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Journal of Medicinal Plants Research Vol. 6(27), pp. 4368-4374, 18 July, 2012 
Available online at http://www.academicjournals.org/JMPR 
DOI: 10.5897/JMPR12.279 
ISSN 1996-0875 ©2012 Academic Journals 
Review 
Medicinal properties of Moringa oleifera: An overview 
of promising healer 
Fozia Farooq1*, Meenu Rai2, Avinash Tiwari1, Abdul Arif Khan3 and Shaila Farooq4 
1School of Studies in Botany, Jiwaji University, Gwalior-474001 (MP), India. 
2Life Science Department, Vijayaraje Institute of Science and Management, Turari, NH 75, Gwalior (MP), India. 
3Department of Pharmaceutics, College of Pharmacy, P. O. Box 2457, King Saud University, Riyadh 11451, 
Saudi Arabia. 
4School of Studies in Biotechnology, Jiwaji University, Gwalior-474001 (MP), India. 
Accepted 3 May, 2012 
Moringa oleifera Lam. (MO) is a small size tree with approximately 5 to 10 m height. It is cultivated all 
over the world due to its multiple utilities. Every part of Moringa is used for certain nutritional and/or 
medicinal propose. Besides being a good source of protein, vitamins, oils, fatty acids, micro-macro 
minerals elements and various phenolics, it is also reported as anti-inflammatory, antimicrobial, 
antioxidant, anticancer, cardiovascular, hepatoprotective, anti-ulcer, diuretic, antiurolithiatic, and 
antihelmintic. Its multiple pharmaceutical effects are capitalized as therapeutic remedy for various 
diseases in traditional medicinal system. Further research on this charismatic healer may lead to the 
development of novel agents for various diseases. This study provides a brief overview about medicinal 
potential of Moringa and its future as a component of modern medicinal system. This study concludes 
that Moringa needs legitimate appraisal to establish its pharmaceutical knack in modern medicine. 
Key word: Moringa oleifera, medicinal plant, anti-inflammatory, anti-microbial, antioxidant, antiulcer, diuretic. 
INTRODUCTION 
Moringa oleifera (MO) is an aboriginal of Indian 
subcontinent and has become naturalized in the tropical 
and subtropical areas around the world. Nearly thirteen 
species of Moringa are included in the family 
Moringaceae (Nadkarni, 1976). Indians have been using 
it as a regular component of conventional eatables for 
nearly 5000 years (Anwar et al., 2005; Anwar and 
Bhanger, 2003; D'Souza and Kulkarni, 1993). Moringa 
tree can grow well in the humid tropic or hot dry land with 
average height that ranges from 5 to 10 m. It can survive 
in harsh climatic condition including destitute soil without 
being much affected by drought (Morton, 1991). It can 
tolerate wide range of rainfall requirements estimated at 
250 mm and maximum at over 3000 mm and a pH of 5.0 
to 9.0 (Palada and Chang, 2003). Its trunk is soft, white 
*Corresponding author. E-mail: foziarifkhan@gmail.com. 
Abbreviations: MO, Moringa oleifera; GK, Goto-Kakizaki; ISP, 
isoproterenol. 
corky and branches bearing a gummy bark. Each 
tripinnately compound leaves bear several small leaf 
legs. The flowers are white and the three wings seeds 
are scattered by the winds. The flowers, tenders leaves 
and pods are eaten as vegetables. The leaves are rich in 
iron and therefore highly recommended for expected 
mothers. In some part of the world, MO is referred to as 
the ‘drum stick tree’ or the ‘horse radish tree’, whereas in 
others, it is known as the kelor, marango, mlonge, 
moonga, mulangay, nebeday, saijhan, sajna or Ben oil 
tree (Anwar and Bhanger, 2003; Prabhu et al., 2011). In 
India and Pakistan, MO is locally known as Sohanjna and 
is grown and cultivated all over the country (Anwar et al., 
2005; Qaisar, 1973). It has been reported by Bureau of 
plant industry that Moringa is an outstanding source 
nutritional components. Its leaves (weight per weight) 
have the calcium equivalent of four times that of milk, the 
vitamin C content is seven times that of oranges, while its 
potassium is three times that of bananas, three times the 
iron of spinach, four times the amount of vitamin A in 
carrots, and two times the protein in milk (Kamal, 2008). 
Besides, Moringa is also suggested as a viable
supplement of dietary minerals. The pods and leaves of 
Moringa contains high amount of Ca, Mg, K, Mn, P, Zn, 
Na, Cu, and Fe (Aslam et al., 2005). Although, minerals 
content of Moringa shows variation in composition with 
changes in location (Anjorin et al., 2010). 
Ancient medicinal system relies on several plant 
products used by traditionally human communities in 
many parts of the world for different diseases. Among 
these plants, MO has its great contribution from ancient 
time. It is a plant with exceptional medicinal properties 
which can resolves the health care needs in several 
situations. Easy cultivation of Moringa within adverse 
environmental condition and wide availability attract 
attention for economic and health related potential in 
resource limited developing countries. This study 
discusses medicinal potential of this exceptional plant 
and its potential as a commercial medicinal and 
nutritional supplement. 
MEDICINAL PROPERTIES OF MORINGA 
MO has enormous medicinal potential, which has long 
been recognized in the Ayurvedic and Unani system 
(Mughal et al., 1999). Nearly every part of this plant, 
including root, bark, gum, leaf, fruit (pods), flowers, seed, 
and seed oil have been used for various ailments in the 
indigenous medicine (Odebiyi and Sofowora, 1999), but 
recent research is also indicating about several active 
constituents for accepting its applicability in modern 
medicine (Table 1). Few representatives of these are 
discussed in this article. 
