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A systematic review on antimicrobial activities of green synthesised Selaginella silver nanoparticles

Published online by Cambridge University Press:  03 August 2023

Khushbu Wadhwa
Affiliation:
Ramjas College, University of Delhi, Delhi, India
Hardeep Kaur*
Affiliation:
Ramjas College, University of Delhi, Delhi, India
Neha Kapoor
Affiliation:
Hindu College, University of Delhi, Delhi, India
Soma M. Ghorai
Affiliation:
Hindu College, University of Delhi, Delhi, India
Renu Gupta
Affiliation:
Ramjas College, University of Delhi, Delhi, India
Arunima Sahgal
Affiliation:
Ramjas College, University of Delhi, Delhi, India
*
Corresponding author: Hardeep Kaur; Email: hardeepkaur@ramjas.du.ac.in
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Abstract

Background

Metallic nanoparticles from different natural sources exhibit superior therapeutic options as compared to the conventional methods. Selaginella species have attracted special attention of researchers worldwide due to the presence of bioactive molecules such as flavonoids, biflavonoids, triterpenes, steroids, saponins, tannins and other secondary metabolites that exhibit antimicrobial, antiplasmodial, anticancer and anti-inflammatory activities. Environment friendly green synthesised silver nanoparticles from Selaginella species provide viable, safe and efficient treatment against different fungal pathogens.

Objective

This systematic review aims to summarise the literature pertaining to superior antifungal ability of green synthesised silver nanoparticles using plant extracts of Selaginella spp. in comparison to both aqueous and ethanolic raw plant extracts by electronically collecting articles from databases.

Methods

The recommendations of the Preferred Reporting Items for Systematic Reviews and Meta-Analysis were taken into consideration while preparing this review. The titles and abstracts of the collected data were stored in Endnote20 based on the inclusion and exclusion criteria. The search strategy included literature from established sources like PubMed, Google Scholar and Retrieval System Online using subject descriptors.

Results

The search yielded 60 articles with unique hits. After removal of duplications, 46 articles were identified, 40 were assessed and only seven articles were chosen and included in this review based on our eligibility criteria.

Conclusion

The physicochemical and preliminary phytochemical investigations of Selaginella suggest higher drug potency of nanoparticles synthesised from plant extract against different diseases as compared to aqueous and ethanolic plant extracts. The study holds great promise as the synthesis of nanoparticles involves low energy consumption, minimal technology and least toxic effects.

Type
Review
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
Copyright © The Author(s), 2023. Published by Cambridge University Press

Introduction

Traditional herbal medicines exhibit great importance and are now being increasingly re-evaluated all over the world to determine their efficacy for the safer development of drug against different diseases. The heterosporous fern genus Selaginella is very rich in species (over 700), and is mainly found in the warm and moist climate having a worldwide distribution (Ref. Reference Weng and Noel1). The desiccation-tolerant Selaginella bryopteris (L.) Bak. is an Indian resurrection and medicinal plant (Ref. Reference Pandey2). It belongs to the family Selaginellaceae and is commonly called ‘Sanjeevani’ for its therapeutic properties (Ref. Reference Ganeshaiah, Vasudeva and Shaanker3). Selaginella bryopteris is found in the hilly terrain of Bihar, Jharkhand and Uttar-Pradesh. During monsoon season, it acquires a green appearance, while in dry season it undergoes extreme desiccation and revives only with return of favourable conditions, thus exhibiting resurrection capabilities. Most species of Selaginella however tolerate severe drought conditions due to the presence of trehalose; a disaccharide that provides structural and functional stability. In Indian folklore, S. bryopteris is reported to be a traditional herbal drug and considered as a tonic for revitalisation. The anti-cancer effect of S. bryopteris was determined in vitro against human hepatocellular carcinoma HepG2 cell line (Ref. Reference Pal4). Many other species of Selaginella are well documented as Chinese traditional medicines such as Selaginella doederleinii Hieron. and Selaginella pulvinata (Hook. & Grev.) Maxim and are used to treat nasopharyngeal carcinoma and oesophageal cancer. Another herbal medicine found in China, Selaginella tamariscina (Beauv.) Spring, contains selaginellin derivatives that are rarely found in nature. However, clinical applications of S. pulvinata, were found to be very similar to those of S. tamariscina. Selaginellins are a small group of pigments that are exclusively found in the genus Selaginella. Since the first report of selaginellin from Selaginella sinensis (Desv.) Springs in 2007, more than 110 selaginellins, with different types of polyphenolic compounds, have been reported. Further, the secondary metabolites of resurrection plant species have also received special attention in the field of biotechnology and medicine. The major natural phytocompounds in the genus Selaginella are characteristic flavonoid-dimers (biflavonoids). The biflavonoids isolated from S. tamariscina show anti-inflammatory activity on lipopolysaccharide (LPS)-induced murine macrophages and colon epithelial cells (Ref. Reference Shim, Lee and Lee5). Besides this, the use of S. tamariscina ethanol extract (STE) against glutamate-induced oxidative stress and neuronal cell death by controlling autophagy in a mouse hippocampal neuron cell line has also been reported (Ref. Reference Jeong6). One of the earliest reported articles on pharmacognostical studies of Indian Selaginella spp. was done by our group where we showed antimicrobial properties of its extracts (Ref. Reference Saxena, Kaur and Kapoor7). Thereafter, our team worked on the synthesis of Selaginella silver nanoparticles by green method and observed much better antimicrobial properties in comparison to its raw extract (Ref. Reference Yadav, Kapoor and Ghorai8). Biosynthesised nanoparticles hold special mention in the category of phytomedicine due to their ease of production, lower cost, least toxicity and ecofriendly nature. To understand the superior antimicrobial potency of nano-formulations of Selaginella, identification of the early diagnostic markers and therapeutic targets is the primary step. This systematic review was hence designed to make a clear distinction between the competences of raw extract of Selaginella viz a viz the nano-drug prepared from its extract. We also propose that Selaginella nanoparticles might have a wide range of applications not only as anti-microbial drugs but also in the conservation of environment. Our claim is further substantiated by certain recent studies wherein green synthesised nanoparticles from Selaginella have shown excellent antimicrobial, anticoagulant and antiplatelet activities (Ref. Reference Dakshayani9).

