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PHARMACEUTICAL STANDARDIZATION
Year : 2013  |  Volume : 34  |  Issue : 1  |  Page : 103-107  

Standardization of Shadbindu Taila: An Ayurvedic oil based medicine


1 Associate Professor, Department of Botany and In-charge, Herbal Research Laboratory, Ramnarain Ruia College, Matunga, Mumbai, Maharashtra, India
2 Assistant Director, Institute for Advanced Training and Research in Interdisciplinary Sciences (Therapeutic Drug Monitoring Laboratory), Sion Koliwada, Mumbai, Maharashtra, India
3 Research Scholar, Herbal Research Laboratory, Ramnarain Ruia College, Matunga, Mumbai, Maharashtra, India
4 Research Scholar, Institute for Advanced Training and Research in Interdisciplinary Sciences (Therapeutic Drug Monitoring Laboratory), Sion Koliwada, Mumbai, Maharashtra, India

Date of Web Publication23-Jul-2013

Correspondence Address:
Sunita Shailajan
Herbal Research Lab, Ramnarain Ruia College, Matunga, Mumbai - 400 019, Maharashtra
India
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Source of Support: None, Conflict of Interest: None


DOI: 10.4103/0974-8520.115442

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   Abstract 

Shadbindu Taila (ST) is an Ayurvedic formulation used as a remedy for loosening of tooth, weakness of the eyesight, loss of hair, diseases of head, etc., Present study is an attempt to develop some newer approaches for the quality control and standardization of ST. Standardized operating procedure for the preparation of ST was developed in accordance with Ayurvedic Formulary of India. Preliminary phytochemical, physicochemical, and chromatographic evaluation of ST was carried out. Safety of ST was evaluated in terms of skin irritation test and presence of heavy metals. Chemical characterization of ST was done on the basis of kaempferol using validated -High Performance Thin Layer Chromatographic (HPTLC) method. ST did not show presence of any of the heavy metals analyzed and was found non-irritant on rabbit skin. The quality control parameters resulted after scientific evaluation of ST can be used as reference standard for quality control/assurance laboratory of a pharmaceutical firm in order to have a proper quality check over its preparation and processing.

Keywords: High performance thin layer chromatography, kaempferol, safety, Shadbindu Taila, standardization


How to cite this article:
Shailajan S, Menon SN, Tiwari BR, Singh AS. Standardization of Shadbindu Taila: An Ayurvedic oil based medicine. AYU 2013;34:103-7

How to cite this URL:
Shailajan S, Menon SN, Tiwari BR, Singh AS. Standardization of Shadbindu Taila: An Ayurvedic oil based medicine. AYU [serial online] 2013 [cited 2020 Oct 27];34:103-7. Available from: https://www.ayujournal.org/text.asp?2013/34/1/103/115442


   Introduction Top


Siddha Taila (medicated/processed oil) is prepared by protracted boiling of the Sneha Dravya (base oil) with prescribed Drava Dravya (liquid drug) and Kalka Dravya (drugs used as a fine paste) to dehydration or near dehydration. This process results in the transfer of some therapeutically active principles of the ingredients into the base oil. [1] Thus, Taila Paka Vidhi (traditional method of Taila preparation) assures the enrichment of Sneha dravya with the active principles of the ingredients.

Shadbindu Taila (ST) is a polyherbo-mineral Ayurvedic formulation prescribed widely for several conditions such as Danta Chalana (loosening of tooth), Drishti Daurbalya (weakness of the eyesight), Keshashata (loss of hair), Siroroga (diseases of head), etc., Following are the ingredients used for the preparation of ST: [2]

  • Sneha Dravya: Murcchita Krishna Tila Taila (MKTT) (processed oil from black seeds of Sesamum indicum L.)
  • Drava Dravya: Bhringa Rasa (juice obtained from macerated whole plant of Eclipta alba (L.) Hassk.) and Aja Paya (goat milk)
  • Kalka Dravya: A fine paste obtained from the powdered mixture of Eranda (Ricinus communis L.), Tagara (Valeriana wallichii DC.), Shatahva (Anethum sowa Roxb.), Jivanti (Leptadenia reticulata [Retz.] Wight and Arn.), Rasna (Alpinia galanga (L.) Swartz), Bhringa (Eclipta alba (L.) Hassk.), Vidanga (Embelia ribes Burm.f.), Yashti (Glycyrrhiza glabra L.) and Shunthi (Zingiber officinale Roscoe.) and Saindhava Lavana: Rock salt.
Quality control of ST remains an unexplored issue despite of its increase in the popularity. Thus, in the present work an attempt has been made to use some newer approaches for the standardization of ST with following objectives:

  • To develop Standardized Operating Procedure (SOP) for the preparation of ST.
  • To evaluate the physicochemical, phytochemical and safety profile of ST.
  • To carry out chemical characterization of ST on the basis of active principle(s) of the ingredients, using validated HPTLC method.