Antimicrobial and antihelmintic effects 
Antimicrobial components of MO have been validated 
after the discovery of inhibitory activity against several 
microorganisms. In a recent study, aqueous extracts of 
MO was found to be inhibitory against many pathogenic 
bacteria, including Staphylococcus aureus, Bacillus 
subtilis, Escherichia coli, and Pseudomonas aeruginosa 
in dose dependent manner (Saadabi and Abu Zaid, 
2011). MO extracts was also found to be inhibitory 
against Mycobacterium phlei and B. subtilis (Eilert et al., 
1981). Leaf extract of MO was found to be effective in 
checking growth of fungi Basidiobolus haptosporus and 
Basidiobolus ranarums (Nwosu and Okafor, 1995). 
Another study involving aqueous methanolic extract and 
fixed oil against microorganisms was performed using 
Scenedesmus obliquus (green algae), E. coli ATCC 
13706, P. aeruginosa ATCC10145, S. aureus NAMRU 3 
25923, Bacillus stearothermophilus (bacterial strains) and 
Herpes Simplex virus type 1 (HSV 1) and Polio virus type 
1 (sabin vaccine). Varying degree of antimicrobial activity 
was observed ranging from sensitive for B. 
stearothermophilus to resistant for P. aeruginosa (Ali et 
Farooq et al. 4369 
al., 2004). Beside antibacterial activity of MO oils, it also 
posses anti-fungal activity (Chuang et al., 2007). Study 
comparing relative antimicrobial activity of seed extracts 
against bacteria (Pasturella multocida, E. coli, B. subtilis 
and S. aureus) and fungi (Fusarium solani and Rhizopus 
solani) revealed that P. multocida and B. subtilis were the 
most sensitive strains, and their activity was influenced 
by cations (Na+, K+, Mg2+ and Ca2+) (Jabeen et al., 2008). 
Another relative comparison of antibacterial and 
antifungal efficacy of MO steam distillate observed more 
inhibition for E. coli followed by S. aureus, Klebsiella 
pneumoniae, P. aeruginosa and B. subtilis. In case of 
fungi, Aspergillus niger was strongly inhibited followed by 
Aspergillus oryzae, Aspergillus terreus and Aspergillus 
nidulans (Prashith Kekuda et al., 2010). Contrary to 
resistance against P. aeruginosa and Candida albicans 
for MO in other studies, one study using ethanolic extract 
of leaves, seeds and flowers showed the antimicrobial 
activity against E. coli, K. pneumoniae, Enterobacter 
species, Proteus mirabilis, P. aeruginosa, Salmonella 
typhi A, S. aureus, Streptococcus and Candida albicans 
(Nepolean et al., 2009). Moringa contains pterygospermin 
(originally found in Moringa pterygosperma) which has 
powerful antibacterial and fungicidal effects (Rao et al., 
1946). Several other specific components of Moringa 
have been reported with antibacterial activity, including 4- 
(4'-O-acetyl-a-L-rhamnopyranosyloxy) benzyl 
isothiocyanate, 4-(a-L-rhamnopyranosyloxy) benzyl 
isothiocyanate, niazimicin, benzyl isothiocyanate, and 4- 
(a-L-rhamnopyranosyloxy) benzyl glucosinolate (Fahey, 
2005). Other bioactive compounds, such as Spirochin 
and Anthonine are found in root and are active against 
several bacteria. Anthonine has potent inhibitory activity 
against Vibrio cholerae (Nwosu and Okafor, 1995). MO 
flower and leaves are also capable of controlling parasitic 
worms, their antihelmintic activity has been demonstrated 
during several studies (Bhattacharya et al., 1982). 
Moreover, it has also been reported to inhibit Indian 
earthworm Pheritima posthuma with MO leaves ethanolic 
extracts (Rastogi et al., 2009). 
Anti-inflammatory activity 
Moringa plant parts have substantial anti-inflammatory 
activity. For instance, the root extract exhibits significant 
anti-inflammatory activity in carrageenan induced rat paw 
oedema (Ezeamuzie et al., 1996; Khare et al., 1997). The 
crude methanol extract of the root inhibits carrageenan-induced 
rat paw oedema in a dose dependent manner 
after oral administration (Anonymous, 2005). Moreover, 
n-butanol extract of the seeds of MO shows anti-inflammatory 
activity against ovalbumin-induced airway 
inflammation in guinea pigs (Mahajan et al., 2009). 
Amelioration of inflammation associated chronic diseases 
can be possible with the potent anti-inflammatory activity 
of MO bioactive compounds (Muangnoi et al., 2011).
4370 J. Med. Plants Res. 
Considering potent anti-inflammatory activity of Moringa 
plant, it can be surmised that this plant shows profound 
influence on inflammation associated diseases and 
resultant symptoms. As a consequence, this plant shows 
beneficial effects on asthma, pain, and other resultant 
symptoms. 
Anti-asthmatic activity 
It has been reported a long time ago that Moringa plant 
alkaloid closely resembles ephedrine in action and can 
be used for the treatment of asthma. Alkaloid moringine 
relaxes bronchioles (Kirtikar and Basu, 1975). The seed 
kernels of MO also showed promising effect in the 
treatment of bronchial asthma, during a study to analyze 
efficacy and safety of seed kernels for the management 
of asthmatic patients. The study showed significant 
decrease in the severity of asthma symptoms and also 
concurrent respiratory functions improvement (Agrawal 
and Mehta, 2008). 
Analgesic activity 
The analgesic activity of Moringa has been reported in 
several Moringa species. In a study using ethanolic 
extracts of Moringa concanensis tender pod-like fruits in 
experimental animals, a significant analgesic activity was 
observed (Rao et al., 2008). Furthermore, alcoholic 
extract of the leaves and seeds of MO also possess 
marked analgesic activity as evidenced through hot plate 
and tail immersion method (Sutar et al., 2008). 
Antipyretic activity 
As a result of anti-inflammatory action of Moringa 
bioactive constituents, the antipyretic activity can be 
hypothesized. A study was designed to assess antipyretic 
effect of ethanol, petroleum ether, solvent ether and ethyl 
acetate extracts of MO seeds using yeast induced 
hyperpyrexia method. Paracetamol was used as control 
during the study. Not surprisingly, ethanol and ethyl 
acetate extracts of seeds showed significant antipyretic 
activity in rats (Hukkeri et al., 2006). 
