About Author: 1) Pankaj H. Chaudhary, M.Pharm
Dept. of Pharmacognosy, Government College of Pharmacy,
Kathora Naka, Amravati – 444604, Maharashtra, INDIA.
2) Somshekhar S. Khadabadi*. M.Pharm., PhD.
Dept. of Pharmacognosy, Government College of Pharmacy,
Kathora Naka, Amravati – 444604, Maharashtra, INDIA.
Abstract
In the present study, the aphrodisiac activity of Bombax ceiba Linn. (Bombacaceae) root extract was investigated. The extract (400 mg/kg body wt./day) was administered orally by gavage for 28 days. Mount latency (ML), intromission latency (IL), ejaculation latency (EL), mounting frequency (MF), intromission frequency (IF), ejaculation frequency (EF) and post-ejaculatory interval (PEI) were the parameters observed before and during the sexual behavior study at day 0, 7, 14, 21, and 28. The extract reduced significantly ML, IL, EL and PEI (p < 0.05). The extract also increased significantly MF, IF and EF (p < 0.05). These effects were observed in sexually active and inactive male mice.
Reference ID: PHARMATUTOR-ART-1120
Introduction
Aphrodisiacs are substances that stimulate/increase sexual desire and performance. There are numerous reports of aphrodisiac activity attributed to plants (Chandler, 1988; Sreedhar et al. 1993; Ananthkumar et al. 1994; Subramoniam et al. 1997; Singh and Mukerjee, 1998; Noumi et al. 1998; Sureshkumar et al. 2000), isolated constituents (Waddell and Ibach, 1989) and synthetic compounds (Dallo et al. 1986). Bombax ceiba is reported to possess antihypertensive, antioxidant, antidiabetic, aphrodisiac and uterine tonicity properties (Kirtikar & Basu, 1994; Anonymous, 2001). B. ceiba is also claim (Anonymous, 2003)to use in the treatment of diarrhea, dysentery, menorrhagia, styptic and for wounds. These claims are based largely on subjective opinion rather than scientific observation. The present study was undertaken to investigate the aphrodisiac activity of B. ceiba at doses of 400 mg/kg body wt. in male mice.
Materials and Methods
Plant material and preparation of extracts
Roots of Bombax ceiba were collected from Govt. Vidharbha Institute of Science & Humanities localities, Amravati (Maharashtra). The plant was identified and authenticated by Dr. Vishal R. Marathe of Department of Botany, Shri Shivaji Science College, Amravati and dried in the shade at room temperature. Dried roots were powdered in grinder and powder material (100 g) was suspended in 1 liter mixture of ethanol: distilled water (70:30). The suspension was stirred at 40 °C for 24 h and heated at 50 °C for 2 h. The extract was filtered then and dried (2.4 % w/w yield).
Animals
Adult Swiss albino mice (weight – 25 to 35 gm) of either sex were used for the study. The animals were fed with standard animal feed and water ad libitum. The animals were housed at a temperature of 25 ± 1 0C with a reversed light dark cycle (light from 2300 h to 1100 h) and relative humidity of 45–55 %. The study was performed as per the protocols and recommendation of the Institutional Animal Ethics Committee, Govt. College of Pharmacy, Amravati.
Male mice (n = 5/group) were trained for sexual experience. To provide sexual experience, each male mice was allowed 30 min exposure to a female mice (used as mating stimulus) in behavioral estrous, several days before testing for copulatory performance in a transparent arena. The animal were tested 3 times over a 10 day period for copulatory behavior and divided into active and inactive groups. Sexually active animals were divided into control (saline), Chlorophytum boriviliannum treated (400 mg/kg body wt.) and Bombax ceiba treated (400 mg/kg body wt.) groups. The animals that did not show any sexual interest during training were considered the inactive group that was administrated Bombax ceiba (400 mg/kg body wt.).
Female mice were artificially brought into estrous by the administration of a single subcutaneous dose of 2 µg/kg body wt. of estrogen benzoate and 500 µg/kg body wt. progesterone 48 h and 6 h before the copulatory study (S. Ramachandran et al.2004).
