods are being studied to increase the bioavailability and absorption of bakuchiol and its sources. Cho et al. (2011) studied the stability and physicochemical property of P. corylifolia extract encapsulated in 3 different vesicles (liposome, niosome, and transfersome) in nude mouse skin. 32 The results of this study suggest that the use of niosome and transfersome could be a good bioavailability enhancement system (BAES) for P. corylifolia extract to improve skin permeation and stability, highlighting the importance of finding methods to increase the bioavailability of bakuchiol and other phenolic phytochemicals. 32
Therapeutic applications of bakuchiol
A large number of studies have evaluated the role of various phytochemicals and their pharmacological applications in communicable and non-communicable diseases. 33 In addition, other potentially beneficial compounds have also been extracted from the plant sources of bakuchiol. 31 However, since this review focuses on bakuchiol and its pharmacological benefits, other phytochemicals and compounds will not be reviewed in detail and will only be referred to as appropriate. A brief description of the extraction and solubility of bakuchiol precedes the comprehensive analyses of its various pharmacological benefits. The mechanism of actions, functions, and uses of the naturally occurring compound, bakuchiol and its implications in therapeutic approaches are described below and illustrated in Figure 3.
Anti-Inflammatory effects of bakuchiol
Inflammation is generally caused by the production of pro-inflammatory mediators and cytokines such as nitric acid, prostaglandin E2 (PGE2), tumor necrosis factor-alpha (TNF-α), and interleukin 6 (IL-6). 34 The anti-inflammatory effects of bakuchiol have been evaluated in multiple studies, and it has been found that the anti-inflammatory effects of bakuchiol work via various mechanisms. 7 It can inhibit the degranulation of neutrophils and decrease cell migration and myeloperoxidase activity (involved in producing oxidants such as hypochlorous acid) in inflammatory sites, generating multiple mechanisms of controlling leukocyte function and inflammation in various types of cells. 35
Studies have reported the ability of bakuchiol to inhibit nitric acid and PGE2 production, both pro-inflammatory mediators generated by inducible enzymes nitric oxide synthase and cyclooxygenase-2. 6 – 8 A concentration of 50μM of bakuchiol has shown a reduction in nitric acid and PGE2 in macrophages by over 50% without exhibiting cytotoxicity. 6 Bakuchiol can inhibit the expression of nitric acid synthase gene via the inactivation of nuclear factor kappa-light-chain-enhancer of activated B cells (NFkB), which can inhibit nitric acid production and IL-6 induced signal transducer and activator of transcription 3 (STAT3) activation, inhibiting IL-6 production in multiple cell lines. 36 This is comparable to other natural compounds, such as aurantiamide acetate from the roots of the Baphicacanthus cusia. 37
Bakuchiol can suppress inflammatory, responses via downregulation of the p38 MAPK/ERK signaling pathway in microglia cells controlling neuroinflammation. 7 Moreover, it can reduce the production of leukotriene B4 (LTB4), which contributes to disease severity in chronic inflammatory diseases in a dose-dependent manner. 38 LTB4 can generate reactive oxygen species (ROS) via a Rac-dependent pathway, and a reduction in LTB4 production also reduces ROS production. 39 Bakuchiol and its derivatives have also exhibited inhibitory activities in lipopolysaccharide (LPS) induced NO production in macrophages. 40
Bakuchiol decreases the phosphorylation of ERK, p38, and NF-κB. It arrests the mRNA expression of pro-inflammatory molecules, including TNF-α and interleukin-1β (IL-1β), and inducible nitric oxide synthases (iNOS) in Methylglyoxal-administered mice, which reduces inflammation and helps in the prevention and control of diabetes. 41
Altogether, bakuchiol can provide beneficial therapeutic implications in treating inflammatory diseases such as nephritis, asthma, diabetes, skin inflammatory conditions such as psoriasis, and neurodegenerative disorders such as Alzheimer’s. 40 – 42
Antimicrobial effects of bakuchiol
Nature provides a great potential source for antimicrobial drug discovery. Phytochemicals extracted from natural sources are considered to have fewer side effects and a variety of functions, and some exhibit antimicrobial activity. In addition, natural compounds are much more accessible than synthetic compounds available for treatment; most developing countries depend on plant-based medications as the first line of treatment. 43
Terpenes such as thymol, carvacrol, eugenol, and menthol, most commonly used in fragrances and aromatherapy, show broad-spectrum antimicrobial activity through efflux pump inhibition and inhibition of bacterial growth. 44 – 46 Bakuchiol is also a terpene that has recently been characterized to have multi-beneficiary effects on disease control, both communicable and non-communicable.