Antihypertensive, diuretic and cholesterol lowering 
activities 
Moringa leaves contain several bio active compounds, 
they exert direct effect on blood pressure, and thus these 
can be used for stabilizing blood pressure. MO com-pounds 
leading to blood pressure lowering effect includes 
nitrile, mustard oil glycosides and thiocarbamate 
glycosides present in Moringa leaves (Anwar et al., 
2007). In addition, diuretic activity of Moringa exists in its 
roots, leaves, flowers, gum and the aqueous infusion of 
seeds (Morton, 1991). Moreover, Moringa leaves also 
contain bioactive phytoconstituent, (that is, b-sitosterol) 
with cholesterol lowering effect. This compound is 
capable to reduce cholesterol level from the serum of 
high fat diet fed rats (Ghasi et al., 2000). 
Antidiabetic activity 
Several medicinal plants have been evaluated for their 
potential as therapeutic agent for diabetes. MO is also an 
important component in this category. MO leaves 
significantly decrease blood glucose concentration in 
Wistar rats and Goto-Kakizaki (GK) rats, modeled type 2 
diabetes (Ndong et al., 2007). Another study indicated 
that the extract from Moringa leaf is effective in lowering 
blood sugar levels within 3 h after ingestion (Mittal et al., 
2007). As a mechanistic model for antidiabetic activity of 
MO, it has been indicated that dark chocolate 
polyphenols (Grassi et al., 2005) and other polyphenols 
(Al-Awwadi et al., 2004; Moharram et al., 2003) are 
responsible for hypoglycemic activity. Moringa leaves are 
potent source of polyphenols, including quercetin-3- 
glycoside, rutin, kaempferol glycosides, and other 
polyphenols (Ndong et al., 2007). Thus, potential anti-diabetic 
activity of MO can be commercialized through 
the development of suitable technology with achieving 
anti-diabetic activity up to conventional drugs. 
Antioxidant activity 
MO is a rich source of antioxidant (Chumark et al., 2008). 
It has been reported that aqueous extracts of leaf, fruit 
and seed of MO act as an antioxidant (Singh et al., 
2009). During a study reporting antioxidant property of 
freeze dried Moringa leaves from different extraction 
procedures, it was found that methanol and ethanol 
extracts of Indian origin MO have the highest antioxidant 
activity with 65.1 and 66.8%, respectively (Lalas and 
Tsaknis, 2002; Siddhuraju and Becker, 2003). It was also 
reported that the major bioactive compounds of 
phenolics, such as quercetin and kaempferol are 
responsible for antioxidant activity (Bajpai et al., 2005; 
Siddhuraju and Becker, 2003). During another study, 
quercetin and kaempferol have shown good antioxidant 
activity on hepatocyte growth factor (HGF) induced Met 
phosphorylation with IC50 value for 12 and ~6 μM/L, 
respectively (Labbe et al., 2009). Another recent study 
comparing palm oil with MO seeds for their antioxidant 
potential found out that MO seed are superiors for radical 
scavenging (Ogbunugafor et al., 2011). 
Hepatoprotective activity 
MO has shown significant hepatoprotective activity in
several studies. MO leaves ethanolic extracts showed 
significant protection against liver damage induced by 
antitubercular drugs [isoniazid (INH), rifampicin (RMP), 
and pyrazinamide (PZA)] in rats. It was found that 
hepatoprotective activity of MO is medicated by its effect 
on the levels of glutamic oxaloacetic transaminase 
(aspartate aminotransferase), glutamic pyruvic 
transaminase (alanine aminotransferase), alkaline 
phosphatase, and bilirubin in the serum; lipids, and lipid 
peroxidation levels in liver (Pari and Kumar, 2002). 
Moreover, methanolic and chloroform extracts of MO 
leaves also showed significant protection against CCl4 
induced liver damage in albino rats. Besides 
hepatoprotective activity of MO leaves, its root and 
flowers also possess strong hepatoprotective activity. 
Moringa flowers contain a well recognized flavonoid 
(Quercetin), which may be responsible for its potent 
hepatoprotective activity (Ruckmani et al., 1998; 
Selvakumar and Natarajan, 2008). In a recent study 
evaluating the effect of MO seed extract on liver fibrosis, 
it was found that MO seed extract has the ability to 
subside liver fibrosis. This study involved CCl4 induced 
liver fibrosis and concurrent administration of MO seed 
extract. MO seed extract control the elevation of serum 
aminotransferase activities and globulin level induced by 
CCl4. Moreover, immunohistochemical studies also 
showed that MO reduces liver fibrosis (Hamza, 2010). 
Antitumor activity 
MO has been found as a potent anticancer plant and 
several bioactive compounds with significant antitumor 
activity have been discovered from MO. Among bioactive 
compounds from MO, niazimicin, a MO leaves 
thiocarbamate was found to have potent anticancer 
activity (Guevaraa et al., 1999). Furthermore, niazimicin 
also shows the inhibition of tumor promoter teleocidin B- 
4-induced Epstein-Barr virus (EBV) activation (Murakami 
et al., 1998). Another study involving 11 plants used in 
Bangladeshi folk medicine, MO was considered as 
potential source of anticancer compounds. During this 
study, the plant extract were analyzed for cytotoxicity 
through brine shrimp lethality assay, sea urchin eggs 
assay, hemolysis assay and MTT assay using tumor cell 
lines. The study also indicated the potential cytotoxic 
effects of MO leaf extract on human multiple myeloma 
cell lines (Costa-Lotufo et al., 2005; Parvathy and 
Umamaheshwari, 2007). Beside leaves, MO seed 
extracts also have anticancer activity through its effects 
on hepatic carcinogen metabolizing enzymes, and 
antioxidant property (Bharali et al., 2003). 