   Materials and Methods Top


Selection, processing and quality evaluation of the raw materials

As identification of the raw materials used to prepare any finished product is a must, all ingredients procured through local market were authenticated by Department of Botany (HRL/Auth/10/14-33). Raw materials complying pharmacopoeial quality were further used for ST preparation. Plant raw materials were dried in oven at 45°C, powdered, sieved (BSS sieve, 85-mesh) and stored in air tight containers.

Preparation of ST

The SOP for the preparation of ST involved following steps:

  • Preparation of MKTT: The reference from Ayurvedic Formulary of India [2] was followed for Murcchana of Krishna Tila Taila (KTT). Ingredients and parts used are mentioned in [Table 1]
    Table 1: List of ingredients for the Murchana of Krishna Tila Taila

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  • Preparation of Bhringa Rasa: Fresh juice obtained from macerated whole plant of E. alba was considered as Bhringa Rasa
  • Preparation of Kalka: Each Kalka Dravya (19.0 g powder) was taken in a vessel and mixed, followed by addition of sufficient amount of water until a uniform paste was obtained
  • Preparation of ST: As per [Table 2], MKTT (0.768 l) was indirectly heated on a mild flame (by placing a pan between burner and vessel to avoid direct heating) with Bhringa Rasa (3.072 l), Saindhava Lavana (19.0 g powder) and Kalka obtained from Kalka Dravya. Mixture was stirred intermittently till it became slimy. The heating was stopped and Aja Paya (3.072 l) was added. The mixture was kept standing overnight. Next day, the heating was continued till the mixture attained Sneha Siddhi Lakshana (completion test for chief desired characteristics) like Gandha-Varna-Rasotpatti (desired smell, color and taste), Shabdahinata (no cracking sound), Phenodgama (appearance of froth) and Vartivat Kalka (rolling of paste of herbal drugs between fingers). Finally, the mixture was filtered when hot through muslin cloth and stored in amber colored bottle until use. ST was prepared in three batches.
    Table 2: List of ingredients for the preparation of Shadbindu Taila

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Quality evaluation of ST

Quality of ST was analyzed by employing following quality control methods:

  • Preliminary phytochemical tests for major secondary metabolites [3]
  • Physicochemical analysis [4] : Comparative evaluation of ST with KTT and MKTT.
  • Extraction of phytochemical constituents from ST:

    For extraction 5 ml ST was mixed with 10 ml of 90% aqueous methanol solvent. The mixture was stirred for 1h by using a magnetic stirrer. Then it was stored in deep freezer at -20°C for 2 days. After 2 days, mixture was filtered through Whatman filter paper no. 41 and filtrate was used for HPTLC profiling.
  • HPTLC profile for estimation of kaempferol and method validation. [5]

    Equipment details: Sample spotter (CAMAG Linomat 5 with syringe [Hamilton]), Visualizer (CAMAG UV Cabinet), Phodocumentation unit (CAMAG Reprostar 3), Scanner (CAMAG Scanner 4 with winCATS planar chromatography manager software version 1.4.7), Wavelength (254 nm), Stationary phase (Merck silica gel 60 F 254 HPTLC pre-coated plates of 0.2 mm thickness with aluminium sheet support), Mobile phase (n-hexane: ethyl acetate: formic acid (6.0:4:0.2, v/v/v)].
  • Safety evaluation: Heavy metal analysis using - Inductively Coupled Plamsa-Optical Emission Spectroscopic (ICP-OES) technique and skin irritation test in animals. [6],[7]
Statistical analysis

Microsoft Excel-2007 was used to determine mean, standard deviation, relative standard deviation and mean difference during the analysis.