The antimicrobial effects of bakuchiol have been studied as a natural source of oral healthcare, and multiple studies have shown potent antimicrobial activity. 11 , 47 , 48 Studies evaluating bakuchiol’s antimicrobial effect have shown potent antibiotic effects against Streptococcus aureus. Another study examining the antimicrobial effects of bakuchiol against Streptococcus mutans showed increased inhibition in the growth of colonies in a dose-dependent manner. Similar results were observed for Streptococcus sanguis, Streptococcus salivarius, Streptococcus sobrinus, Enterococcus faecalis, Enterococcus faecium, Lactobacillus acidophilus, Lactobacillus casei, Lactobacillus casei, Lactobacillus plantarum, Actinomyces viscosus, Porphyromonas gingivalis and other bacterial strains that contribute to oral diseases. 11
Conventional treatments for oral infections usually contain chlorhexidine, a gold standard. 49 However, as it was toxic in large quantities and caused discoloration of the tooth surface, other natural-based alternatives were evaluated, some of which were successful inhibitors for antimicrobial growth. 50 – 53 There is also a concern about emerging antimicrobial resistance, which has increased rapidly in the past decade and is now one of the leading causes of death. 54 , 55 Given the increasing emergence of antimicrobial drug-resistant strains, finding nature-based alternatives to antibiotics is vital to help control the resistance.
Bakuchiol works by rupturing the cell membrane in bacterial strains, inhibiting DNA polymerase and other DNA replication enzymes, and reducing biofilm production by E. faecalis and E. faecium. 56 These studies implicate the potential uses of bakuchiol in maintaining oral health care. It can potentially be used in combination with other natural pre-existing methods of oral healthcare to target the increasing demand in the market for natural healthcare products.
Bakuchiol also has antifungal effects, and ethanol isolates of bakuchiol from PF effectively inhibit the growth of dermatophytes in vitro. 57 Oral Candida species have also been susceptible to bakuchiol treatment with minimum inhibitory concentration (MIC) ranging from 12.5 to 100 μg/mL, causing a reduction in growth rates, viable counts, cell metabolic activity and biofilm mass. 58
Bakuchiol in the treatment of skin disorders
Bakuchiol has recently gained mass popularity as an active component in skin care products due to its functional similarity with retinoid compounds and relatively higher tolerability. 59 It has been shown to work with melatonin and vitamin C derivatives to regulate genes involved in the modulation of angiogenesis, collagen biosynthesis, skin barrier function, and other aspects of skin cell biology. 9 Bakuchiol also has retinol-like properties in modulating genes that regulate extracellular matrix production and the dermal-epidermal junction. 60 It can help deter skin aging by enhancing human fibroblast cell activity and inhibiting the expression of matrix metalloproteinases by increasing tissue inhibitors of metalloproteinases-1 (TIMP-1), tissue inhibitors of metalloproteinases-2 (TIMP-2), collagen type I (Col I), and collagen type III (Col III) mRNA, and decreasing the expression of matrix metalloproteinase-1 (MMP-1) mRNA. 61
Bakuchiol exhibits retinol-like functionality, causing upregulation of types I, III, and IV collagen, which make up the skin’s extracellular matrix and basement membrane, in in vitro models. 4 When formulated into a skincare product, regularly applied, and tested under clinical settings for 12 weeks, significant improvement in facial fine lines and wrinkles were observed, along with improvements in skin elasticity, firmness, and pigmentation, as well as a reduction in photodamage. 4 This effect was observed in multiple studies on participants of varying races. 4 , 59 In addition, other studies have also confirmed an increase in moisture retention from the regular application of products formulated with bakuchiol extract. 62 It also works synergistically with other natural compounds to reduce inflammation and protect and maintain naturally aging skin. 10
This higher tolerability allows bakuchiol to be an effective anti-aging treatment for people of all skin types. Furthermore, it can also be formulated for people with hyperpigmentation, historically perceived as less tolerant of retinol. 63
Unlike retinoids, bakuchiol can be used daily due to its photostability. 59 Combinations of retinoid and bakuchiol therapy also reduce oxidative stress induced by retinoids, 64 as bakuchiol helps to stabilize retinol under photo-oxidative environments.
Bakuchiol works as an antioxidative agent due to its ability to interfere with free radical production, decrease the translocation of mitochondrial apoptosis-inducing factors, and its ability to quench superoxides and other radicals in vitro. 13 , 49 Overall, it can be deduced that its naturally occurring phytochemical functions as a potent antioxidant that can help maintain cellular turnover and ensure protective functions for all organs. With higher tolerability, photostability, and ability to slow down skin aging, bakuchiol can be considered a suitable plant-based alternative to retinol, traditionally extracted from animal sources.