Antifertility activity 
MO plant also has pertinent antifertility activity. The 
aqueous extract obtained from root and bark of MO 
Farooq et al. 4371 
showed post-coital antifertility effect in rat and also 
induced foetal resorption at late pregnancy (Prakash et 
al., 1987). Moreover, aqueous extract of MO roots was 
also evaluated for estrogenic, anti-estrogenic, pro-gestational 
and antiprogestational activities. This extract 
induces several consequences for affecting its antifertility 
property (Shukla et al., 1988). During another study 
analyzing anti reproductive potential of folk medicine 
plants, MO leaf extracts were found to be 100% abortive 
with doses equivalent to 175 mg/kg of starting dry 
material (Nath et al., 1992). 
Antispasmodic and antiulcer effects 
Moringa root and leaves contain several compounds with 
spasmolytic activity. These compounds include 4- (alpha- 
L-rhamnosyloxybenzyl)-o-methyl thiocarbamate which is 
possibly affected through calcium channel blockade, 
niazinin A, niazinin B, niazimicin, etc., with hypotensive 
and bradycardiac effect. The spasmolytic activity of 
different constituents support for traditional uses of this 
plant in gastrointestinal motility disorder (Gilani et al., 
1994). MO methanolic extract is also capable in 
protecting experimental rats from gastric lesions induced 
by acetylsalicylic acid, serotonin and indomethacin. In 
addition, it also enhances healing process of chronic 
gastric lesions induced by acetic acid in experimental 
animals (Pal et al., 1995). Another study have reported 
the antiulcer effect of MO leaves aqueous extract on 
adult Holtzman albino rats (Debnath and Guha, 2007). 
Cardiac and circulatory stimulant 
In addition to earlier mentioned bradycardiac effect of MO 
leaves, all parts of MO are reported with somewhat 
cardiac and circulatory stimulant activity. Root bark of 
Moringa contains alkaloid moringinine which acts as 
cardiac stimulant through its effect on sympathetic 
nervous system (Duke, 2001). The aforementioned 
effects can also result due to the prevention of 
hyperlipidemia. It has been demonstrated that MO 
prevent hyperlipidemia in male Wister rat due to iron 
deficiency (Ndong et al., 2007). During a study 
performing comparison of MO leaf extract with antenolol 
(a selective β1 receptor antagonist drug, used for 
cardiovascular diseases) on serum cholesterol level, 
serum triglyceride level, blood glucose level, heart weight 
and body weight of adrenaline induced rats, it was found 
that MO leaf extract cause significant changes in 
cardiovascular parameters. This study reported MO leaf 
extract as hypolipidimic, lowering body weight, heart 
weight, serum triglyceride level and serum cholesterol 
level in experimental animals (Ara et al., 2008). In 
addition to the aforementioned studies, antiatheroscle-rotic 
and hypolipidaemic effect of MO leaves were also
4372 J. Med. Plants Res. 
Table 1. Major pharmaceutical components present in Moringa and their importance. 
S/N Compound Method used for detection Potential 
application Reference 
1 Pterygospermin Solvent extraction followed by MIC 
analysis 
Antibacterial and 
fungicidal effects 
Rao et al. (1946) 
2 4-(4'-O-acetyl-a-L-rhamnopyranosyloxy) 
benzyl isothiocyanate, 4-(a-L-rhamnopyranosyloxy) 
benzyl 
isothiocyanate, niazimicin, benzyl 
isothiocyanate, and 4-(a-L-rhamnopyranosyloxy) 
benzyl 
glucosinolate, Anthonine and Spirochin 
Solvent extraction followed by MIC 
analysis (Busani et al., 2012) Antibacterial 
Fahey (2005) and 
Nwosu and Okafor 
(1995) 
3 Alkaloid Moringine 
Clinical study involving 
consumption of Moringa followed 
by antiasthmatic activity evaluation 
using spirometer 
Antiasthmatic 
Agrawal and Mehta 
(2008) and Kirtikar and 
Basu (1975) 
4 Nitrile, mustard oil glycosides and 
thiocarbamate glycosides 
Bioassay directed isolation Hypotensive Anwar et al. (2007) and 
Faizi et al. (1995) 
5 b-sitosterol 
Study involved consumption of 
Moringa leaves with cholesterol 
and subsequent measurement of 
cholesterol lowering activity (Ghasi 
et al., 2000). 
Cholesterol 
lowering effects Ghasi et al. (2000) 
6 Dark chocolate polyphenols and other 
polyphenols 
Administration of MO leaves in 
diabetic and control rats and 
hypoglycemic activity evaluation 
and characterization of 
polyphenols using HPLC (Ndong 
et al., 2007). 
Hypoglycemic 
effects 
Grassi et al. (2005), Al- 
Awwadi et al. (2004) 
and Moharram et al. 
(2003) 
7 Quecertin and kaempferol Solvent extraction followed by 
antioxidant activity analysis 
Antioxidant, 
hepatoprotective 
Bajpai et al. (2005), 
Siddhuraju and Becker 
(2003), Ruckmani et al. 
(1998) and Selvakumar 
and Natarajan (2008) 
8 Niazimicin, 
Solvent extraction followed by in 
vitro anticancer activity Anticancer Guevaraa et al. (1999) 
9 
4- (alpha- L-rhamnosyloxybenzyl)-o-methyl 
thiocarbamate, niazinin A, 
niazinin B, niazimicin etc. 
Solvent extraction for purification 
of compounds followed by 
intravenous administration of each 
compound in anaesthetized rats 
and subsequent evaluation of their 
activity in experimental animals 
Spasmolytic, 
hypotensive and 
bradycardiac 
Gilani et al. (1994) 
analyzed in another study using simvastatin as control 
(Chumark et al., 2008). MO also causes cardio protective 
effects in isoproterenol (ISP)-induced myocardial 
infarction in male Wistar albino rats. It was reported that 
MO treatment plays favorable modulation on biochemical 
enzymatic parameters including, superoxide dismutase, 
catalase, glutathione peroxidase, lactate dehydrogenase, 
and creatine kinase-MB. Moreover, it also prevents 
histopathological damage and ultra-structure perturbation 
caused due to ISP induced myocardial infarction
(Nandave et al., 2009). 
