Skip to main content
PMC home page
SpringerPlus logoLink to SpringerPlus
. 2013 Jul 31;2:363. doi: 10.1186/2193-1801-2-363

Antibacterial activities of the methanol extracts of seven Cameroonian dietary plants against bacteria expressing MDR phenotypes

Jackson A Seukep 1, Aimé G Fankam 1, Doriane E Djeussi 1, Igor K Voukeng 1, Simplice B Tankeo 1, Jaurès AK Noumdem 1, Antoine HLN Kuete 2, Victor Kuete 1,
PMCID: PMC3738912  PMID: 23961425

Abstract

The morbidity and mortality caused by bacterial infections significantly increased with resistance to commonly used antibiotics. This is partially due to the activation of efflux pumps in Gram-negative bacteria. The present work designed to assess the in vitro antibacterial activities of seven Cameroonian dietary plants (Sesamum indicum, Sesamum radiatum, Cinnamomum zeylanicum, Corchous olitorius, Cyperus esculentus, Adansonia digitata, Aframomum kayserianum), against multidrug resistant (MDR) Gram-negative bacteria over expressing active efflux pumps. The standard phytochemical methods were used to detect the main classes of secondary metabolites in the extracts. The antibacterial activities of the studied extracts in the absence or presence of an efflux pump inhibitor (PAβN) were evaluated using liquid microbroth dilution method. The results obtained indicated that apart from the extract of C. esculentus, all other samples contained alkaloids, phenols and polyphenols meanwhile other classes of chemicals were selectively present. The studied extracts displayed antibacterial activities with minimal inhibitory concentrations (MICs) values ranged from 64 to 1024 μg/mL on the majority of the 27 tested microbial strains. The extract of S. indicum was active against 77.77% of the tested microorganisms whilst the lowest MIC value (64 μg/mL) was recorded with that of A. kayserianum against E. aerogenes EA294. The results of the present work provide baseline information on the possible used of the tested Cameroonian dietary plants in the treatment of bacterial infections including multi-drug resistant phenotypes.

Keywords: Antibacterial activity, Cameroon, Dietary plants, Efflux pumps, Gram-negative bacteria, Multi-drug resistant

Introduction

The continuous emergence of multidrug-resistant (MDR) bacteria drastically reduces the efficacy of our antibiotic armory, and consequently increases the frequency of therapeutic failure Falagas and Bliziotis (2007). The resistance of bacteria to chemically unrelated antimicrobial agents may be associated with the over-expression of efflux pumps (Poole 2004 Li and Nikaido 2009). In Gram-negative bacteria, many of these efflux pumps belong to the resistance-nodulation-cell division (RND) family of tripartite efflux pumps. Among those efflux pumps, those belonging to the AcrAB-TolC family are detected in many clinical bacterial isolates and are reported to be a key factor in the expression of the MDR phenotypes (Mallea et al. 2003; Lomovskaya et al. 2004). This efflux pumps mechanism can be blocked by various inhibitors which restore the intracellular concentration as well as the activities of the antibiotics (Chollet et al. 2004; Pagès and Amaral 2009). The scarcity of original synthetic antibiotics has stimulated the search for new antibacterial agents from medicinal plants. This explains our endeavor to evaluate in vitro the antibacterial activities of Cameroonian dietary plants namely the beans of Sesamum indicum, the stem and leaves of Sesamum radiatum, Corchous olitorius and Cyperus esculentus, the bark of Cinnamomum zeylanicum, the fruits of Adansonia digitata and Aframomum kayserianum against Gram-negative bacteria expressing MDR phenotypes. The role of efflux pumps in the activity of our plants extracts was also investigated using a previously described efflux pump inhibitor.

Material and methods

Plant materials and extraction

The seven edible plants used in this work were purchased from Bafoussam local market, West Region of Cameroon in January 2012. The collected plant samples were the beans of Sesamum indicum, the stem and leaves of Sesamum radiatum, Corchous olitorius and Cyperus esculentus, the bark of Cinnamomum zeylanicum, the fruits of Adansonia digitata and Aframomum kayserianum. The plants were further identified at the National Herbarium (Yaoundé, Cameroon) where voucher specimens were deposited under a reference number (Table 1). The powdered air-dried sample from each plant was extracted with methanol for 48 h at room temperature. The extract was then concentrated under reduced pressure to give a residue that constituted the crude extract. They were then kept under 4°C until further use.

Table 1.