   Results Top


A bio-analytical approach was employed for the quality control and standardization of ST. SOP for the preparation of ST was developed and ST was prepared in three batches. [Table 3], [Table 4], [Table 5], [Table 6], [Table 7] and [Table 8] provide the results of the analysis carried out on ST.
Table 3: Results of preliminary phytochemical analysis of Shadbindu Taila

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Table 4: Results of physicochemical analysis of Krishna Tila Taila, Murcchita Krishna Tila Taila and Shadbindu Taila

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Table 5: Results of HPTLC evaluation of Shadbindu Taila

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Table 6: Results of HPTLC method validation for the estimation of kaempferol

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Table 7: Results of heavy metal analysis of Shadbindu Taila

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Table 8: Results of skin irritation potential of Shadbindu Taila on rabbit skin

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   Discussion Top


Quality assurance is an integral part of all systems of medicine to ensure the quality medicament. Various multi-disciplinary and bio-analytical approaches such as development of SOP, [8] preliminary phytochemical and physicochemical evaluation, [9] chromatographic evaluation, [10] safety evaluation, [11] efficacy evaluation [12] etc., have been employed and reported for the scientific evaluation of various traditional formulations. In the present research work, only suitable and available techniques were selected for the quality evaluation of ST.

SOP of ST was prepared and ST was subjected to various quality methods to standardize for further studies and utility. Murchhana of KTT and preparation of ST were carried out till the achievement of desired Sneha Siddhi Lakshana. Murcchana resulted in the elimination of undesired smell and incorporation of color in KTT (pale yellow color of KTT changed to orange-red because of Manjishtha) and the entire process took about 40-42 h with the average recovery of 79.75 ± 0.08%. All three batches of ST were prepared in between 21 h and 22 h with the average recovery of 80.26 ± 1.01%. ST was found more viscous than MKTT, probably because of goat milk.

During the Taila Murcchana and preparation of ST, mild and indirect heating (peak temperature of 90°C-95°C) was carried out along with the continuous stirring for proper extraction, to lessen the possible chances of degradation of some active constituents, which may be decomposed due to hydrolysis and to facilitate the natural circulation evaporation.

Qualitative tests are used to detect the presence of some major phytochemicals which play a very important role in the expression of biological activity. [13] Almost all the phytochemical groups analyzed were found to be available in ST except resins and steroids. Presence of such secondary metabolites into ST assures the traditional process of medicating the oils.

The physicochemical parameters of KTT, MKTT and ST were compared. In comparison with KTT, acid value, saponification value and unsaponifiable matter of MKTT and ST were increased while the iodine and peroxide values were decreased. There was no change observed in the refractive index and specific gravity of KTT, MKTT and ST; while variations in optical rotation were observed. The results were in compliance with some recently published reports on physicochemical analysis of some Ayurvedic Taila. [8],[11] These observations suggest that Taila Paka Vidhi affects physicochemical parameters of Sneha Dravya during processing.

The ingredients of ST possess potential therapeutic agents such as kaempferol, luteolin, embelin, lupeol, β-sitosterol, etc., Presence of these markers in ST was evaluated using HPTLC technique. Extraction of these markers from ST was found to be a daunting task because of its complex oil-based matrix and herbo-mineral nature. This created a major problem during development of phytochemical fingerprint and detection/separation of marker compound(s). Hence, a reported method for the extraction of phytochemical constituents from Taila[1] was modified and optimized in order to develop phytochemical fingerprint and to separate active principles from ST.

As, kaempferol is reported to possess anticancer, antioxidant, anti-inflammatory, analgesic and antimicrobial activity, [14] a HPTLC method was developed in order to separate it from other interfering phytochemical constituents of ST. This was achieved on HPTLC plates using n-hexane: ethyl acetate: formic acid (6.0:4:0.2, v/v/v) as a mobile phase. In HPTLC of ST, five major spots were observed at 254 nm [Table 5], [Figure 1] indicating its possible compounds of the matrix which may be responsible for its therapeutic activity. Among these spots, kaempferol was detected at R f = 0.32 and its identity in Taila matrix was confirmed by overlay and its UV absorption spectra with that of the standard [Figure 1]. Using the regression equation, the exact content of kaempferol was determined. The method was found rapid, specific, precise, sensitive and rugged during validation experiment. The developed HPTLC fingerprint of the drug along with the presence of kaempferol in it within the specified limits can be useful to verify the quality and purity of ST. This method can be applied to various polyherbal formulations of any matrices containing kaempferol.
Figure 1: Kaempferol in Shadbindu Taila (ST) at UV-254 using HPTLC. (a) Plate photo (b) Overlay (c) absorption spectra of ST (A) and kaempferol (B)

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ST was analyzed for the presence of some heavy metals which were found to be below the detection limits of the instrument. Topical application of ST on rabbit skin did not show any adverse effects and dermal irritation which was well supported by the value of primary irritation index. Heavy metal analysis and skin irritation study revealed that ST has adequate safety margin to be used on human skin.