Antitumorigenic effects of bakuchiol and Hormone replacement therapy
Bakuchiol has traditionally been used in medicine for the treatment of various cancers. Early studies have shown that bakuchiol can inhibit cell proliferation, and further studies have recently evaluated its mechanisms of action in various cancer cell lines compared to its analogue resveratrol. 12 It can induce ROS-related apoptosis in lung adenocarcinoma A549 cell line, S phase arrest, caspase 9/3 activation, p53 up-regulation, and B-cell lymphoma 2 (Bcl-2) downregulation, all of which contribute to anticancer activities. 12 Bakuchiol has also shown inhibitory effects on DNA polymerase enzymes, while a related compound Bakuchicin inhibits the actions of topoisomerase II. 65 Its effects on DNA replication enzymes and relatively much lower cytotoxic effects than its analogue resveratrol make it a potent tolerable therapeutic compound for treating non-small cell lung cancer. 12
High doses of bakuchiol (>2 μg/mL) inhibited cell proliferation of breast cancer MCF-7 cells through actions via estrogen receptors (ER), inducing ERβ expression and suppressing ERα expression. 66 S phase arrest was also observed in MCF-7 cells along with upregulation of ATM serine/threonine kinase (ATM), phosphorylated cell division cycle protein 2 (P-Cdc2), p21, myelin transcription factor 1 (Myt1), and downregulation of Cyclin B1, which implies the blocking of Cdc2 activation by upregulation of ERβ may play a role in the S phase arrest. 66 It also induced apoptosis in MCF-7 cells with an increase in expression of pro-apoptotic Bcl-2 and cleaved caspase proteins, pointing towards its involvement in apoptosis via the intrinsic mitochondrial pathway, similar to that observed in the lung adenocarcinoma A549 cell line and even liver cancer cell lines. 12 , 66
In addition, bakuchiol was found to effectively inhibit the activation of hypoxia-inducible factor 1 (HIF-1) and NFkB in gastric cancer AGS and cervical adenocarcinoma HeLa cell lines. 67 It also inhibits proliferation, migration and invasion of androgen-independent prostate cancer cell line PC-3 by inactivating NF-κB signaling via Androgen receptor (AR) and ERβ expression in a time and dose-dependent manner. Bakuchiol’s cytotoxicity was considered in this assay via LDH assay, and the non-toxic concentration used in further experimentation was determined to be at 10 μM. 68
Bakuchiol-treated NUGC3 gastric cancer cells have also been shown to express reduced levels of phosphorylated protein kinase B (AKT) protein and increased p-extracellular signal-related kinase 1/2 (ERK1/2) and p-c-Jun N-terminal kinase (JNK) expression, indicating the induction of cell death was mitochondria-dependent, working via the MAPK/PI3K/AKT pathways. 69
Furthermore, bakuchiol was shown to induce estrogenic activity in vivo and in vitro study models. 66 It activates the ERβ receptor and suppresses the ERα receptor, which reduces CDC2 activity and promotes S phase arrest, reducing tumor cell proliferation. 66 This promotes bakuchiol as a phytoestrogen and anticancer drug, promoting safer hormone replacement therapeutics. Bakuchiol can also prevent bone loss and delay osteoporosis in post-menopausal women by activating the ERs. 70 This is of increased significance as hormone replacement therapies usually use estrogen, which is linked with an increased risk of breast cancer.
There have also been other compounds extracted from Psoralea corylifolia L.that express similar pharmacological activities. 71 Psoralidin, a natural phenolic coumarin, is one such compound that is beneficial in various diseases, including osteoporosis and hormonal cancers. 72 This is elucidated by inducing oxidative stress and apoptosis in tumorigenic cells, which promote autophagy-dependent cell death and activate the ER signaling pathway. The use of bakuchiol or other anticancer natural compounds should be evaluated to check further their efficacy in preventing or controlling cancer development. This would provide a suitable cheaper alternative to current cancer chemotherapeutics in the market, which are not accessible equitably among patients due to high costs.