Plants used in the present study and evidence of their activities

Plants samples, part used
and herbarium voucher numbera 		Traditional used Known antimicrobial activities of plants
Bombaceae Adansonia digitata (Fruits) 42417/HNC Febrifuge, antidysentery, antioxydant, analgesic, antidiarrheal (Kaboré et al. 2011); immunostimulant, hepatoprotective (Al-Qarawi et al. 2010); anti-small pox, anti-rubella (Wickens 1979). Aqueous, ethanol and petroleum ether extracts Q : Ec (Yagoub 2008). Antiviral activity against Vi, Vhs (Vimalanathan and Hudson 2009), Vp (Anani et al. 2000).
Cyperaceae Cyperus esculentus (Fruits)14977/SRFC (/)b (/)
Pedaliaceae Sesamum indicum (Beans) 42898/HNC Liniment, laxative, emollient (Kokate et al. 2005); lenitif, anticonstipation, anti-carries (Awobajo et al. 2009), antitumor (Xu et al. 2010), hepatoprotective (Kumar et al. 2011), hypoglycemic (Nakano and Kwak 2006). (/)
Lauraceae Cinnamomum zeylanicum. (Bark) Blume 22309/SRFC Digestive disorders, anti dysentery, laxative. Isolated compounds (Cinnamaldehyde and Eugenol) from essential oil showed an activity: against Pl (Gende et al. 2008) ; antibacterial activities against multi-resistant Gram-negative bacteria (Pa, PS, Kp, EC., Ea, Ecl) (Voukeng et al. 2012)
Tiliaceae Corchous olitorius (Stem and leaves) 14725/SRFC Gonorrhoea, cystitis chronic, analgesic, febrifuge, antitumor, anti-inflammatory (Zacharia et al. 2006; Ramadevi and Ganapaty 2011), diuretic, cardiotonic (Ramadevi and Ganapaty 2011). Methanol, chloroform and petroleum ether extracts. S: Bs, Pa, Sm. F: Sa, Ec, La, ML, San, Sau, Kp. M: Ea, Pv. Q: Rs, Ca (Ramadevi and Ganapaty 2011), Ec Zacharia et al. (2006) Sau Bp, St, Sb, Ss, Sd,Pa, Kp, Ec,Vc Pal et al. (2006).
Pedaliaceae Sesamum radiatum Schum et Thom (Stem and leaves) 8797/SRFC Antirhume, anticatarrate, against ocular pains and cutaneous eruptions (Bankole et al. 2007), antimicrobial (Shittu et al. 2007; Osibote et al. 2010). Methanol and ethanol extracts S : Ca (Shittu et al. 2007). Essential oil :Q: Csp. Ec, Ec ATCC 25922, Kp, Pm, Pa, Sal, Sa, Sm Tane et al. (2005).
Zingiberaceae Aframomum kayserianum (Fruits) K.schum 18884/SRFC Anti-mumps, dysmenorrhoeas, vermifuge (Tane et al. 2005). Isolated compound Aframodial from this plant showed an activity: S : Sc, Sp,Ha, Cu, Scl, Pc.; M : Mm, Rc, An, Sau, Bs. F : Ec, Pa (Ayafor et al. 1994).
Open in a new tab

a(HNC), Cameroon National Herbarium; (SRF), Société des reserves forestière du Cameroun; b(/). Not reported. Screened Activity: Significant (S:MIC < 100 μg/mL), moderate (M: 100 < MIC ≤ 625 μg/mL), Weak (F:MIC > 625 μg/mL) (Kuete 2010), Q, qualitative activity based on the determination of the inhibition zone. Ca Candida albicans, St Salmonella typhi, An Aspergilus nicfer, Bs Bacillus subtilis, EC Escherichia coli, Kp Klebsiella pneumoniae, Pa Pseudomonas aeruginosa, Pvt Proteus vulgaris, Sau Staphylococcus aureus, Cu Candida utilis, Sc Saccharomyces cereviciae, Sm Streptococcus mutans, Sa Streptococcus aeoginosa, La Lactobacillus acidophillus, ML Micrococcus luteus, San Streptococcus anginosus, Ea Enterobacter aerogenes, Rs Rhizoctonia solanic, Bp Bacillus punilus, Sb Shigella boydii, Ss Shigella sonnei, Sd Shigella dysenteria, Vc Vibrio cholerae, Csp Citrobacter sp, Pm Proteus mirabilis, Sal Staphylococcus albus, Sma Serratia marcescens, Sp Schizosaccharomyces pombe, Ha Hansenula anomala, Scl Sclerotinia libertiana, PC Penicillim crustasum, Mm Mucor mucedo, Rc Rhizopus chinensis, Ecl Enterobacter cloacae, PS Providencia stuartii, Pl Paenibacillus larvae,Vhs herpes simplex virus,Vp Virus of poliomyelitis, VI Influenza. Virus.

Preliminary phytochemical investigations

The presence of major secondary metabolite classes, namely, alkaloids, flavonoids, phenols, saponins, tannins, anthocyanins, anthraquinones, sterol, and triterpenes (Table 2) was determined using common phytochemical methods Harbone (1973).

Table 2.