Materials and methods

This systematic literature review was conducted according to the recommendations of the Preferred Reporting Items for Systematic Reviews and Meta-Analysis guidelines.

Search strategy

A search was performed using Google Scholar, Medline, Scopus and PubMed databases. The combination of the following keywords were selected and used for the search: Selaginella derived nanoparticles, bio efficacy of silver nanoparticles and phytochemistry of genus Selaginella. Articles that might be missed during various database searches were identified from the reference list of articles that were retrieved from initial search and were added to the list of selected articles.

Eligibility criteria

Articles, titles and abstracts of literature paper were manually screened to exclude the data not related to the study. Relevant articles were studied to determine the eligibility criteria of this review. The following inclusion criteria were applied to select the studies: (1) only articles written in English; (2) observational original studies; (3) studies on Selaginella derived nanoparticles; (4) studies representing the bio-efficacy of nanoparticles derived from Selaginella; (5) studies that presented the aqueous and alcoholic extract of Selaginella and their various activities. The exclusion criteria were based on (1) general reviews on resurrection plants; (2) clinical reports and case studies; (3) book chapters, news, conference proceedings and editorial letters.

Experimental

Study selection and data collection

The identification of eligible criteria was performed by reading the titles and abstracts. The screening was performed by all the authors independently. The eligible full articles were then read by the authors and the inclusion and exclusion criteria were applied again. The included articles were determined by consensus among the authors and were critically appraised to assess the quality of the studies. The following data were extracted from the included articles: authors, year of publication, study design, bio-efficacy of Selaginella species, chemical extracts of Selaginella and its pharmaceutics, chemistry of various bioactive compounds in the extracts, Selaginella-derived nanoparticles and their bio-efficacy as targeted drug delivery agents (Table 1).

Table 1. Reference articles selected for study and data collection

Data analysis

Microsoft Excel was used to tabulate the collected data. Various Selaginella species were classified according to their usage as traditional drugs in the Indo-pacific part of the world; mainly India, China, Sri Lanka and Indonesia (Table 2). In order to answer the objectives of this systematic review, a ‘directly proportional’ relationship was considered when the correlation analyses were positive, demonstrating the advantage of nano-synthesis of Selaginella over raw extracts. On the other hand, they were considered ‘inversely proportional’ when the correlation analyses were negative, that is, when very few reports (only three) were found for bio-efficacy of S. bryopteris nanoparticles, and the rest were for raw extracts that possess poor solubility and bioavailability capabilities. Eligible articles were analysed in detail using the content analysis method without any statistical tests.