Antioxidative effects of bakuchiol
There has been an increasing interest in identifying and characterizing antioxidant compounds to treat oxidative stress and related diseases, among which bakuchiol has been characterized as it has shown vital antioxidant activities in multiple studies. 5 , 20 , 73 When studying the scavenging activity of bakuchiol against various oxidizing radicals, it was determined that the terpenoid chains present in bakuchiol play a role in preventing lipid peroxidation. 13 It can protect against rat liver injury by inhibiting lipid peroxidation, 74 with similar effects expressed by studies on other natural products such as pumpkin seeds and acanthoic acid. 75 Bakuchiol can also inhibit liver fibrosis and show hepatoprotective effects by inhibiting oxidative stress while inducing apoptosis in myofibroblasts, relieving the hepatotoxicity of various toxicants. 74 , 76 Bakuchiol reduced cell death in retinal ganglion cells (RGC-5) and reduced ROS-induced apoptosis and cell death in vitro. 49
In vivo studies have demonstrated that bakuchiol reduces retinal degeneration following optic nerve injury. 49 It has also been observed that bakuchiol can protect against sepsis and sepsis-induced acute kidney injury by significantly reducing inflammation and renal oxidative stress while inhibiting induced activation of NFkB and p38-MAPK signaling pathways in the kidneys. 77 Its ability to block NFkB signaling also allows for cardioprotective functions, as seen in various mice models, allowing its application as a potential treatment for pathological cardiac hypertrophy. 78
In another study, bakuchiol showed protective effects against early brain injury by reducing ROS, malondialdehyde (MDA), 4-Hydroxynonenal (4-HNE), 3-Nitrotyrosine (3-NT), and other biomarkers of oxidative stress produced by lipid peroxidation. 79 Conversely, it causes increases in the enzyme activity of superoxide dismutase (SOD) and inducible glutathione peroxidase (GSH-Pxi), both of which play crucial roles in the body’s antioxidant defense system while reducing mitochondrial damage. As seen in this study, phosphorylation of AMP-activated protein kinase (AMPK) and thioredoxin 1 (Trx1) protein levels increased. In contrast, thioredoxin-interacting protein (TXNIP) levels decreased due to treatment with bakuchiol, which was thought to have occurred due to the regulation of Trx1 and TXNIP levels.
Bakuchiol may be considered a potential candidate for the prevention and treatment of insulin resistance as it can reduce induced insulin resistance and oxidative stress with reduced ROS expression and enhanced antioxidant enzyme expression. 41
Bakuchiol can also reduce the severity of myocardial ischemia-reperfusion injury (IRI) by impairing mitochondrial oxidative damage through regulation of sirtuin 1/proliferator-activated receptor gamma coactivator 1-alpha (SIRT1/PGC-1α) pathway signaling via increased in the expression of SIRT1. 80 It reduced mitochondrial oxidative damage by increasing the action of mitochondrial succinate dehydrogenase, cytochrome c oxidase, and mitochondrial SOD and decreased the production of malondialdehyde. 79
Bakuchiol has also increased anti-apoptotic Bcl2 and decreased pro-apoptotic Bax and cleaved caspase 3, which helps control injury-induced cell death, and inhibitors of SIRT1 abolished the effects of bakuchiol further highlight the role of its interaction with SIRT1 signaling. 78 Bakuchiol has also been found to reduce hyperglycemia-induced cardiomyopathy by activating the SIRT1/Nrf2 pathway, which reduces myocardial oxidative stress and elevates antioxidant production. 73
Similar effects are observed in other natural products such as curcumin, melatonin, berberine, and icariin. 80 – 84 These also reduce myocardial IRI via other pathways, highlighting the importance of studying the other potential signaling pathways regulated by bakuchiol, which leads to its ability to reduce injury-induced cell damage. Moreover, bakuchiol should be combined with other natural compounds with similar protective effects for potential synergistic activity.
Antiviral effects of bakuchiol
The antiviral effect of bakuchiol has been evaluated in some studies. 15 , 85 , 86 Viral diseases are constantly evolving in pathogenicity, and certain strains have been reported to be highly pathogenic to humans, as was seen in the influenza A pandemic in 1918, causing 50 million deaths, 87 and in the current pandemic caused by the SARS-CoV-2 virus, 88 which has infected more than 500 million people and has caused more than 6 million deaths since its first reported case on December 31, 2019. 89 The SARS-CoV-2 virus enters the host cell via the interaction between its receptor-binding domain (RBD) of spike glycoprotein with the angiotensin-converting enzyme 2 (ACE2) receptor found on the plasma membrane of the host cell. 90 Given the rapid emergence of resistant viral strains, searching for potent and tolerable antiviral drugs is essential to combat and control viral infections.