Bacterial strains and features

Bacteria Features References
Escherichia coli
ATCC8739 Reference strain of Escherichia coli
ATCC10536 Reference strain of Escherichia coli
W3110 Wild-type E. coli K-12 (Bagliomi et al. 2003)
MC4100 Wild-type E. coli K-12 , KANR (Martina 2002)
AG100A AG100 ΔacrAB::KANR (Monks et al. 1992; Okusu et al. 1996; Pradel and Pagès 2002)
AG100Atet ΔacrAB mutant AG100, owing acrF gene markedly overexpressed; TETR Monks et al. (1992)
AG102 ΔacrAB mutant AG100 Chevalier et al. (2000)
AG100 Wild-type E. coli K-12 Lorenzi et al. (2009)
E. aerugenes
ATCC13048 Reference strain
EA294 EA 289 ΔacrAB: KANR (Pradel and Pagès 2002; Ghisalberti et al. 2005)
CM64 CHLR resistant variant obtained from ATCC13048 over-expressing the AcrAB pump Ghisalberti et al. (2005)
EA298 EA 289 tolC::KANR (Pradel and Pagès 2002; Ghisalberti et al. 2005)
EA27 Clinical MDR isolate exhibiting energy-dependent norfloxacin and chloramphenicol efflux with KANR and AMPR and NALR and STRR and TETR (Mallèa et al. 2002; Ghisalberti et al. 2005)
EA289 KAN sensitive derivative of EA27 Ghisalberti et al. (2005)
Klebsiella pneumoniae
ATCC11296 Reference strain
Kp55 Clinical MDR isolate, TETR ,AMPR ,ATMR , and CEFR Chevalier et al. (2000)
Kp63 Clinical MDR isolate, TETR,CHLR,AMPR, and ATMR Fredrickson et al. (2004)
K2 Klebsiella pneumonia AcrAB-TolC Laboratory collection
K24 Klebsiella pneumoniae AcrAB-Tolc
Pseudomonas aeruginosa
PA01 Reference strain
PA124 MDR clinical isolate Lorenzi et al. (2009)
Providencia stuartii
ATCC29916 Reference strain
PS2636 Clinical MDR isolate, AcrAB Laboratory collection
PS299645 Clinical MDR isolate, AcrAB
Enterobacter cloacae
BM47 Enterobacter cloacae AcrAB-Tolc
ECCI69 Enterobacter cloacae AcrAB-TolC
BM67 Enterobacter cloacae AcrAB-TolC
Open in a new tab

AMPR, ATMR, CEFR, CFTR, CHLR, FEPR, KANR, MOXR, NALR, NORR STRR, and TETR Resistance to ampicillin, aztreonam, cephalothin, cefadroxil, chloramphenicol, cefepime, kanamycin, moxalactam, streptomycin, and tetracycline; MDR multidrug resistant., OMPF and OMPC Outer Membran Protein F and C respectively. AcrAB-TolC efflux pump AcrAB associate to TolC porine, Pa Pseudomonas aeruginosa.

Bacteria strains and culture media

The studied microorganisms included references (from the American Type Culture Collection) and clinical (Laboratory collection) strains of Escherichia coli, Enterobacter aerogenes, Providencia stuartii, Pseudomonas aeruginosa, Klebsiella pneumoniae, and Enterobacter cloacae (Table 2). They were maintained on agar slant at 4°C and sub-cultured on a fresh appropriate agar plates 24 h prior to any antimicrobial test. Mueller Hinton Agar (MHA) was used for the activation of bacteria and the Mueller Hinton Broth (MHB) was used for the MIC determinations.

Bacterial susceptibility determinations

The respective MICs of samples on the studied bacteria were determined by using rapid INT colorimetric assay Mativandlela et al. (2006). Briefly, the test samples were first dissolved in DMSO/MHB. The solution obtained was then added to MHB, and serially diluted two fold (in a 96-well microplate). One hundred microlitres (100 μL) of inoculum (1.5 × 106 CFU/mL) prepared in MHB was then added. The plates were covered with a sterile plate sealer, then agitated to mix the contents of the wells using a shaker and incubated at 37°C for 18 hrs. Wells containing MHB, 100 μL of inoculum and DMSO at a final concentration of 2.5% served as negative control (this internal control was systematically added). Chloramphenicol (CHL) was used as reference antibiotic. The MICs of samples were detected after 18 hrs of incubation at 37°C, following addition (40 μL) of 0.2 mg/mL INT and incubation at 37°C for 30 min Kuete et al. (2008). Viable bacteria reduced the yellow dye to pink. MIC was defined as the lowest sample concentration that prevented this change and exhibited complete inhibition of bacterial growth. For the determination of MBC, he microplates ones were filled by 150 μL of MHB without extract of plant; for wells not having received a INT (during the reading of the MIC), 50 μL of the contents of the wells corresponding to the concentrations higher or equal to the MIC was taken and introduced into these microplates. These were then incubated during 48 h à 37°C followed by revelation with the INT. All the concentrations to which we did not observe pink coloring were taken as bactericides and smallest of those, was noted as MBC. Samples were tested alone and then, in the presence of PAβN at 30 μg/mL final concentration.

Results

Phytochemical composition of the plant extracts

The results of qualitative analysis showed that all the crude extracts tested, except that for C. esculentus, contained alkaloids, phenols and polyphenols; others phytochemicals classes being selectively detected (Table 3).

Table 3.

Parts used, extraction yields, physical aspect and phytochemical composition of the plant extracts

Extracts S. radiatum C. zeylanicum C. olitorius S. indicum A. kayserianum A. digitata C. esculentus
Parts used Stem and leaves Bark Stem and leaves Beans Fruits Fruits Fruits
Yield* (%) 6.67 5.65 4.81 4.87 4.95 3.40 15.21
Alkaloids + + + + + + -
Anthocyanins - + - - + - -
Anthraquinones - - - + - - -
Flavonoids + - - - - + -
Phenols + + + + + + -
Tannins + - + - + - -
Triterpenes - + - + + + +
Sterols + - + + - + +
Saponins - - + + + + +
Open in a new tab

(+): Present; (−): Absent; * yield calculated as the ratio of the mass of the obtained methanol extract/mass of the plant powder.