The quality control parameters resulted after scientific evaluation of ST can be used as reference standard for quality control/assurance laboratory of a pharmaceutical firm in order to have a proper quality check over its preparation and processing. Use of such scientific techniques routinely may lead to standardization of ST to a certain extent and would definitely help in building confidence in its use.


   Conclusion Top


It can be concluded that the bio-analytical approaches used in the present study is useful in the quality control and standardization of ST. As ST contains a wide range of phytochemical components, it is needed to validate its therapeutic utility through preclinical and clinical studies.


   Acknowledgment Top


We are thankful to AYUSH, Ministry of Health and family Welfare, Government of India for financial assistance under the APC Scheme and Mr. Harshvardhan Joshi for technical assistance.

 
   References Top

1.Lahorkar P, Ramitha K, Bansal V, Anantha Narayana DB. A comparative evaluation of medicated oils prepared using Ayurvedic and modified processes. Indian J Pharm Sci 2009;71:656-62.  Back to cited text no. 1
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2.Anonymous. The Ayurvedic Formulary of India. Part I, 2 nd revised English ed. New Delhi: Government of India, Ministry of Health and Family Welfare, Department of Indian System of Medicine and Homeopathy; 2003. p. 154, 351.  Back to cited text no. 2
    
3.Khandelwal KR. Preliminary phytochemical screening. Practical Pharmacognosy Techniques and Experiments. 19 th ed. Pune: Nirali Prakashan Publishers; 2008. p. 149-56.  Back to cited text no. 3
    
4.Anonymous. The Indian Pharmacopoeia, Government of India, Ministry of Health and Family Welfare. 6 th ed., Vol. I. Ghaziabad: The Indian Pharmacopoeia Commission; 2010. p. 201.  Back to cited text no. 4
    
5.Reich E, Schibli A. High-performance thin-layer chromatography for the analysis of medicin1al plants. New York: Thieme Medical Publishers; 2007.  Back to cited text no. 5
    
6.Marin S, Lacrimioara S, Cecilia R. Evaluation of performance parameters for trace elements analysis in perennial plants using ICP-OES technique. J Plant Develop 2011;18:87-93.  Back to cited text no. 6
    
7.Shailajan S, Menon S, Pednekar S, Singh A. Wound healing efficacy of Jatyadi Taila: In vivo evaluation in rat using excision wound model. J Ethnopharmacol 2011;138:99-104.  Back to cited text no. 7
[PUBMED]    
8.Shailajan S, Menon S, Trivedi M, Tiwari B. Quality assessment of a traditional oil based Ayurvedic formulation - Yashtimadhuka Taila. J Pharm Res 2012;5:1112-5.  Back to cited text no. 8
    
9.Yadav SS, Galib, Patgiri BJ, Shukla VJ, Prajapati PK. Standardization of Shirishavaleha with reference to physico-chemical characteristics. AYU 2011;32:560-5.  Back to cited text no. 9
[PUBMED]  Medknow Journal  
10.Shailajan S, Menon SN, Singh A. Quantitative analysis of piperine from Ayurvedic polyherbal formulation using reverse phase high performance liquid chromatography. Int J Pharma Bio Sci 2009;1:1-10.  Back to cited text no. 10
    
11.Shailajan S, Singh A, Tiwari B. Quality control and standardization of an Ayurvedic Taila formulation. Int J Biomed Res Anal 2010;1:78-81.  Back to cited text no. 11
    
12.Thanki KH, Joshi NP, Shah NB. A comparative study of Anu Taila and Mashadi Taila Nasya on Ardita (Facial paralysis). AYU 2009;30:201-4.  Back to cited text no. 12
  Medknow Journal  
13.Kalsariya BD, Patgiri BJ, Prajapati PK. Standard manufacturing procedure for syrup and tablet forms of Jwarahara Dashemani. Ayu 2010;31:255-9.  Back to cited text no. 13
[PUBMED]  Medknow Journal  
14.Singh B, Mungara P, Nivsarkara M, Anandjiwala S. HPTLC densitometric quantification of glycirrhizin, glycirrhetinic acid, epigenin, kaempferol and qercetin from Glycirrhiza glabra. Chromatographia 2009;70:1665-72.  Back to cited text no. 14
    


    Figures

  [Figure 1]
 
 
    Tables

  [Table 1], [Table 2], [Table 3], [Table 4], [Table 5], [Table 6], [Table 7], [Table 8]


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