Plant-based natural compounds are being examined extensively for their therapeutic effects, 91 , 92 and bakuchiol has also been evaluated, given its use in traditional medicine systems to treat a wide range of diseases. In in vitro studies on Madin-Darby canine kidney (MDCK) cells infected with influenza A H1N1 strain, the naturally occurring form of bakuchiol was found to inhibit influenza A growth and infection while reducing expression of viral mRNAs and proteins, decreasing viral load. 15 In addition, it also was able to activate Nrf2 and two Nrf2-induced genes, NAD(P)H quinone oxidoreductase 1 and glutathione S-transferase A3, promoting activation of transcriptional regulation and regulating virus-induced host body oxidative stress response. To a lesser extent, these effects were also observed in its enantiomer form, highlighting the importance of chirality in designing potent antiviral drugs.
Further studies on related compounds such as cyclobakuchiols A, B, and C, derived from (+)-(S)-Bakuchiol as well as from its natural sources, have also established strong potential to inhibit viral growth, infection, and expression of viral mRNAs and proteins in influenza A virus-infected MDCK cells via similar mechanisms. 85 Other natural compounds derived from natural sources show antiviral actions against Influenza A, such as aurantiamide acetate extracted from the plant’s roots Baphicacanthus cusia. 37 These compounds work via similar mechanisms as bakuchiol, as observed in MDCK cells. In addition, these natural compounds also reduce virus-induced inflammatory responses via the suppression of NF-kB signaling pathways and pro-inflammatory cytokines. 93
In a more recent study, bakuchiol effectively inhibited severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) pseudovirus entry at concentrations of up to 100 μM without Toxicity. Furthermore, in HEK293 cell lines overexpressing human ACE2 receptors, bakuchiol also effectively blocked RBD-ACE2 binding at the cell membrane. 86 This also implies that further evaluation of bakuchiol on its effect on other viral diseases is critical in the current pandemic setting caused by the SARS-CoV-2 virus to find effective antiviral treatments to reduce disease transmission and severity.
Other natural compounds have also been evaluated in recent studies, among which epigallocatechin gallate (EGCG), 20(S)-ginsenoside Rg3 (SRg3), 20(R)-ginsenoside Rg3 (RRg3), isobavachalcone (Ibvc), and isochlorogenic A (IscA) were found to effectively inhibited pseudovirus entry at concentrations up to 100 μM. 86 , 94
Among these compounds, EGCG and lbvc have shown comparable effects to bakuchiol administration by inhibiting the SARS-CoV-2-induced cytopathic effect and plaque formation and demonstrating a dual binding to RBD and ACE2. 93 Another compound, 1,2,3,4,6-O-Pentagalloylglucose (PGG), also effectively inhibited virus binding and infection in ACE2 overexpressing human host cells, binding more with Spike-RBD than ACE2 receptors. 95 It blocks the fusion of SARS-CoV-2 to hACE2 receptors on a dose-dependent level. Spike RBD PGG was also found to exhibit anti-influenza-virus activity by reducing the accumulation of nucleoprotein and viral hemagglutinin in plasma membranes at the late stage of the replication cycle and inhibiting the release of progeny virus from infected cells. PGG also works in ameliorating HBV, HCV, HIV infections. 95 PGG may be a safe and potential antiviral agent against COVID-19 by blocking the fusion of SARS-CoV-2 spike-RBD.
Combination effects
Most studies evaluating the effects of bakuchiol used in combination with other molecules tend to be formulated by the cosmeceutical industry. It is also used in combination with retinol to help increase its photostability, or moisturizing molecules like squalene, working synergistically to improve skin elasticity and texture.
Bakuchiol can be combined with Vanilla tahitensis extract to inhibit skin photoaging and cause improvement in skin barrier function and elasticity, increasing cellular turnover and improving signs of aging. 10 A study by Bacqueville et al. used an in vitro skin model made of human dermal fibroblasts treated with the compounds alone or in combination, after which they were exposed to an acute dose of UVA. Exposure to UVA-induced significant morphological changes and increased IL-8 and p16 expression in the control model (no treatment), suggesting inflammation and senescence. Compared to control, treatment with either compound alone prevented actin network alteration and IL-8 upregulation while protecting against IL-8 and p16 overexpression in combination. This combination was also formulated into serum and tested in participants who applied it twice daily for 56 days. These compounds can work synergistically to reduce ptosis and skin deformation and improve the radiance of naturally aged skin in women.