Antibacterial activity of the plant extracts

The various strains and MDR isolates were tested for their susceptibilities to plants extracts and reference antibiotic (chloramphenicol). Chloramphenicol was also tested the presence of PAßN, a well-known efflux pump inhibitor to confirm the role of efflux pumps in the resistance of the studied microorganisms. Assays were performed using the broth microdilution method. The results depicted in Table 4 indicate that the plant extracts exhibited activities depending of bacteria strains, with MICs values ranged from 64 to 1024 μg/mL on the majority of the 27 tested microbial strains. At the tested concentration range (8 to 1024 μg/mL), the extracts which displayed activities against the majority of bacteria strains were those from S. indicum (active against 77.77% of the tested bacteria), C. zeylanicum (70.37%), S. radiatum (66.66%), C. olitorius (62.96%), A. kayserianum (51.85%), C. esculentus (18,52%) and A. digitata (14,81%). The lowest MIC value (64 μg/mL) was recorded with the extract of A. kayserianum against E. aerogenes EA294. Other extracts exhibited weak activities against a limited number of strains studied. A keen look of the results of Table 4 also shows that the extract of S. indicum displayed the best spectrum of bactericidal effect with a ratio MBC/MIC ≤ 4 on 6 bacterial strains, followed by that of S. radiatum (2/27) and those of C zeylanicum, C. olitorius, A. kayserianum (1/27). Only the extract of A. digitata did not present any bactericidal activity.

Table 4.

MIC, MBC and MBC/MIC ratios of plants extracts and CHL on the studied bacterial species

Tested bacteria Extracts and antimicrobial parameters (MIC and MBC in μg/mL)
S. radiatum C. zeylanicum C. olitorius S. indicum A. kayserianum A. digitata C. esculentus CHL CHL + PβBN
E. coli
ATCC8739 1024 (−) - - - - - - 8 (512) 4
ATCC10536 512 (−) - 1024 (−) 512 (−) - 512 (−) 512 (512) 4 (128) 1
W 3110 - 1024 (−) - 1024 (−) 512 (−) - - 4 (32) 1
MC4100 - 512 (512-) 1024 (−) - 1024 (−) - - 128 (512) 8
AG100 A - 512 (−) 128 (512) 512 (512) 1024 (−) - 256 (−) 4 (64) 0.5
AG100Atet 1024 (−) 512 (−) 1024 (−) 512 (−) 512 (−) - 1024 (−) 64 (8) 8
AG102 1024 (−) 512 (−) 1024 (−) 1024 (−) 1024 (−) - - 32 (512) 8
AG100 - 1024 (−) 512 (−) 512 (−) - - - 4(128) <4
E.aerogenes
ATCC13048 - - 512 (−) 1024 (−) - - - 8 (32) 4
EA294 - 256 (−) - - 64 (512) - - 32 (512) 8
CM64 1024 (−) 1024(−) - (−) 1024 (−) - - - 128 (−) 64
EA298 1024 (−) 512 (−) 1024 (−) 1024 (1024) 1024 (−) 256 (−) 512 (−) 256 (−) 64
EA27 - - 1024 (−) 256 (1024) 512 (−) - - - 32
EA289 1024 (−) 1024 (−) - 1024 (−) - - - 256 (−) 64
K.pneumoniae
ATCC11296 512 (−) 256 (−) - 512 (−) - - - 8 (256) 4
KP55 512 (−) 512 (−) 1024 (−) 512 (512) 1024 (1024) - - 4 (128) 1
KP63 1024 (−) 1024 (−) 1024 (−) 1024 (−) 1024 (−) - - 128 (−) 32
K2 1024 (−) 1024 (−) 512 (−) 256 (256) - 1024 (−) - 4 (128) 1
K24 - 512 (−) 1024 (−) 256 (−) 512 (−) - - 32 (512) 32
P.aeruginosa
PA01 1024 (−) - - - - - - 32 (256) 8
PA124 1024 (−) - - - - - - 64 (512) 16
P.stuartii
ATCC29916 256 (1024) 256 (−) - - 512 (−) - - 4 (32) 2
PS2636 1024 (−) - 512 (−) 512 (1024) 1024 (−) - - 4 (64) 2
PS299645 - 512 (−) 1024 (−) 1024 (−) - 256 (−) 1024 (−) 16 (64) 4
E.cloacae
BM47 1024 (−) 1024 (−) 1024 (−) 1024 (−) - - - 256 (−) 16
ECCI69 1024 (−) - 512 (−) 1024 (−) - - - 256 (−) 16
BM67 512 512 512 (−) - 1024 (−) 1024 (−) - - 512 (−) 16
Open in a new tab

(−):> 1024 μg/mL for the extracts and > 512 μg/mL for chloramphenicol and non given MBC/MIC. NT: not tested. (): MBC in μg/m.

Role of efflux pumps in susceptibility of Gram-negative bacteria to the tested plants extracts

The various strains and MDR isolates were also tested for their susceptibility to CHL in the presence of PAβN. As shown in Table 4, PAβN improved the activity of CHL to all studied bacteria.