Table 2. Summary of various Selaginella spp. and their important natural bioactive compounds found in different parts of the world

This particular research article mentions the strain name as S. convolute (Ref. Reference Xu33).

Results

The literature search identified a total of 46 articles in the Google Scholar, Medline, Scopus and PubMed databases that pertain to Selaginella spp. as medicinal plant, wherein S. bryopteris is an Indian medicinal plant. Among these 46 articles, 40 were eligible for reading the title and summary. Thirty articles showed differing bio-efficacy of raw extract of Selaginella but did not show results for our designed study. Therefore, a total of seven articles were included in this systematic review (Fig. 1). These seven articles were published between 2016 and 2020. All articles were observational cross-sectional studies and the methodological quality analyses indicated that 57.14% (n = 4) of the studies were considered with low risk of bias; and 42.86% (n = 3) were considered with medium/moderate risk of bias (Table 3). These seven articles also show different types of nanoparticles derived from various species of Selaginella such as S. doederleinii Hieron., Selaginella myosurus (SW.) Alston, Selaginella convoluta (Arn.) Spring and S. bryopteris (L.) Bak. (Refs Reference Yadav, Kapoor and Ghorai8, Reference Dakshayani9, Reference Biswas32, Reference Xu33, Reference Zhao34, Reference Juniarti35, Reference Kedi36). Nanoparticles derived from these species of Selaginella plant exhibited anti-cancer, anti-inflammatory, antimicrobial, anticoagulant, antiplatelet activities and also help in the management of pain. Only three articles clearly depicted the bio-efficacies shown by nanoparticles derived from S. bryopteris. Out of ten, three articles described the commercially marketed nanodrugs of Selaginella.

Figure 1. Flow diagram summarising systematic search and study selection.

Table 3. Characteristics of the seven articles included in this study

Discussion

This Study performed an analysis of the correlation between the bio-efficiency of nano-formulation derived from natural sources over the raw extracts from microbes. It lists and documents all the studies that have been done to characterise Selaginella derived natural phytochemicals with specific activities both as raw extracts as well as nano-formulations (Ref. Reference Yu40). This study therefore provides an insight regarding future drug development where natural products can be explored as alternate medicines in many diseased conditions.

Antimicrobial action of Selaginella extract

The compounds isolated from Selaginella belong to a wide class of alkaloids, benzenoids, chromones, coumarins, flavonoids, lignans, oxygen heterocycle, phenylpropanoids, pigments, quinoids, steroids, secolignans, neolignans and caffeoyl derivatives. The research on S. pulvinata extract revealed the presence of selaginellin derivatives, namely selaginellin G and selaginellin H, together with the biflavonoids and flavonoids. The presence of unique acetylene bond and p-quinone-methide functionalities in the selaginellin derivatives represents a rare group of naturally occurring phenolic compounds (Ref. Reference Cao10). The Chinese medicinal plant, S. tamariscina contains a novel biflavonoid named isocryptomerin that exhibits antifungal and antibacterial activities on human pathogens, without any haemolytic effect on human erythrocytes (Ref. Reference Lee16). Few others like S. tamariscina and S. pulvinata are very useful to promote blood circulation, while S. doederleinii is used as an antibacterial agent and to cure cardiovascular diseases. The antifungal effect of amentoflavone, another compound extracted from S. tamariscina, has paved the way for scientists to explore the antimicrobial properties in S. bryopteris, against bacterial and fungal pathogens such as Staphylococcus aureus and Candida albicans.

Antioxidant, anti-inflammatory, anticancer and cardio and neuro-protective role of Selaginella extract

In recent years, medicinal plants have received more attention owing to their pharmacological profile and easy availability to common people. Hepatocellular carcinoma (HCC) is considered as most common and leading cause of cancer-related mortality worldwide. The anti-cancer effect of S. bryopteris was evaluated by Pal et al. (Ref. Reference Pal4), using a human hepatocellular carcinoma HepG2 cell line. Gas chromatography-mass spectrometry (GC-MS) was performed to analyse the phytochemicals present in S. bryopteris extract (SBE). The major bioactive phytocompounds identified by GC-MS were imidazole, amentoflavone, gallic acid, catechine, palmitic acid, lupeol, L-fucitol and myo-inositol. The anti-proliferative activity of SBE was evaluated by using MTT assay and further determined by change in the mitochondrial membrane potential, reactive oxygen species (ROS generation) and alteration in nuclear morphology (Fig. 2). A study by Jeong et al. (Ref. Reference Jeong6) have demonstrated the role of STE in inhibiting autophagy that may be useful for preventing and treating neurodegenerative diseases. Oxidative stress due to excessive production of ROS is considered as major cause of neurodegenerative disorders, including Parkinson's disease, Alzheimer's disease and cerebral ischemia. Prolonged oxidative stress leads to autophagy process that further results in autophagic cell death in the neuronal system. Administration of STE extract decreases the glutamate-induced cytotoxicity in HT22 cells via inhibition of ROS production and apoptosis (Ref. Reference Jeong6).