In ocular diseases 
Vitamin A deficiency is a major cause of blindness, which 
ranges from impaired dark adaptation to night blindness. 
Consumption of MO leaves, and pods and leaf powder 
which contain high proportion of vitamin A can help to 
prevent night blindness and eye problems in children. 
Ingesting drumstick leaves with oils can improve vitamin 
A nutrition and can delay the development of cataract 
(Pullakhandam and Failla, 2007). In fact the use of MO 
as a supplementary food was highly accepted for 
integrated child development scheme supplementary 
food (ICDS-SFP) for its potential as vitamin A source 
(Nambiar et al., 2003). 
Conclusion 
Medicinal potential of MO is enormous and difficult to 
cover in a single article, despite this current article 
provided glimpses of MO applications for performing 
appraisal of this promising nutrition and medicinal plant. 
Although, many bioactive compounds have been 
discovered from Moringa, still the knowledge is in infancy, 
in term of its total reserve. Perhaps, future rigorous 
studies directed towards the detection, and 
commercialization of MO bioactive compounds can lead 
to the development of remedies for several ailments. 
Thus, it can also prove the validity of traditional utility of 
MO in various folklores. 
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Medicinal properties of_moringa_oleifera

  • 1. Journal of Medicinal Plants Research Vol. 6(27), pp. 4368-4374, 18 July, 2012 Available online at http://www.academicjournals.org/JMPR DOI: 10.5897/JMPR12.279 ISSN 1996-0875 ©2012 Academic Journals Review Medicinal properties of Moringa oleifera: An overview of promising healer Fozia Farooq1*, Meenu Rai2, Avinash Tiwari1, Abdul Arif Khan3 and Shaila Farooq4 1School of Studies in Botany, Jiwaji University, Gwalior-474001 (MP), India. 2Life Science Department, Vijayaraje Institute of Science and Management, Turari, NH 75, Gwalior (MP), India. 3Department of Pharmaceutics, College of Pharmacy, P. O. Box 2457, King Saud University, Riyadh 11451, Saudi Arabia. 4School of Studies in Biotechnology, Jiwaji University, Gwalior-474001 (MP), India. Accepted 3 May, 2012 Moringa oleifera Lam. (MO) is a small size tree with approximately 5 to 10 m height. It is cultivated all over the world due to its multiple utilities. Every part of Moringa is used for certain nutritional and/or medicinal propose. Besides being a good source of protein, vitamins, oils, fatty acids, micro-macro minerals elements and various phenolics, it is also reported as anti-inflammatory, antimicrobial, antioxidant, anticancer, cardiovascular, hepatoprotective, anti-ulcer, diuretic, antiurolithiatic, and antihelmintic. Its multiple pharmaceutical effects are capitalized as therapeutic remedy for various diseases in traditional medicinal system. Further research on this charismatic healer may lead to the development of novel agents for various diseases. This study provides a brief overview about medicinal potential of Moringa and its future as a component of modern medicinal system. This study concludes that Moringa needs legitimate appraisal to establish its pharmaceutical knack in modern medicine. Key word: Moringa oleifera, medicinal plant, anti-inflammatory, anti-microbial, antioxidant, antiulcer, diuretic. INTRODUCTION Moringa oleifera (MO) is an aboriginal of Indian subcontinent and has become naturalized in the tropical and subtropical areas around the world. Nearly thirteen species of Moringa are included in the family Moringaceae (Nadkarni, 1976). Indians have been using it as a regular component of conventional eatables for nearly 5000 years (Anwar et al., 2005; Anwar and Bhanger, 2003; D'Souza and Kulkarni, 1993). Moringa tree can grow well in the humid tropic or hot dry land with average height that ranges from 5 to 10 m. It can survive in harsh climatic condition including destitute soil without being much affected by drought (Morton, 1991). It can tolerate wide range of rainfall requirements estimated at 250 mm and maximum at over 3000 mm and a pH of 5.0 to 9.0 (Palada and Chang, 2003). Its trunk is soft, white *Corresponding author. E-mail: foziarifkhan@gmail.com. Abbreviations: MO, Moringa oleifera; GK, Goto-Kakizaki; ISP, isoproterenol. corky and branches bearing a gummy bark. Each tripinnately compound leaves bear several small leaf legs. The flowers are white and the three wings seeds are scattered by the winds. The flowers, tenders leaves and pods are eaten as vegetables. The leaves are rich in iron and therefore highly recommended for expected mothers. In some part of the world, MO is referred to as the ‘drum stick tree’ or the ‘horse radish tree’, whereas in others, it is known as the kelor, marango, mlonge, moonga, mulangay, nebeday, saijhan, sajna or Ben oil tree (Anwar and Bhanger, 2003; Prabhu et al., 2011). In India and Pakistan, MO is locally known as Sohanjna and is grown and cultivated all over the country (Anwar et al., 2005; Qaisar, 1973). It has been reported by Bureau of plant industry that Moringa is an outstanding source nutritional components. Its leaves (weight per weight) have the calcium equivalent of four times that of milk, the vitamin C content is seven times that of oranges, while its potassium is three times that of bananas, three times the iron of spinach, four times the amount of vitamin A in carrots, and two times the protein in milk (Kamal, 2008). Besides, Moringa is also suggested as a viable