Discussion

The extract from A. digitata, others extracts exhibited antibacterial activities against at least one of the tested bacteria. The differences in antibacterial activities were noted between the various extracts and could be related to the differences in their phytochemical composition as shown in Table 2. Except in the extract of C. esculentus, the alkaloids, phenols and polyphenols were detected in all extracts. The antibacterial activities of many molecules belonging to these classes of compounds were shown (Cowan 1999; Kuete et al. 2009). Sharma and Singh (2011) also associated the antibacterial activities of the medicinal plants to the presence of flavonoids, tannins and alkaloids. It should however be mentioned that the detection of the bioactive phytochemical classes in a plant is not a guarantee for any biological property, as this will depend on the types of compounds, as well as their concentrations and possible interaction with other constituents.

Alkaloids, phenols, sterols, polyphenols, triterpenes, anthraquinones and saponins were detected in the extract of S. indicum. The presence of the anthocyanins and the flavonoids in this plant was previously reported Awobajo et al. (2009), though such classes of chemicals were not detected in this work. This could be explained by fact that the presence of the secondary metabolites in a plant depend on the environmental factors such as climate, chemical nature of the ground in which plant grow, the period of harvest, conditions of drying and extraction method Bruneton (1999). To the best of our knowledge, no antibacterial activity of this plant was shown up to now, but presence of the various classes of secondary metabolites could explain its activity on majority of tested strains obtained in this work. In addition the antibacterial activities of the essential oil of S. radiatum (Shittu et al. 2006 Shittu et al. 2007; Konan et al. 2008).

Voukeng and collaborators (2012) documented the antibacterial activities of methanol extract of the sheets of C. zeylanicum against MDR Gram-negative bacteria used in this work. The presence of the phenolic compounds detected in thebark of this plant could explain its activities. Significantantibacterial activities of the methanol extract of C. olitorius were shown against the Gram-positive bacteria Pal et al. (2006). Also, the roots of this plant showed a significant antibacterial activity Ramadevi and Ganapaty (2011). The antibacterial activities of this plant as shown in this work provide therefore additional data on its antimicrobial potentials. Plants of the genus Aframomum are known for their antibacterial activities, and this has been assigned to the presence of terpenoids such as aframodial Ayafor et al. (1994). This could also explain the activity observed with the extract of A. kayserianum in the present work. Several former studies showed the presence of the terpenoids, phenolic and alkaloids in the extract of A. digitata (Wickens 1979; Chadare et al. 2009). The aqueous, ethanol, and petroleum-ether extracts of this plant have shown an antibacterial activity against E. coli Yagoub (2008). However, we observed a weak antibacterial activity of this plant. The extract of C. esculentus contains less secondary classes of metabolites. Only sterols, triterpenes and saponins were detected. To the best of our knowledge, the antibacterial of this plant is being reported for the first time. Generally, the weak antibacterial activity observed with the majority of the extracts could be explained by the fact that bacterial strains used are MDR phenotypes expressing active efflux pumps Cattoir (2004), as shown with the increase of the activity of CHL in the presence of PAβN (Table 4). It was demonstrated that efflux pumps decrease the intracellular concentration of chemicals and consequently their activities (Bambeke and Pagès 2010; Kuete 2010). These efflux pumps can be blocked in a competitive way or not, by an efflux inhibitor, which restore therefore not only intracellular concentration, but also the activity of antibiotics (Pagès and Amaral 2009; Kuete 2010). Finally, the results obtained with the studied plants are encouraging not only because we are dealing with MDR bacteria, but also the fact investigated plant materials are food plants which are relatively non toxic.

Conclusion

The results of the present work provide baseline information on the possible used of the tested Cameroonian dietary plants in the treatment of bacterial infections including MDR phenotypes.

Footnotes

Competing interests

The authors declare that they have no competing interests.

Authors’ contributions

AJS, AGF, DED, JAKN, IKV, SBT and AHLN carried out the study; VK designed the experiments and supervised the work; AGF and AJS wrote the manuscript; VK provided the bacterial strains; All authors read and approved the final manuscript.

Contributor Information

Jackson A Seukep, Email: seukepp@yahoo.fr.

Aimé G Fankam, Email: agfankam@yahoo.fr.

Doriane E Djeussi, Email: princessedoriane@yahoo.fr.

Igor K Voukeng, Email: tefogang@yahoo.fr.

Simplice B Tankeo, Email: presidentankeo@yahoo.fr.

Jaurès AK Noumdem, Email: jauresnoume@yahoo.fr.

Antoine HLN Kuete, Email: hantoineit@yahoo.fr.

Victor Kuete, Email: kuetevictor@yahoo.fr.