Sexual behavior study
The following guidelines (Hart et al. 1983; Islam et al. 1991) were followed in the study: a) males were kept individually but females were kept in groups; b) training of each male for 15 min at a time was performed until sexual behavior was elicited and when the behavior was noticed, males were exposed to receptive females (1 male with 5 females); c) repeated training to overcome the lack of sexual response in the presence of observers; d) the study was conducted in a silent room under dim red light; e) any jerking movement of the mating area was avoided to enable the mice to chase each other; and g) cleaning of the mating area was performed after each trial, since the urine trails left by one mice might alter the sexual behavior of the next mice.
NOW YOU CAN ALSO PUBLISH YOUR ARTICLE ONLINE.
SUBMIT YOUR ARTICLE/PROJECT AT articles@pharmatutor.org
Subscribe to Pharmatutor Job Alerts by Email
FIND OUT MORE ARTICLES AT OUR DATABASE
Bombax ceiba (400 mg/kg body wt. /day) and all ready standardized alcoholic roots extract from Green Chem Bangalore of Chlorophytum boriviliannum(400 mg/kg body wt. /day) in distilled water were administered for 28 days orally by gavages. Chlorophytum boriviliannum served as herbal standard (Kenjale R. et al. 2008; Thakur M. et al. 2009).The control groups received 1 ml saline. Each group consisted of six animals (1 male & 5 female).The following parameters of the copulatory behavior were recorded with help of video tracking media (I) mount latency (ML) – time taken for the first mount following the introduction of females; (II) intromission latency (IL) – time taken for first intromission following introduction of the female; (III) ejaculation latency (EL) – time interval between first intromission and first ejaculation; (IV) mount frequency (MF) – no. of mounts observed in 30 min; (V) intromission frequency (IF) – No. of intromission observed in 30 min; (VI) ejaculation frequency (EF) No. of ejaculations observed in 30 min; (VII) post-ejaculatory interval (PEI) – the time between the occurrence of ejaculation and the resumption of sexual activity, as indicated by next intromission.The copulatory behavior study was conducted at 0, 7th, 14th, 21st & 28th days.
Acute toxicity tests
To determine acute toxicity, if any, dose of 0, 0.5, 1.0 and 2 g/kg. (p.o) respectively of the ethanol: water (70:30) Bombax ceiba roots extract were given to 4 groups each containing 6 mice. The control mice received saline in an identical manner. The mice were observed continuously for 1hr for any gross behavioral changes & deaths, if any and intermittently for the next 6 hrs and then again at 24 hrs after dosing. The behavior parameters observed were convulsion, hyperactivity, sedation, grooming, loss of righting reflex & increased respiration (Sureshkumar P.K. et al. 2000).
Statistical Analysis
All the results are expressed as the mean ± S.E.M. The data were analyzed for statistical significance by one-way analysis of variance (ANOVA) followed by Tukey test using computerized Graph Pad Prism, version 4.03 software (Graph Pad Software Inc). Values of p < 0.05 were considered statistically significant.(*p < 0.05, **p < 0.01, ***p < 0.001)
Results and Discussion
The observation of the sexual behavior study shows that Bombax ceiba extract reduced ML, IL, EL and PEI significantly in both active and inactive male mice. Bombax ceiba extract also increased MF, IF and EF significantly in both active and inactive male mice. All these effects were observed from the 21st and 28th days of study.
Sexually active and inactive animals showed increased and improved sexual performance, when Bombax ceiba roots extract (400 mg/kg body wt.) was administered for a period of 21 to 28 days. The present study confirmed the claims of Bombax ceiba as an aphrodisiac agent.
In the present study, the hydro-alcohol extract of this drug was found to be devoid of any general conspicuous short term toxicity. Long term toxicity studies as well as systemic toxicity, if any, remain to be studied. However, since this drug is used in ethnomedical practices without any recorded toxicity, this plant is likely to be a safe drug.
Generally sexual behaviors are enhanced by elevated testosterone levels. Drug induced changes in neurotransmitter levels or their action in the cells could also change sexual behavior. In this connection it should be remembered that on ethnomedical practices this herb is also considered as a nervous stimulant. Active investigations will help to explore the possible mechanisms of action.
The brain area most associated with sexual behavior is the limbic system. Research with various animal and human models indicates a relationship between brain dopamine, 5HT and sexual behavior (Singh and Mukherjee, 1998). Both dopamine and 5HT are implicated in depression. The relationship of dopamine to human sexual behavior is supported by reports of per-sexuality behavior induced by L-dopa in parkinsonian patients. Stimulants and antidepressants are known to effect libido, erection, ejaculation and orgasm. It is also suspected that monoamines (Waddell and Ibach, 1989) play a crucial role in the regulation of sexual behavior, particularly that of dopaminergic transmission in the facilitation of masculine activity. Thus, both dopaminergic and adrenergic receptors are involved in sexual behavior.