  • 2. supplement of dietary minerals. The pods and leaves of Moringa contains high amount of Ca, Mg, K, Mn, P, Zn, Na, Cu, and Fe (Aslam et al., 2005). Although, minerals content of Moringa shows variation in composition with changes in location (Anjorin et al., 2010). Ancient medicinal system relies on several plant products used by traditionally human communities in many parts of the world for different diseases. Among these plants, MO has its great contribution from ancient time. It is a plant with exceptional medicinal properties which can resolves the health care needs in several situations. Easy cultivation of Moringa within adverse environmental condition and wide availability attract attention for economic and health related potential in resource limited developing countries. This study discusses medicinal potential of this exceptional plant and its potential as a commercial medicinal and nutritional supplement. MEDICINAL PROPERTIES OF MORINGA MO has enormous medicinal potential, which has long been recognized in the Ayurvedic and Unani system (Mughal et al., 1999). Nearly every part of this plant, including root, bark, gum, leaf, fruit (pods), flowers, seed, and seed oil have been used for various ailments in the indigenous medicine (Odebiyi and Sofowora, 1999), but recent research is also indicating about several active constituents for accepting its applicability in modern medicine (Table 1). Few representatives of these are discussed in this article. Antimicrobial and antihelmintic effects Antimicrobial components of MO have been validated after the discovery of inhibitory activity against several microorganisms. In a recent study, aqueous extracts of MO was found to be inhibitory against many pathogenic bacteria, including Staphylococcus aureus, Bacillus subtilis, Escherichia coli, and Pseudomonas aeruginosa in dose dependent manner (Saadabi and Abu Zaid, 2011). MO extracts was also found to be inhibitory against Mycobacterium phlei and B. subtilis (Eilert et al., 1981). Leaf extract of MO was found to be effective in checking growth of fungi Basidiobolus haptosporus and Basidiobolus ranarums (Nwosu and Okafor, 1995). Another study involving aqueous methanolic extract and fixed oil against microorganisms was performed using Scenedesmus obliquus (green algae), E. coli ATCC 13706, P. aeruginosa ATCC10145, S. aureus NAMRU 3 25923, Bacillus stearothermophilus (bacterial strains) and Herpes Simplex virus type 1 (HSV 1) and Polio virus type 1 (sabin vaccine). Varying degree of antimicrobial activity was observed ranging from sensitive for B. stearothermophilus to resistant for P. aeruginosa (Ali et Farooq et al. 4369 al., 2004). Beside antibacterial activity of MO oils, it also posses anti-fungal activity (Chuang et al., 2007). Study comparing relative antimicrobial activity of seed extracts against bacteria (Pasturella multocida, E. coli, B. subtilis and S. aureus) and fungi (Fusarium solani and Rhizopus solani) revealed that P. multocida and B. subtilis were the most sensitive strains, and their activity was influenced by cations (Na+, K+, Mg2+ and Ca2+) (Jabeen et al., 2008). Another relative comparison of antibacterial and antifungal efficacy of MO steam distillate observed more inhibition for E. coli followed by S. aureus, Klebsiella pneumoniae, P. aeruginosa and B. subtilis. In case of fungi, Aspergillus niger was strongly inhibited followed by Aspergillus oryzae, Aspergillus terreus and Aspergillus nidulans (Prashith Kekuda et al., 2010). Contrary to resistance against P. aeruginosa and Candida albicans for MO in other studies, one study using ethanolic extract of leaves, seeds and flowers showed the antimicrobial activity against E. coli, K. pneumoniae, Enterobacter species, Proteus mirabilis, P. aeruginosa, Salmonella typhi A, S. aureus, Streptococcus and Candida albicans (Nepolean et al., 2009). Moringa contains pterygospermin (originally found in Moringa pterygosperma) which has powerful antibacterial and fungicidal effects (Rao et al., 1946). Several other specific components of Moringa have been reported with antibacterial activity, including 4- (4'-O-acetyl-a-L-rhamnopyranosyloxy) benzyl isothiocyanate, 4-(a-L-rhamnopyranosyloxy) benzyl isothiocyanate, niazimicin, benzyl isothiocyanate, and 4- (a-L-rhamnopyranosyloxy) benzyl glucosinolate (Fahey, 2005). Other bioactive compounds, such as Spirochin and Anthonine are found in root and are active against several bacteria. Anthonine has potent inhibitory activity against Vibrio cholerae (Nwosu and Okafor, 1995). MO flower and leaves are also capable of controlling parasitic worms, their antihelmintic activity has been demonstrated during several studies (Bhattacharya et al., 1982). Moreover, it has also been reported to inhibit Indian earthworm Pheritima posthuma with MO leaves ethanolic extracts (Rastogi et al., 2009). Anti-inflammatory activity Moringa plant parts have substantial anti-inflammatory activity. For instance, the root extract exhibits significant anti-inflammatory activity in carrageenan induced rat paw oedema (Ezeamuzie et al., 1996; Khare et al., 1997). The crude methanol extract of the root inhibits carrageenan-induced rat paw oedema in a dose dependent manner after oral administration (Anonymous, 2005). Moreover, n-butanol extract of the seeds of MO shows anti-inflammatory activity against ovalbumin-induced airway inflammation in guinea pigs (Mahajan et al., 2009). Amelioration of inflammation associated chronic diseases can be possible with the potent anti-inflammatory activity of MO bioactive compounds (Muangnoi et al., 2011).