References

  1. Al-Qarawi AA, Al-Damegh MA, El-Mougy SA. Hepatoprotective Influence of Adansonia digitata Pulp. Journal of Herbs Spices and Medicinal Plants. 2010;10:1–6. doi: 10.1300/J044v10n03_01. [DOI] [Google Scholar]
  2. Anani K, Hudson JB, Souzal C, Akpagana K, Tower GHN, Amason JT, Gbeassor M. Investigation of medicinal plants of Togo for antiviral and antimicrobial activities. Pharmceut Biol. 2000;38:40–45. doi: 10.1076/1388-0209(200001)3811-BFT040. [DOI] [PubMed] [Google Scholar]
  3. Awobajo FO, Omorodion-Osagie E, Olatunji-Bello II, Adegoke OA, Adeleke TL. Acute oral toxicity and phytochemistry of some West African medicinal plants. Nigerian Quarterly Journal of Hospital Medicine. 2009;19:320–329. doi: 10.4314/nqjhm.v19i1.50209. [DOI] [PubMed] [Google Scholar]
  4. Ayafor JF, Tchuendem MH, Nyasse AB, Tillequin AH. Aframodial and other bioactive diterpenoids from Aframomum species. Appl Chem. 1994;66:2327–2330. doi: 10.1351/pac199466102327. [DOI] [PubMed] [Google Scholar]
  5. Bagliomi P, Liberatori S, Pallini V, Marri L. Proteome analysis of Escherichia coli W3110 expressing an heterogenous sigma factor. Proteomics. 2003;3:1060–1065. doi: 10.1002/pmic.200300403. [DOI] [PubMed] [Google Scholar]
  6. Bambeke F, Pages J-M, Lee VJ. Inhibitor of bacterial efflux pumps as adjuvants in antibacterial therapy and diagnostic tools for detection of resistance by efflux. Frontier in Anti-Infective Drug Discovery. 2010;1:00–34. doi: 10.2174/157489106777452692. [DOI] [PubMed] [Google Scholar]
  7. Bankole MA, Shittu TA, Ahmed MN, Bankole RK, Shittu T, Kpela AOA. Synergistic antimicrobial activities of phytoestrogens in crude extract of two sesame species against some common microorganisms. Afr J Trad Compl Altern Med. 2007;4:427–433. doi: 10.4314/ajtcam.v4i4.31237. [DOI] [PMC free article] [PubMed] [Google Scholar]
  8. Bruneton J. Plantes Médicinales, Pharmacognosie, phytochimie. Paris: Tec et Doc; 1999. [Google Scholar]
  9. Cattoir V. Pompes d’efflux et résistance aux antibiotiques chez les bactéries. Pathol Biol. 2004;52:607–616. doi: 10.1016/j.patbio.2004.09.001. [DOI] [PubMed] [Google Scholar]
  10. Chadare FJ, Linnemann AR, Hounhouigan JD, Nout MJR, Van B. Baobab food products: a review on their composition and nutritional value. Critical Review in Food Science and Nutrition. 2009;49:254–274. doi: 10.1080/10408390701856330. [DOI] [PubMed] [Google Scholar]
  11. Chevalier J, Pagès J-M, Eyraud A, Malléa M. Membrane permeability modifications are involved in antibiotic resistance in Klebsiella pneumoniae. Biochem Biophys Res Commun. 2000;274:496–499. doi: 10.1006/bbrc.2000.3159. [DOI] [PubMed] [Google Scholar]
  12. Chollet R, Chevalier J, Bryskier A, Pagès J-M. The AcrAB-TolC pump is involved in macrolide resistance but not in telithromycin efflux in Enterobacter aerogenes and Escherichia coli. Antimicrob Agents Chemother. 2004;48:3621–3624. doi: 10.1128/AAC.48.9.3621-3624.2004. [DOI] [PMC free article] [PubMed] [Google Scholar]
  13. Cowan MM. Plant products as antimicrobial agents. Clin Microb Rev. 1999;12:564–582. doi: 10.1128/cmr.12.4.564. [DOI] [PMC free article] [PubMed] [Google Scholar]
  14. Falagas ME, Bliziotis IA. Pandrug-resistant Gram-negative bacteria (2007) the dawn of the post-antibiotic era. Int J Antimicrob Ag. 2007;29:630–636. doi: 10.1016/j.ijantimicag.2006.12.012. [DOI] [PubMed] [Google Scholar]
  15. Fredrickson J, Zachara J, Balkwill D. Geomicrobiology of high-level nuclear waste-contaminated vadose sediments at the Hanford site, Washington state. Appl Environ Microbiol. 2004;70:4230–4241. doi: 10.1128/AEM.70.7.4230-4241.2004. [DOI] [PMC free article] [PubMed] [Google Scholar]
  16. Gende LB, Ignazio F, Rosalia F, Martin JE. Antimicrobial activity of cinnamon (Cinnamomum zeylanicum) essential oil and its main components against Paenibacillus larvae from Argentine. Bull Insectology. 2008;61:1–4. [Google Scholar]
  17. Ghisalberti D, Masi M, Pagès J-M, Chevalier J. Chloramphenicol and expression of multidrug efflux pump in Enterobacter aerogenes. Biochem Biophys Res Commun. 2005;328:1113–1118. doi: 10.1016/j.bbrc.2005.01.069. [DOI] [PubMed] [Google Scholar]
  18. Harbone JB. Phytochemical methods: A guide to modern techniques of plant analysis. London: Chapman and Hall; 1973. [Google Scholar]