Figure 2. Schematic representation of the progression of cancer in human liver tissue.

S. tamariscina has been used for the treatment of dysmenorrhoea, amenorrhoea, haematuria, chronic hepatitis and hyperglycaemia. The study by Shim et al. (Ref. Reference Shim, Lee and Lee5) demonstrated the anti-inflammatory activity of two biflavonoid compound called as Hinokiflavone (H) and 7′-O-methylhinokiflavone (mH). They also examined their activity in LPS-mediated murine macrophages (RAW 264.7) and colon epithelial cells (HT-29). Both H and mH can suppress the production of LPS-induced expression of inducible nitric oxide synthase (iNOS) and cyclooxygenase (COX-2) and can lead to activation of nuclear factor-κB (NF-κB) and extracellular regulated kinases (ERK), thus inhibiting inflammation (Fig. 3).

Figure 3. Schematic representation of the anti-inflammatory effect of S. tamariscina phytochemicals against cyclooxygenase enzymes; Cyclooxygenase 1 (COX1), Cyclooxygenase 2 (COX2).

A study by Adnan, et al. (Ref. Reference Adnan17) has demonstrated the phytochemistry of S. repanda (Desv. & Poir.) Spring. ethanolic crude extract using Ultra High Performance Liquid Chromatography–PDA detector mass spectrophotometer. The study has revealed the presence of various phenols such as chlorogenic acid, 7-hydroxycoumarine, 2-amino-1,3,4-octadecanetriol, 4-coumaric acid, 4-methoxy cinnamic acid, caffeic acid, coumarin, isoferulic acid and formononetin. The flavonoids compounds identified in this study are rutin, apigenin, vitexin, genistein, glycitin, luteolin, rhamnetin, kaempferol, diosmetin, quercetin, quercetin-3β-D-glucoside and glycitein. The identified phytochemicals exhibit therapeutic applications including antioxidant, anti-inflammatory, anticancer and cardio-protective effects.

A study by Muema et al. (Ref. Reference Muema41) has evaluated the anti-proliferative activities of both Dichloromethane (DCM) and ethyl-acetate (EA) extract of S. doederleinii on three cancer cell lines HT-29, He-La and A549 at different concentration ranging from 12.5 to 200 μg/ml. The EA fraction exhibited anti-proliferative activity against the HT-29, He-La cell lines by inhibiting the cell growth rate in a dose-dependent manner with IC50 values of 55.6 ± 1.3 and 69.2 ± 1.3 μg/ml, while the DCM fraction exhibited the activity against A549 cell line with an IC50 value of 55.9 ± 12.6 μg/ml. Furthermore, phytochemical investigation of DCM extracts has led to the identification of 7″-methyl ether tetrahydrohinokiflavone that exhibited the strongest activity against all three cell lines by inhibiting the cell growth rate in a dose-dependent manner.

Role of green synthesised nanoparticles from Selaginella

Among the articles in literature, many provide strong evidence of therapeutic and medicinal value of Selaginella and show a directly proportional interaction between raw extracts and their bio-efficacy with respect to antimicrobial and anti-inflammatory properties. On the other hand, very few articles showed that silver nanoparticles synthesised from the plant extract of Selaginella exhibits enormous therapeutic applications. The plant extract of Selaginella acts as a capping and reducing agent (Ref. Reference Dakshayani9). Besides containing various secondary metabolites such as carbohydrates, chromones, flavonoids, steroids, quinoids, lignans, the raw extract of Selaginella also contains functional organic groups like -OH, -COOH, C-C, C-O containing coumarins (Ref. Reference Setyawan11). These secondary metabolites exhibit ligation properties by binding to metal ions and get reduced to form metal nanoparticles. For the green synthesis and determination of cytotoxicity of silver nanoparticles, several factors must be considered including chemical composition, surface chemistry, size and its distribution, coating/capping, agglomeration, dissolution rate, particle morphology and reactivity in solution, efficiency of ion release and the type of reducing agents (Ref. Reference Vanlalveni42).