  • 3. 4370 J. Med. Plants Res. Considering potent anti-inflammatory activity of Moringa plant, it can be surmised that this plant shows profound influence on inflammation associated diseases and resultant symptoms. As a consequence, this plant shows beneficial effects on asthma, pain, and other resultant symptoms. Anti-asthmatic activity It has been reported a long time ago that Moringa plant alkaloid closely resembles ephedrine in action and can be used for the treatment of asthma. Alkaloid moringine relaxes bronchioles (Kirtikar and Basu, 1975). The seed kernels of MO also showed promising effect in the treatment of bronchial asthma, during a study to analyze efficacy and safety of seed kernels for the management of asthmatic patients. The study showed significant decrease in the severity of asthma symptoms and also concurrent respiratory functions improvement (Agrawal and Mehta, 2008). Analgesic activity The analgesic activity of Moringa has been reported in several Moringa species. In a study using ethanolic extracts of Moringa concanensis tender pod-like fruits in experimental animals, a significant analgesic activity was observed (Rao et al., 2008). Furthermore, alcoholic extract of the leaves and seeds of MO also possess marked analgesic activity as evidenced through hot plate and tail immersion method (Sutar et al., 2008). Antipyretic activity As a result of anti-inflammatory action of Moringa bioactive constituents, the antipyretic activity can be hypothesized. A study was designed to assess antipyretic effect of ethanol, petroleum ether, solvent ether and ethyl acetate extracts of MO seeds using yeast induced hyperpyrexia method. Paracetamol was used as control during the study. Not surprisingly, ethanol and ethyl acetate extracts of seeds showed significant antipyretic activity in rats (Hukkeri et al., 2006). Antihypertensive, diuretic and cholesterol lowering activities Moringa leaves contain several bio active compounds, they exert direct effect on blood pressure, and thus these can be used for stabilizing blood pressure. MO com-pounds leading to blood pressure lowering effect includes nitrile, mustard oil glycosides and thiocarbamate glycosides present in Moringa leaves (Anwar et al., 2007). In addition, diuretic activity of Moringa exists in its roots, leaves, flowers, gum and the aqueous infusion of seeds (Morton, 1991). Moreover, Moringa leaves also contain bioactive phytoconstituent, (that is, b-sitosterol) with cholesterol lowering effect. This compound is capable to reduce cholesterol level from the serum of high fat diet fed rats (Ghasi et al., 2000). Antidiabetic activity Several medicinal plants have been evaluated for their potential as therapeutic agent for diabetes. MO is also an important component in this category. MO leaves significantly decrease blood glucose concentration in Wistar rats and Goto-Kakizaki (GK) rats, modeled type 2 diabetes (Ndong et al., 2007). Another study indicated that the extract from Moringa leaf is effective in lowering blood sugar levels within 3 h after ingestion (Mittal et al., 2007). As a mechanistic model for antidiabetic activity of MO, it has been indicated that dark chocolate polyphenols (Grassi et al., 2005) and other polyphenols (Al-Awwadi et al., 2004; Moharram et al., 2003) are responsible for hypoglycemic activity. Moringa leaves are potent source of polyphenols, including quercetin-3- glycoside, rutin, kaempferol glycosides, and other polyphenols (Ndong et al., 2007). Thus, potential anti-diabetic activity of MO can be commercialized through the development of suitable technology with achieving anti-diabetic activity up to conventional drugs. Antioxidant activity MO is a rich source of antioxidant (Chumark et al., 2008). It has been reported that aqueous extracts of leaf, fruit and seed of MO act as an antioxidant (Singh et al., 2009). During a study reporting antioxidant property of freeze dried Moringa leaves from different extraction procedures, it was found that methanol and ethanol extracts of Indian origin MO have the highest antioxidant activity with 65.1 and 66.8%, respectively (Lalas and Tsaknis, 2002; Siddhuraju and Becker, 2003). It was also reported that the major bioactive compounds of phenolics, such as quercetin and kaempferol are responsible for antioxidant activity (Bajpai et al., 2005; Siddhuraju and Becker, 2003). During another study, quercetin and kaempferol have shown good antioxidant activity on hepatocyte growth factor (HGF) induced Met phosphorylation with IC50 value for 12 and ~6 μM/L, respectively (Labbe et al., 2009). Another recent study comparing palm oil with MO seeds for their antioxidant potential found out that MO seed are superiors for radical scavenging (Ogbunugafor et al., 2011). Hepatoprotective activity MO has shown significant hepatoprotective activity in
  • 4. several studies. MO leaves ethanolic extracts showed significant protection against liver damage induced by antitubercular drugs [isoniazid (INH), rifampicin (RMP), and pyrazinamide (PZA)] in rats. It was found that hepatoprotective activity of MO is medicated by its effect on the levels of glutamic oxaloacetic transaminase (aspartate aminotransferase), glutamic pyruvic transaminase (alanine aminotransferase), alkaline phosphatase, and bilirubin in the serum; lipids, and lipid peroxidation levels in liver (Pari and Kumar, 2002). Moreover, methanolic and chloroform extracts of MO leaves also showed significant protection against CCl4 induced liver damage in albino rats. Besides hepatoprotective activity of MO leaves, its root and flowers also possess strong hepatoprotective activity. Moringa flowers contain a well recognized flavonoid (Quercetin), which may be responsible for its potent hepatoprotective activity (Ruckmani et al., 1998; Selvakumar and Natarajan, 2008). In a recent study evaluating the effect of MO seed extract on liver fibrosis, it was found that MO seed extract has the ability to subside liver fibrosis. This study involved CCl4 induced liver fibrosis and concurrent administration of MO seed extract. MO seed extract control the elevation of serum aminotransferase activities and globulin level induced by CCl4. Moreover, immunohistochemical studies also showed that MO reduces liver fibrosis (Hamza, 2010). Antitumor activity MO has been found as a potent anticancer plant and several bioactive compounds with significant antitumor activity have been discovered from MO. Among bioactive compounds from MO, niazimicin, a MO leaves thiocarbamate was found to have potent anticancer activity (Guevaraa et al., 1999). Furthermore, niazimicin also shows the inhibition of tumor promoter teleocidin B- 4-induced Epstein-Barr virus (EBV) activation (Murakami et al., 1998). Another study involving 11 plants used in Bangladeshi folk medicine, MO was considered as potential source of anticancer compounds. During this study, the plant extract were analyzed for cytotoxicity through brine shrimp lethality