  19. Kaboré D, Hagrétou S, Bréhima D, Compaoré CS, Dicko MH, Mogens J. A review of baobab (Adansonia digitata) products effect of processing techniques, medicinal properties and uses. African Journal of Food Science. 2011;5:833–844. [Google Scholar]
  20. Kokate C, Purohit A, Gokhale S. Pharmacognosy. 17. Pune: New Delhi; 2005. [Google Scholar]
  21. Konan AB, Datte JY, Yapo PA. Nitric oxide pathway-mediated relaxant effect of aqueous sesame leaves extract (Sesamum radiatum) in the guinea pig isolated aorta smooth muscle. BMC Complement Alter Med. 2008;8:23. doi: 10.1186/1472-6882-8-23. [DOI] [PMC free article] [PubMed] [Google Scholar]
  22. Kuete V, Fozing DC, Kapche WFGD, Mbaveng AT, Kuiate JR, Ngadjui BT, Abegaz BM. Antimicrobial activity of the methanolic extract and compounds from Morus mesozygia stem bark. J Ethnopharmacol. 2009;124:551–555. doi: 10.1016/j.jep.2009.05.004. [DOI] [PubMed] [Google Scholar]
  23. Kuete V, Ngameni B, Simo CCF, Tankeu RK, Ngadjui BT, Meyer JJM, Lall N, Kuiate JR. Antimicrobial activity of the crude extracts and compounds from Ficus chlamydocarpa and Ficus cordata (Moraceae) J Ethnopharmacol. 2008;120:17–24. doi: 10.1016/j.jep.2008.07.026. [DOI] [PubMed] [Google Scholar]
  24. Kuete V, Ngameni B, Tangmouo JG, Bolla J-M, Alibert-Franco S, Ngadjui BT, Pagès J-M. Efflux pumps are involved in the defence of Gram-negative bacterial against the natural products isobavachalcone and diospyrone. Antimicrob ag chemother. 2010;54:1749–1752. doi: 10.1128/AAC.01533-09. [DOI] [PMC free article] [PubMed] [Google Scholar]
  25. Kuete V. Potential of Cameroonian plants and derived products against microbial infections: a review. Planta Med. 2010;76:1–13. doi: 10.1055/s-0030-1250027. [DOI] [PubMed] [Google Scholar]
  26. Kumar M, Anjoo K, Sidhraj S. Hepatoprotective activity of Sesamum Indicum Linn. against Ccl4-induced hepatic damage in rats. International Journal of Pharmaceutical and Biological Archives. 2011;2:710–715. [Google Scholar]
  27. Li XZ, Nikaido H. Efflux-mediated drug resistance in bacteria: an update. Drugs. 2009;69:1555–1623. doi: 10.2165/11317030-000000000-00000. [DOI] [PMC free article] [PubMed] [Google Scholar]
  28. Lomovskaya OMS, Warren A, Lee J, Galazzo R, Fronko M, Lee J, Blais J, Cho D, Chamberland S, Renau T, Leger R, Hecker S, Watkins W, Hoshino K, Ishida H, Lee VJ. Identification and characterization of inhibitors of multidrug resistance efflux pumps in Pseudomonas aeruginosa: novel agents for combination therapy. Antimicrob Ag Chemother. 2004;45:105–116. doi: 10.1128/AAC.45.1.105-116.2001. [DOI] [PMC free article] [PubMed] [Google Scholar]
  29. Lorenzi V, Muselli A, Bernadini AF, Berti L, Pages J-M. Geraniol restores antibiotic activities against multidrugs resistant isolates from Gram-negative species. Antimicrob Ag Chemother. 2009;53:2209–2211. doi: 10.1128/AAC.00919-08. [DOI] [PMC free article] [PubMed] [Google Scholar]
  30. Mallèa M, Chevalier J, Eyraud A, Pagès J-M. Inhibitors of antibiotic efflux pumps in resistant Enterobacter aerogenes strains. Biochem Biophys Res Commun. 2002;293:1370–1373. doi: 10.1016/S0006-291X(02)00404-7. [DOI] [PubMed] [Google Scholar]
  31. Mallea M, Mahamoud A, Chevalier J, Alibert-Franco S, Brouant P, Barbe J, Pages JM. Alkylaminoquinolines inhibit the bacterial antibiotic efflux pump in multidrug-resistant clinical isolates. Biochemical Journal. 2003;376:801–805. doi: 10.1042/BJ20030963. [DOI] [PMC free article] [PubMed] [Google Scholar]
  32. Martina AW: Identification and characterization of sulfur-regulated gene in Escherichia coli MC4100. Zurich: degree of Doctor of Natural Sciences; 2002. [A dissertation submitted to the Swiss Institute of technology]
  33. Mativandlela SPN, Lall N, Meyer JJM. Antibacterial, antifungal and antitubercular activity of (the roots of) Pelargonium reniforme (CURT) and Pelargonium sidoides (DC) (Geraniaceae) root extracts. S Afr J Bot. 2006;72:232–237. doi: 10.1016/j.sajb.2005.08.002. [DOI] [Google Scholar]
  34. Monks TJ, Hanzlik RP, Cohen GM, Ross D, Graham DG. Quinone chemistry and toxicity. Toxicol Appl Pharmacol. 1992;112:2–16. doi: 10.1016/0041-008X(92)90273-U. [DOI] [PubMed] [Google Scholar]