The small number of screened articles evaluated the antimicrobial activity of Selaginella-derived silver nanoparticles by using agar disc-diffusion methods against bacterial and fungal pathogens. To study the antimicrobial activity of SPE-Ag-NPs (Selaginella plant extract Ag-NPs), Ciprofloxacin and Amphotericin B were used as standard drugs and these nanoparticles were examined by measuring the diameter of the zone of inhibition around each well (Ref. Reference Biswas32). The zone of inhibition and MIC values were determined for plant extract as well as for crude compounds against the gram-positive and gram-negative bacteria and also against Candida species (Ref. Reference Verma18). The radial growth inhibition zone exhibited an increase with enhanced concentration of SPE-AgNPs, thus evincing their potent antimicrobial activity as compared to the raw extracts from Selaginella or the traditionally used drugs.

The articles included in this systematic review also analysed the functional capability of other nanoparticles, such as Zinc oxide derived nanoparticles (ZnO NPs) – which demonstrate considerable biological activities. The ZnO NPs prepared from leaf extracts of S. convoluta show good potency as anti-nociceptive and a muscle relaxant, thus holding promise in pain management as an emerging nursing care in the future (Ref. Reference Xu33). Also, articles were included which demonstrated that nanoparticles synthesised by charcoal processing of S. tamariscina, called S. tamariscina carbonisatus (STC), act as a type of calcined herb-drug to promote haemostasis. The effects of STC-NPs showed low toxicity in the hemorheological and coagulation systems and can be a promising candidate for biological application. This haemostatic effect of STC-NPs suggests a new approach for the development of therapeutic drugs that can be used in the management of haemorrhagic diseases (Ref. Reference Zhao34). It has also been reported that nanoparticles synthesised from S. doederleinii possesses anti-cancer activity due to the presence of phytochemical compounds, especially flavonoids such as flavones (apigenin) and flavonones (naringenin) (Ref. Reference Juniarti35). Additionally, silver nanoparticles synthesised from S. myosurus by green, novel and environmentally friendly pathway exhibit an anti-inflammatory activity by inhibiting the denaturation of albumin protein; which is the major cause of tissue damage in arthritic reactions during inflammation (Ref. Reference Kedi36).

Drug delivery system for better action of bio-formulations

Few articles were worth considering for their reference of drug delivery systems especially through the oral route owing to the safety and simplicity of their administration. Nevertheless, several new formulations such as liposomes, nanoparticles, self-nano emulsifying drug delivery systems and solid dispersions are recommended to enhance the aqueous solubility and oral bioavailability of some compounds. Among these preparations, solid dispersion is one of the most fascinating formulations that improve drug release, enhance gastrointestinal absorption and oral bioavailability (Ref. Reference Mitragotri, Burke and Langer43). Amorphous solid dispersions (ASDs) are defined as molecular mixtures of hydrophobic drugs with a hydrophilic carrier that can provide more solubility over the crystalline form (Ref. Reference Li and Taylor44). ASDs are generally prepared from polymers, specifically a hydrophobic polymer that is capable of inhibiting drug crystallisation and helping in better drug release. Hinokiflavone (HF), a biflavonoid isolated from the medicinal plant S. tamariscina (Ref. Reference Zhang12) has been shown to have antitumor capacity but possesses poor solubility and low bioavailability that restricts its use for medicinal purposes. To overcome these challenges, Polyvinyl caprolactam-polyvinyl acetate-polyethylene glycol (Soluplus®) is used which is an amphiphilic polymer that has the capacity to increase the solubility of hydrophobic drugs. This polymer helps in the formation of a micellar-like structure in a solution having a low critical micelle concentration (CMC). The molecular structure of Soluplus contains a hydrophilic portion of polyethylene glycol backbone and a hydrophobic portion of ethylene caprolactam/vinyl acetate side chain (Ref. Reference Bernabeu37). The use of D-α-Tocopherol acid polyethylene glycol 1000 succinate (TPGS), the derivative of vitamin E, a non-ionic surfactant containing the hydrophilic head and lipophilic tail helps to improve drug solubility and drug encapsulation efficiency. The physicochemical properties of HF hybrid micelles are investigated including particle size, zeta potential, encapsulation efficiency, drug loading, CMC value and stability. Nevertheless, HF hybrid micelles exhibit improved anticancer activity and induce mitochondrial-mediated apoptosis by increasing the levels of ROS. They may be considered as a potential drug delivery system for the treatment of lung adenocarcinoma (Ref. Reference Chen38). Similarly, amentoflavone, robustaflavone, 2″,3″-dihydro-3′,3″′-biapigenin, 3′,3″′-binaringenein and delicaflavone are the five major components in the total biflavonoid extract from S. doederleinii (TBESD) that display anticancer properties. To ameliorate the solubility, dissolution rate and bioavailability of TBESD, a new oral drug delivery formulation has been made with the help of a solid dispersion technique. TBESD amorphous solid dispersion (TBESD-ASD) with polyvinylpyrrolidone K-30 was prepared by using the solvent evaporation technique which showed higher solubility and dissolution rates as compared to raw TBESD (Ref. Reference Chen39) and hence can prove to be a good promising chemotherapeutic agent for cancer treatment.