assay, sea urchin eggs assay, hemolysis assay and MTT assay using tumor cell lines. The study also indicated the potential cytotoxic effects of MO leaf extract on human multiple myeloma cell lines (Costa-Lotufo et al., 2005; Parvathy and Umamaheshwari, 2007). Beside leaves, MO seed extracts also have anticancer activity through its effects on hepatic carcinogen metabolizing enzymes, and antioxidant property (Bharali et al., 2003). Antifertility activity MO plant also has pertinent antifertility activity. The aqueous extract obtained from root and bark of MO Farooq et al. 4371 showed post-coital antifertility effect in rat and also induced foetal resorption at late pregnancy (Prakash et al., 1987). Moreover, aqueous extract of MO roots was also evaluated for estrogenic, anti-estrogenic, pro-gestational and antiprogestational activities. This extract induces several consequences for affecting its antifertility property (Shukla et al., 1988). During another study analyzing anti reproductive potential of folk medicine plants, MO leaf extracts were found to be 100% abortive with doses equivalent to 175 mg/kg of starting dry material (Nath et al., 1992). Antispasmodic and antiulcer effects Moringa root and leaves contain several compounds with spasmolytic activity. These compounds include 4- (alpha- L-rhamnosyloxybenzyl)-o-methyl thiocarbamate which is possibly affected through calcium channel blockade, niazinin A, niazinin B, niazimicin, etc., with hypotensive and bradycardiac effect. The spasmolytic activity of different constituents support for traditional uses of this plant in gastrointestinal motility disorder (Gilani et al., 1994). MO methanolic extract is also capable in protecting experimental rats from gastric lesions induced by acetylsalicylic acid, serotonin and indomethacin. In addition, it also enhances healing process of chronic gastric lesions induced by acetic acid in experimental animals (Pal et al., 1995). Another study have reported the antiulcer effect of MO leaves aqueous extract on adult Holtzman albino rats (Debnath and Guha, 2007). Cardiac and circulatory stimulant In addition to earlier mentioned bradycardiac effect of MO leaves, all parts of MO are reported with somewhat cardiac and circulatory stimulant activity. Root bark of Moringa contains alkaloid moringinine which acts as cardiac stimulant through its effect on sympathetic nervous system (Duke, 2001). The aforementioned effects can also result due to the prevention of hyperlipidemia. It has been demonstrated that MO prevent hyperlipidemia in male Wister rat due to iron deficiency (Ndong et al., 2007). During a study performing comparison of MO leaf extract with antenolol (a selective β1 receptor antagonist drug, used for cardiovascular diseases) on serum cholesterol level, serum triglyceride level, blood glucose level, heart weight and body weight of adrenaline induced rats, it was found that MO leaf extract cause significant changes in cardiovascular parameters. This study reported MO leaf extract as hypolipidimic, lowering body weight, heart weight, serum triglyceride level and serum cholesterol level in experimental animals (Ara et al., 2008). In addition to the aforementioned studies, antiatheroscle-rotic and hypolipidaemic effect of MO leaves were also
  • 5. 4372 J. Med. Plants Res. Table 1. Major pharmaceutical components present in Moringa and their importance. S/N Compound Method used for detection Potential application Reference 1 Pterygospermin Solvent extraction followed by MIC analysis Antibacterial and fungicidal effects Rao et al. (1946) 2 4-(4'-O-acetyl-a-L-rhamnopyranosyloxy) benzyl isothiocyanate, 4-(a-L-rhamnopyranosyloxy) benzyl isothiocyanate, niazimicin, benzyl isothiocyanate, and 4-(a-L-rhamnopyranosyloxy) benzyl glucosinolate, Anthonine and Spirochin Solvent extraction followed by MIC analysis (Busani et al., 2012) Antibacterial Fahey (2005) and Nwosu and Okafor (1995) 3 Alkaloid Moringine Clinical study involving consumption of Moringa followed by antiasthmatic activity evaluation using spirometer Antiasthmatic Agrawal and Mehta (2008) and Kirtikar and Basu (1975) 4 Nitrile, mustard oil glycosides and thiocarbamate glycosides Bioassay directed isolation Hypotensive Anwar et al. (2007) and Faizi et al. (1995) 5 b-sitosterol Study involved consumption of Moringa leaves with cholesterol and subsequent measurement of cholesterol lowering activity (Ghasi et al., 2000). Cholesterol lowering effects Ghasi et al. (2000) 6 Dark chocolate polyphenols and other polyphenols Administration of MO leaves in diabetic and control rats and hypoglycemic activity evaluation and characterization of polyphenols using HPLC (Ndong et al., 2007). Hypoglycemic effects Grassi et al. (2005), Al- Awwadi et al. (2004) and Moharram et al. (2003) 7 Quecertin and kaempferol Solvent extraction followed by antioxidant activity analysis Antioxidant, hepatoprotective Bajpai et al. (2005), Siddhuraju and Becker (2003), Ruckmani et al. (1998) and Selvakumar and Natarajan (2008) 8 Niazimicin, Solvent extraction followed by in vitro anticancer activity Anticancer Guevaraa et al. (1999) 9 4- (alpha- L-rhamnosyloxybenzyl)-o-methyl thiocarbamate, niazinin A, niazinin B, niazimicin etc. Solvent extraction for purification of compounds followed by intravenous administration of each compound in anaesthetized rats and subsequent evaluation of their activity in experimental animals Spasmolytic, hypotensive and bradycardiac Gilani et al. (1994) analyzed in another study using simvastatin as control (Chumark et al., 2008). MO also causes cardio protective effects in isoproterenol (ISP)-induced myocardial infarction in male Wistar albino rats. It was reported that MO treatment plays favorable modulation on biochemical enzymatic parameters including, superoxide dismutase, catalase, glutathione peroxidase, lactate dehydrogenase, and creatine kinase-MB. Moreover, it also prevents histopathological damage and ultra-structure perturbation caused due to ISP induced myocardial infarction
  • 6. (Nandave et al., 2009). In ocular diseases Vitamin A deficiency is a major cause of blindness, which ranges from impaired dark adaptation to night blindness. Consumption of MO leaves, and pods and leaf powder which contain high proportion of vitamin A can help to prevent night blindness and eye problems in children. Ingesting drumstick leaves with oils can improve vitamin A nutrition and can delay the development of cataract (Pullakhandam and Failla, 2007). In fact the use of MO as a supplementary food was highly accepted for integrated child development scheme supplementary food (ICDS-SFP) for its potential as vitamin A source (Nambiar et al., 2003). Conclusion Medicinal potential of MO is enormous and difficult to cover in a single article, despite this current article provided glimpses of MO applications for performing appraisal of this promising nutrition and medicinal plant. 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