  35. Nakano D, Kwak CJ. Sesamine metabolites induce an endothelial nitric acid dependent vasorelaxation. J Pharmacol Exp Ther. 2006;318:328–335. doi: 10.1124/jpet.105.100149. [DOI] [PubMed] [Google Scholar]
  36. Okusu H, Ma D, Nikaido HD. AcrAB efflux pump plays a major role in the antibiotic resistance phenotype of Escherichia coli multiple-antibiotic-resistance Mar. mutants. J Bacteriol. 1996;178:306–308. doi: 10.1128/jb.178.1.306-308.1996. [DOI] [PMC free article] [PubMed] [Google Scholar]
  37. Osibote EAS, Ogunlesi M, Okiei W, Asekun T, Familani OB. Assessment of antimicrobial activity of the essential oil from the stem powder of Cissus populnea and the leaves of Sesamum radiatum, herbal medications for male infertility factor. J Med Plants Res. 2010;4:14–20. doi: 10.3923/rjmp.2010.14.20. [DOI] [Google Scholar]
  38. Pagès J-M, Amaral L. Mechanisms of drug efflux and strategies to combat them: challenging the efflux pump of Gram-negative bacteria. Biochim Biophys Acta. 2009;1794:826–833. doi: 10.1016/j.bbapap.2008.12.011. [DOI] [PubMed] [Google Scholar]
  39. Pal D, Mandal GP, Padhiari SA. Antibacterial activity of Cuscuta reflexa stem and Corchous olitorius seed. Fitoterapia. 2006;77:589–591. doi: 10.1016/j.fitote.2006.06.015. [DOI] [PubMed] [Google Scholar]
  40. Poole K. Efflux-mediated multiresistance in Gram-negative bacteria. Clin Microbiol Infect. 2004;10:12–26. doi: 10.1111/j.1469-0691.2004.00763.x. [DOI] [PubMed] [Google Scholar]
  41. Pradel E, Pagès J-M. The AcrAB-TolC efflux pump contributes to multidrug resistance in the nosocomial pathogen Enterobacter aerogenes. Antimicrobl Ag Chemother. 2002;46:2640–2643. doi: 10.1128/AAC.46.8.2640-2643.2002. [DOI] [PMC free article] [PubMed] [Google Scholar]
  42. Ramadevi D, Ganapaty S. Antimicrobial activity of Corchous olitorius L. Pharmacology online. 2011;2:1303–1308. [Google Scholar]
  43. Sharma SK, Singh AP. Antimicrobial investigations on rhizomes of Cyperus rotundus Linn. Der Pharmacia Lettre. 2011;3:427–431. [Google Scholar]
  44. Shittu L, Bankole MA, Ahmed T, Bankole MN, Shittu RK, Saalu CL, Ashiru OA. Antibacterial and antifungal activities of essential oils of crude extracts of Sesame Radiatum against some common pathogenic microorganisms. Iranian Journal of Pharmacology and Therapeutics. 2007;6:165–170. [Google Scholar]
  45. Shittu LAJ, Bankole MA, Ahmed T, Aile K, Akinsanya MA. Differential antimicrobial activity of the various crude leaves extracts of Sesamum radiatum against some common pathogenic microorganisms. Scientific Research and Essays. 2006;1:108–111. [Google Scholar]
  46. Tane P, Tatsimo SD, Ayimele GA, Conolly JD. Bioactive metabolites from Afromomum species. Antananarivo: Madagascar: 11th NAPRECA Symposium Book of Proceedings; 2005. pp. 214–223. [Google Scholar]
  47. Vimalanathan S, Hudson JB. Multiple inflammatory and antiviral activities in Adansonia digitata (Baobab) leaves, fruits and seeds. Journal of Medicinal Plants Research. 2009;3:576–582. [Google Scholar]
  48. Voukeng I, Kuete V, Dzoyem JP, Fankam AG, Noumedem JA, Kuiate JR. Pages J-M (2012) antibacterial and antibiotic-potentiation activities of the methanol extract of some Cameroonian spices against Gram-negative multi-drug resistant phenotypes. BMC Res Notes. 2012;5:299. doi: 10.1186/1756-0500-5-299. [DOI] [PMC free article] [PubMed] [Google Scholar]
  49. Wickens GE. The uses of the baobab (Adansonia digitata L.) in Africa. In: Kunkel G, editor. Taxonomic aspects of African economic botany. Las Palmas de Gran Canaria: A.E.T.F.A.T; 1979. pp. 27–34. [Google Scholar]
  50. Xu H, Yong-ping WZ, Qing H. In vitro antitumour activity of Sesamum indicum Linn flower extracts. Trop J Pharmaceut Res. 2010;9:455–462. [Google Scholar]
  51. Yagoub S. Antimicrobial activity of Tamarindus indica and Adansonia digitata extracts against E. coli isolated from urine and water specimens. Research. Journal of Microbiology. 2008;3:193–197. [Google Scholar]
  52. Zacharia ZA, Somchit MN, Zaiton H, Mat AM, Sulaiman MR, Farah WO, Nazaratulmawarina R, Fatimah CA. The in vitro antibacterial activity of Corchous olitorius extracts. International Journal of Pharmacology. 2006;2:213–215. doi: 10.3923/ijp.2006.213.215. [DOI] [Google Scholar]

Articles from SpringerPlus are provided here courtesy of Springer-Verlag

RESOURCES