Bombax ceiba roots extract (400 mg/kg body wt.) has comparative aphrodisiac activity with that of Chlorophytum boriviliannum roots extract in inactive mice; this suggested that Bombax ceiba will be the best alternative to Chlorophytum boriviliannum as compare to price of row material Bombax ceiba roots (Rs:120/- per kg) where as Chlorophytum boriviliannum roots (Rs:1080/- per kg).
Acknowledgements
The authors thank to the Principal, Prof. I. A. Farooqui and Dr. Pallavi D. Rai of Govt. College of Pharmacy for valuable guidance and providing the facilities for the present study.
References
Ananthakumar KV, Srinivasan KK, Shanbhag T, Rao SG (1994) Aphrodisiac activity of the seeds of Mucuer pruriens. Indian Drugs 31: 321–327
Anonymous (2001) The Useful Plants of India. National Institute of Science Communication, CSIR, New Delhi, India 76
Anonymous (2003) The Wealth of India, Vol-2. Publication and Information Directorate, CSIR, New Delhi, India 177–184
ChandlerRF (1988) Ginseng-Aphrodisiac. Can Pharm J 121: 36-38
Dallo J, Lekka N, Knoll J (1986) Ejaculatory behavior of sexually sluggish male rats treated with (–) deprenyl, apomorphine, bromocriptine and amphetamine. Pol J Pharmacol Pharm 38: 251–255
Hart BL, Wallach SJR, Melese-D’Hospital PY (1983) Difference in responsivess to testosterone of penile reflexes and copulatory behavior of male rats. Hormone and Behavior 7: 274-283
Islam MW, Tasiq M, Ageel AM, Al-Said MS, Al-Yhua AM (1991) Effects of Salvia haematodes on sexual behavior of male rats. J Ethnopharmacol 33: 67–72
Kenjale R, Shah R, Sathaye S. (2008) Effects of Chlorophytum borivilianum Safed Musli on sexual behavior and sperm count in male rats. Phytother Res. 22: 796-801
Kirtikar K, Basu B, (1994) Indian Medicinal Plants 2nd edition. Bishen Singh Mahendra Pal Singh New Delhi 117-121
Noumi P, Zollo PHA, Lontsi D (1998) Aphrodisiac plants used in Cameroon. Fitoterapia 69: 128–134
S. Ramachandran, Y. Sridhar, S. Kishore Gnana Sam, M. Saravanan, J. Thomas Leonard, N. Anbalagan and S. K. Sridhar (2004) Aphrodisiac activity of Butea frondosa Koen. ex Roxb. extract in male rats. Phytomedicine 11: 165–168
Singh G, Mukerjee T (1998) Herbal aphrodisiacs: a review. Indian Drugs 34: 175–182
NOW YOU CAN ALSO PUBLISH YOUR ARTICLE ONLINE.