A face serum containing bakuchiol, palmitoyl tripeptide-38, hydrolyzed hyaluronic acid and a polyherbal and vitamin blend was tested in 55 healthy adults. Daily use for 3 months indicated improvements in skin as seen in in vitro studies and clinical trials on healthy volunteers. 60 Protection of skin structure was observed in vitro with reduced collagenase activity and significant free radical scavenging activity as observed through increased gene expression of dermal collagen, elastin and hyaluronic acid synthesis. In addition, substantial improvements in skin elasticity, hydration, roughness (fine lines and wrinkles), and brightness occurred during the trial.
It also works marvelously in combination with melatonin and ascorbyl tetraisopalmitate to cause significant clinical anti-aging effects when applied once daily, 96 with a statistically significant decrease in wrinkles and redness, an increase in skin firmness and overall improvement in skin quality and complexion as well as hydration. 96 A combination of bakuchiol, Ginkgo biloba extract and mannitol was also shown to improve the efficacy of adapalene treatment in patients suffering from Acne Vulgaris. 9 It has also been found to work exceptionally well with salicylic acid in managing P. acnes. 97
Outside of the dermatocosmetic industry, the use of bakuchiol can also improve the efficacy of various non-cosmetic treatments. Bakuchiol has been found to work in combination with tumor necrosis factor (TNF)- related apoptosis-inducing ligand (TRAIL) to inhibit the growth of TRAIL sensitive (HCT116) and resistant (HT-29) colon cancer cell lines. 98 Combination treatment of bakuchiol with TRAIL on these cell lines significantly upregulated the expression of TRAIL cell death receptors DR4 and DR5 in a dose-dependent manner, as well as the expression of the pro-apoptotic proteins PARP and the cleaved caspases 3, 8 and 9, while suppressing the expression of survival proteins such as cFLIP, survivin, XIAP and Bcl2. Pretreatment of cells with JNK inhibitor SP600125 and ROS scavenger N-acetylcysteine and the depletion of DR4 or DR5 by small interfering RNA reduced the bakuchiol-induced cell growth inhibition. Bakuchiol assists with TRAIL-induced apoptosis via the ROS/JNK pathway.
When used alone or in combination with A llium sativum, it also demonstrated potent antimicrobial properties, with bakuchiol and A llium sativum showing synergistic effects when used in combination. 99
Table 1. Therapeutic applications of bakuchiol.
Therapeutic Application | Mechanism | Extract of Plant | Part of Plant | Plant Name | ED50 value | Reference |
---|---|---|---|---|---|---|
Anti-Inflammatory | Degranulation of neutrophils, decrease cell migration, myeloperoxidase activity, Nitric acid synthase gene inhibition | Ethanol, Seed | Leaves, Seeds | Psoralea glandulosa L. Psoralea corylifolia | 50 μM | 35 |
Antimicrobial | Efflux Inhibition, Microbial growth inhibition, Inhibition E. faecium & E. faecalis DNA polymerase | Ethanol | Leaves | P. lingue | 100mg/L & 1-4 μg/ml | 44 , 56 |
Skin Disorders | Modulate gene of extracellular matrix production, Enhance fibroblast cell activity, Increase inhibition of metalloproteinase-1, Upregulation of collagen, decrease the translocation of mitochondrial apoptosis | Ethanol | Leaves, Dried seeds | Psoralea corylifolia | 0.2 ml/day, 39 μM & 17.7 μM | 4 , 13 , 60 |
Antitumor & Hormone Therapy | Apoptosis in lung adenocarcinoma A549 cell line, DNA polymerase enzyme Inhibition, Brest Cancer cell proliferation inhibition & S phase arrest MCF-7, upregulation of ATM serine/threonine kinase, Inhibit the activation of hypoxia-inducible factor 1 | Phenolic, Ethanol | Seeds, dried ripe fruit | Psoralea corylifolia L. | 9.58± 1.12 μmol/l, 404 µM, >2 μg/mL | 12 , 65 , 66 |
Anti-oxidative effect | Preventing lipid peroxidation, reduces retinal degeneration, reduced ROS-induced apoptosis and Retinal Ganglion Cell death, reducing 4-Hydroxynonenal (4-HNE), 3-Nitrotyrosine (3-NT) oxidative stress, activating the SIRT1/Nrf2 pathway | Ethanol, methylene chloride, Ethanol & sterile saline, | Seeds | Psoralea corylifolia L. | 39 μM, 10 mM | 13 , 49 , 73 |
Anti-Viral | Inhibition of Influenza A and reducing viral mRNA expression, Activating, Nrf genes, NADPH oxidoreductase and Glutathione S-transferase, Suppression to NF-kB inflammatory pathway, Inhibition Covid entry and overexpressing human ACE2 | Ethanol | Seeds | Psoralea corylifolia L. | 25 μM, 100 μM, 40.7 μM | 15 , 86 |
Combination Effect | Inhibit skin photoaging with Vanilla tahitensis, Upregulates DR4 and DR5 | Water | Plant | Psoralea coryfliolia | 0.5 µg/mL | 10 , 98 |
Side effects
Bakuchiol is generally used in the cosmeceutical field as a more tolerable version of retinol, having retinol functionality through retinol-like regulation of gene expression. However, it may initially cause some redness and peeling in sensitive skin, 4 although chances are rare due to the established anti-inflammatory nature of bakuchiol. As it may increase cellular turnover, sunscreen is recommended for use after applying bakuchiol-containing products to reduce damage by UV radiation. Retinol and its derivatives are generally discouraged for use during pregnancy. No studies have evaluated use safety in pregnant women, so use should be carefully conducted. It is difficult to quantify bakuchiol usage’s benefits and side effects as most studies have been done in vitro, potentially introducing a risk of bias.