The solid dispersion nanoparticles with better dissolution and oral bioavailability might therefore prove to be a revolutionary drug delivery system with much better technological advantage as compared to conventional delivery systems.

Limitation: As is true for any research, this systematic review is not without limitations. There is publication bias that must be understood as certain articles (grey literature) were not included. The systematic review clearly has a language bias wherein the articles published in English language were only included. However the systematic review presented here gives a very affirmative role to nanoparticles as potent antimicrobial agents. Hence, this review can serve as a guide towards improving antimicrobial strategy with minimal toxicity.

Conclusion

The study shows that many species of the genus Selaginella are a rich source of various bioactive compounds like flavonoids and biflavonoids. Flavones such as apigenin, luteolin and diosmetin are ubiquitously found in many other popular plant species (Ref. Reference Harborne45), including Selaginella spp. Specific flavonoids such as amentoflavone are also found to be potent antifungal agent (Ref. Reference Hwang46). All the above-mentioned flavones found in Selaginella spp are known to possess anticancer, antimicrobial, anti-inflammatory and many other pharma nutraceutical properties. However, very few articles have emphasised the superior role of nano-formulations made from the raw extracts of Selaginella. Nevertheless, the review of such articles has been very promising highlighting a much better antimicrobial activity of nanoparticles over raw extract. Still more research is needed to further explore the mechanism of action of these compounds and their bioactivities. Nanoparticles synthesised from Selaginella hold promise not only in clinics and pharmaceutics but also in other fields like restoration of old heritage buildings and conservation of environment. Since, Selaginella AgNPs are an efficient anti-microbial and anti-fungal agent; they may be used to remove the fungal and algal growths over the monuments that are responsible for their rapid degradation. Selaginella silver nanoparticles can also be explored in cleaning water ecosystems, wetlands and other ecologically dynamic systems. The chemical and physical methods used for extractions of phytochemicals from Selaginella for its use as medicine involves production of many effluents that are ecologically harmful. Management of such processes for the potential risks needs deeper understanding to improve both nature and human lives. With better knowledge of the alternative synthesis methods, it would be possible to have the same drug quality of Selaginella, with minimal environmental hazards. Therefore, understanding the procedure that involves greener ways of drug synthesis with improved drug delivery system in the form of nano-formulations, as highlighted in this review, is critical. These findings may be utilised to improve the synthesis of nano-drugs from different Selaginella species which entails low cost, minimal technology, less harmful effluents and better drug efficacy.

Acknowledgements

All the authors contributed equally to literature search and analysis of the data. SMG and HK designed and coordinated the study. KW, NK, SMG, RG, AS, HK wrote the article and contributed equally to final version of the manuscript.

Financial support

No funding was utilised in the preparation of this systematic review

Competing interest

None.

Ethical standards

Approval was not required.

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Figure 0

Table 1. Reference articles selected for study and data collection

Figure 1

Table 2. Summary of various Selaginella spp. and their important natural bioactive compounds found in different parts of the world

Figure 2

Figure 1. Flow diagram summarising systematic search and study selection.

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Table 3. Characteristics of the seven articles included in this study

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Figure 2. Schematic representation of the progression of cancer in human liver tissue.

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Figure 3. Schematic representation of the anti-inflammatory effect of S. tamariscina phytochemicals against cyclooxygenase enzymes; Cyclooxygenase 1 (COX1), Cyclooxygenase 2 (COX2).