SUBMIT YOUR ARTICLE/PROJECT AT articles@pharmatutor.org
Subscribe to Pharmatutor Job Alerts by Email
FIND OUT MORE ARTICLES AT OUR DATABASE
Sreedhar M, Srinivasan KK, Shanbhag T, Rao SG (1993) Aphrodisiac activity of Ipomea digita. Indian Drugs 30: 165–169
Subramoniam M, Madhavachandran V, Rajesekharan S, Pushpangadan P (1997) Aphrodisiac property of Trichopus zeylanicus extract in male mice. J Ethnopharmacol 57: 21–27
Sureshkumar PK, Subramoniam A, Pushpangadan P (2000) Aphrodisiac activity of Vanda tessellata (Roxb) hook. ex don extract in male mice. Indian J Pharmacol 32: 300–304
Thakur M, Chauhan NS, Bhargava S, Dixit VK (2009) A Comparative Study on Aphrodisiac Activity of Some Ayurvedic Herbs in Male Albino Rats. Arch Sex Behav 38:1009-15
Waddell TG, Ibach DM (1989) Modern chemical aphrodisiac Indian J Pharm Sci 51: 79–82
Table 1 Sexual behavior study of Bombax ceiba
|
S.N. |
Groups |
Para |
Mean ± SEM |
||||
|
0 day |
7th day |
14th day |
21st day |
28th day |
|||
|
1 |
Active (Control) |
ML |
270±2.12 |
275±2.48 |
260±2.19 |
285±4.02 |
265±4.56 |
|
MF |
31±0.91 |
28±0.91 |
35±1.29 |
25±1.29 |
33.5±1.19 |
||
|
IL |
333±2.38 |
338.75±3.25 |
301±2.61 |
370±3.85 |
310±4.56 |
||
|
IF |
10±0.91 |
9±0.91 |
12±.081 |
8±0.91 |
10±0.91 |
||
|
EL |
930±2.19 |
980±2.38 |
850±6.45 |
1020±4.56 |
850±6.45 |
||
|
EF |
1.5±0.09 |
1.2±0.09 |
1.8±0.18 |
1.2±0.12 |
1.6±0.09 |
||
|
PEI |
242.5±2.78 |
248±3.85 |
215±4.20 |
270±4.56 |
220±3.85 |
||
|
2 |
Active (C. boriviliannum 400mg/kg body wt.) |
ML |
280±2.19 |
270±2.12 |
253±5.17*** |
205±4.39*** |
178±2.94*** |
|
MF |
28±0.91 |
30±0.91 |
32±0.91 |
43±1.29*** |
53±1.47*** |
||
|
IL |
362±2.19 |
350±4.56 |
338±1.82*** |
281±4.41*** |
231±2.04*** |
||
|
IF |
8±0.40 |
9±0.91 |
10.75±0.85 |
16±0.81*** |
21±0.91*** |
||
|
EL |
1000±17.55 |
950±2.44** |
925±4.20*** |
871±2.19*** |
809±4.41*** |
||
|
EF |
1.3±0.09 |
1.4±0.09 |
1.5±0.09 |
1.7±0.09* |
2.3±0.09*** |
||
|
PEI |
260±2.2.19 |
248±3.10 |
237±3.10*** |
208±3.29*** |
167±3.10*** |
||
|
3 |
Active (B. ceiba 400mg/kg body wt.) |
ML |
268±3.65 |
258±2.19 |
247±3.36* |
208±0.23*** |
157±2.38*** |
|
MF |
32±0.91 |
35±0.81 |
38±1.82* |
45±1.22*** |
55±0.91*** |
||
|
IL |
330±2.19 |
322±1.82 |
310±2.61*** |
274±2.19*** |
202±2.73*** |
||
|
IF |
11±0.91 |
13±0.91 |
15±0.91* |
18±0.91*** |
22±0.91*** |
||
|
EL |
900±4.56 |
850±1.82*** |
801±2.58*** |
770±4.20*** |
704±4.20*** |
||
|
EF |
1.4±0.09 |
1.6±0.04 |
1.7±0.09 |
1.9±0.09** |
2.5±0.09*** |
||
|
PEI |
230±2.04 |
205±4.26** |
185±4.02*** |
170±4.56*** |
151±3.85*** |
||
|
4 |
Inactive (B .ceiba 400mg/kg body wt.) |
ML |
325±2.38 |
315±6.24 |
299±2.73** |
270±4.20*** |
199±4.56*** |
|
MF |
21±1.08 |
20.5±1.32 |
24±0.91 |
28±1.68** |
40±0.81*** |
||
|
IL |
380±2.19 |
369±2.38 |
358±4.56*** |
308±2.97*** |
248±1.70*** |
||
|
IF |
4.75±1.10 |
6±0.91 |
7±0.91 |
10±0.91* |
14±0.91*** |
||
|
EL |
1200±36.5 |
1120±8.41* |
1005±4.41*** |
943±3.76*** |
898±1.82*** |
||
|
EF |
1.1±0.09 |
1.2±0.04 |
1.3±0.07 |
1.5±0.09* |
1.9±0.09*** |
||
|
PEI |
325±21.89 |
280±5.94 |
249±2.08* |
252±24.83*** |
178±1.82*** |
||
NOW YOU CAN ALSO PUBLISH YOUR ARTICLE ONLINE.
SUBMIT YOUR ARTICLE/PROJECT AT articles@pharmatutor.org
Subscribe to Pharmatutor Job Alerts by Email
FIND OUT MORE ARTICLES AT OUR DATABASE
.png)