It should be mentioned that studies have found bakuchiol to be non-toxic to cell cultures even in high concentrations of up to 5000 uG/mL, 100 however, this was only observed in in vitro studies, and further studies are required to determine dosage toxicity. Recent clinical reports have indicated that treatment with Psoraleae Fructus (PF), an essential source of Bakuchiol, is associated with an increased risk of liver injury. 25 , 26 , 100 – 104 A study by Guo et al. (2021) indicated that bakuchiol, among other constituents of Psoraleae Fructus induced oxidative stress and mitochondrial damage-mediated apoptosis, alleviated when Ethanol extracts of PF were used. Bakuchiol may induce cholestatic hepatotoxicity as treatment with bakuchiol reduces mRNA expression of CYP7A1, HMG-CoA reductase, PPARα, and SREBP-2. 105
Care should be taken when using bakuchiol in combination therapy because it may cause an increase in cytotoxic effects of bakuchiol, and extensive studies should be conducted to ensure that metabolic toxicity does not occur. Bakuchiol can induce nephrotoxicity when it is used in combination with other natural ingredients, such as Glycyrrhetinic acid (GA) found in licorice, which inhibits the CYP450 isoenzymes (CYP3A4, CYP2C9, CYP1A2) involved in metabolic detoxification of bakuchiol. 106 The presence of GA altered the toxicokinetics of bakuchiol in rats, increased the internal exposure, suppressed the elimination of the bakuchiol prototype, and therefore may have enhanced the renal nephrotoxicity.
Toxicity
Toxicity was observed in a study in which bakuchiol and glycerrhizae redix et rhizome were orally adiministered to both male and female SD rats. Hence, bakuchiol was collected from Psoraleae fructus. The study comprised seven groups, which were treated with distill water, Glycerrhizae redix et rhizome, aristolochic group, bakuchiol group both male and female, and a combination of bakuchiol and Glycerrhizae redix et rhizome group both male and female. Bakuchiol was administered at a rate of 40 g/kg (-1), while the combined dose of both bakuchiol and Glycyrrhizae Radix et Rhizoma was administered at (40+20)g/kg(-1).
Similarly, a combined dose was delivered to a group of male and female rats. Plasma Bakuchiol concentration was measured thoroughly using HPLC-UV method at different time intervals after a single administration. Further, Alanine Transaminase, Aspartate aminotransferase, Blood urea nitrogen, Blood creatinine, N-acetyle-beta-glucoseamindase and kidney injury molecules were also assayed after 24 hours of administration. Toxicities were different according to gender. However, an obvious effect of toxicities while a combined dose of bakuchiol and Glycerrhizae redix et rhizome was administrated with a significant (p < 0.005) value. 107
Further, a study on bakuchiol metabolites using mass spectrometry and LC-MS/MS demonstrated the toxicity of Bakuchoiol. Following the oxidation, bakuchiol is bioactivated to ortho-quinone 3. In addition, cytochrome p450 catalyzes to epoxide. It has been found that all CYT p450 family enzymes are responsible for the bioactivation of bakuchiol into Catechol and perhaps ortho-quinone. In an experiment on animals, bakuchiol was dissolved into corn oil at 75g/kg dose. Subsequently, 100 μM was being used in microsomal assay. Catechol is responsible to alkylating in proteins and/or DNA including hepatotoxicity and carcinogenesis. Thus, bakuchiol is first metabolized to reactive intermediate by Cytochrome p450. 108
An experimental study on renal tubular cell lines HK-2 was carried out to estimate the cytotoxicity of both bakuchiol alone and combined with psoralen. The Study was divided into three groups: Psoralen, bakuchiol and combined bakuchiol with psroalen. Three groups were executed with different dose manner such as 5μmol/L for psoralen, 5, 10, 20, 30, 40 μmol/L for bakuchiol and (20, 30, 40) + 5 μmol/L for bakuchiol+Psoralen respectively. The viabilities were determined using MTT assay. Besides, the membrane injuries were confirmed by detecting the rate of LDH (lactate dehydrogenase) along with the morphological image. No cytotoxicity was found in psoralen. Meanwhile, the viability of HK-2 renal tubular cell lines exposed to both bakuchiol alone and combined with psoralen was reduced after respectively 4, 24, 48 and 72 hours. However, the IC 50 values of bakuchiol were calculated to (26.4±4.8), (21.8±0.6) and (24.1±0.8) μmol/L respectively for 24, 48 and 72-hour time intervals. Nevertheless, in the presence of Hepatic s9 mixture, the LDH release rate significantly increased in both vakuchiol and bakuchiol+psoralen. Despite that, the dose of bakuchiol 40 μmol/L as well as bakuchiol+Psoralen (20, 30, 40)+5 μmol/L showed an apoptotic nature in HK-2 renal tubular cell lines. The apoptotic nature increased and the cell G2 phase decreased in both bakuchiol and bakuchiol+psoralen doses. Moreover, the possible mechanism of the apoptotic and cytotoxic nature is whether direct damage to the cell membrane, inducing cell apoptosis or influencing cell mitosis with proliferation by inhibiting intracellular DNA synthesis. 109
Table 2. Experimental data of toxicity.
Bakuchiol Plant | Other compounds | Other Plant Name | Dose manner/IC50, LD50 value | Toxicity assayed | Method | Reference |
---|---|---|---|---|---|---|
Psoraleae fructus | Glycerrhizae redix et rhizome | Liquiritiae radix | (40+20)g/kg(-1) | ALT, AST, BUN, Cr, NAG, Kim-1 | HPLC-UV | 107 |
Psoralea corylifolia L. | N/A | N/A | 100 μM, 75 mg/kg | GSH (M1-M5), Cytotoxicity, Liver, CYP-1A2, Urinary excretion, Carcinogenesis | Mass Spectrometry, LC-MS/MS | 108 |
Psoralea corylifolia L. | Psoralen | Psoralea | 5,10,20,30,40μmol/L, (20,30,40)+5 μmol/L | Cell membrane Damage, Apoptosis, Intracellular DNA synthesis inhibition | LDH release rate, Contrast Microscope | 109 |
Conclusions and future research
This review focused on the pharmacological benefits of the compound bakuchiol, traditionally isolated from the bakuchi plant and used in traditional medicine for centuries. Recent studies have highlighted its vital role in controlling several activities that lead to health depreciation and the onset of various non-communicable diseases. Additionally, bakuchiol has shown potent antimicrobial and antiviral responses against various pathogens in multiple studies, which allows for the development of potential novel cures and preventive strategies.
Moreover, toxic reports are more with a view to non-toxic bioactivity. As mentioned earlier, the combined doses of Psorlen and Glycerrhizae redix et rhizome have lethal, but the minimum effective and toxic doses is quite unclear. Further, it is important to discover a scientific method to reduce the toxic effect(s) while increasing the pharmacological effect. Further, most of the combination therapies are found to be toxic from the result of this study. Despite that, the result of combined and bakuchiol alone exhibited nonsimilar results. Yet, it is implicit that the mechanism of bakuchiol before and after application.
Moreover, an important study on the mechanism and chemical composition before and after combined therapy can be studied. Thus, extensive research is required on the non-toxic extraction of the compounds, fully realizing its pharmacological and biochemical modes of action, and planning for sustainable ways of growing its sources to meet the increasing demands of the pharmaceutical industries. Further studies should also be done to evaluate the long-term effects of prolonged bakuchiol consumption, possibly via retrospective analyses, which have not been done yet.
However, following the chemical structure of bakuchiol, it appears that a single functional group (OH) is present and actively supporting the compound. In addition, it is composed of both linear chains and cyclic compounds. Therefore, extensive studies can enhance the comprehension of reducing the toxic effects of bakuchiol in combined doses with other compounds. In that case, medicinal chemistry, clinical trials, and bioinformatics can become essential.
Funding Statement
The author(s) declared that no grants were involved in supporting this work.
[version 2; peer review: 2 approved]
Data availability
No data are associated with this article.
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