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Advances in Animal and Veterinary Sciences

AAVS_8_4_360-363

 

 

Short Communication

 

Synthesis of (Hydroxylapatite: Silver) Mixing with Coaltar for Psoriasis Therapy

 

Asmaa Hadi Mohammed1, Marwa Abdul Muhsien Hassan1*, Majid Shanon Khalaf2

1Department of Physics, College of Science, Mustansyriah University, Baghdad, 00964, Iraq; 2Ministry of Science and Technology, Department of Nuclear, Biological and Military Waste, Iraq.

 

Abstract | Psoriasis is a critical and serious disease which can affect the immunity system of the body resulting in a rapid buildup of skin cells. Interests come over this research to know the role of nanomaterial in Psoriasis treatment, so here, Nano biological-materials were prepared from different natural resources for both Hydroxyapatite and Silver using a simple chemical method. The nano products have been characterized using various techniques to measure the structural properties and the grain size. To manifest the appropriate preparation conditions for treating psoriasis, the nano product has been mixed with the coaltar.

 

Keywords | Hydroxylapatite, Ag, Coal tar and psoriasis treatment

 

Received | September 28, 2019; Accepted | March 03, 2020; Published | March 20, 2020

*Correspondence | Marwa Abdul Muhsien Hassan, Department of Physics, College of Science, Mustansyriah University, Baghdad, 00964, Iraq; Email: [email protected]

Citation | Mohammed AH, Hassan MAM, Khalaf MS (2020). Synthesis of (Hydroxylapatite: Silver) mixing with coaltar for psoriasis therapy. Adv. Anim. Vet. Sci. 8(4): 360-363.

DOI | http://dx.doi.org/10.17582/journal.aavs/2020/8.4.360.363

ISSN (Online) | 2307-8316; ISSN (Print) | 2309-3331

Copyright © 2020 Mohammed et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

 

Introduction

 

Psoriasis is a common skin disease that affects the life cycle of skin cells (Jones et al., 2003; Jump, 2013; Menter et al., 2008; Ely and Seabury, 2010; Boehncke and Schön, 2015). As a result of psoriasis, cells quickly build up on the surface of the skin to form thick silver scales and itchy, dry and red layers, sometimes causing pain (Jain, 2012; Parisi et al., 2013; Tamparo, 2011). Psoriasis is a stubborn disease that lasts for a long time (chronic disease). There are periods in which the symptoms of psoriasis improve and alleviate, while psoriasis intensifies in other periods (Palfreeman et al., 2013; Colledge et al., 2010; Zattra et al., 2012; Stanway, 2014; James et al., 2005; Robinson et al., 2012). For some patients, psoriasis is a nuisance. For others, it is possible to cause disability, especially when they are associated with arthritis (Arthritis). Psoriasis is not cured, but psoriasis treatment can significantly improve (Raychaudhuri et al., 2014; Weigle and McBane, 2013; Gudjonsson et al., 2012; Gelmetti, 2009; Yesudian et al., 2012; Ship et al., 2008). Lifestyle measures, such as the use of cortisone ointment, moderate skin exposure to the sun in a controlled manner, can improve psoriasis symptoms.

 

Materials and Methods

 

The method of co-precipitation was used to synthesize hydroxyapatite (HAp) crystals. A solution of 0.6 M H3PO4 under continuous stirring at room temperature was added to a 1 M Ca(OH)2 and 0.5 M Ag(NO3)2 aqueous solution. By adding an ammonia solution, the final pH was adjusted to 11. The resulting precipitate was aged in stirring for 24 hours. Centrifugation collected the obtained white precipitates and washed repeatedly with distilled water. The product was dried for 24 hours in an oven at 80 oC. The obtained HAp crystals were ground with a mortar and pestle, then they were sieved at 45 μm. Finally, in a conventional furnace, the HAp crystals were calcinated for 2 hours in an air atmosphere at 1200 oC. Then the HAp: Ag mixing 50:50 percent with coaltar.

 

Results and Discussion

 

The chemical analysis results showed that the stone coaltar is a very pure containing an element (C, O, Al and Si) as shown in Figure 1A. Where the proportion of carbon element was the highest value in the coaltar and this confirms the purity of the material used for treatment after mixing with the prepared hydroxyapatite: Ag nanomaterial. The result of the energy-dispersive X-ray spectroscopy (EDXS) showed that only Ca, P, Ag and O were composed as synthesized HAp: Ag nanorods. The energy-dispersive X-ray spectroscopy (EDXS) detects no other peaks related to any impurity. Semiquantitative analysis shows that the Ca/P molar ratio is approximately 1.67 and closer to the theoretical value of 1.67, confirming that the nanorods are hydroxyapatite treated at 1200 °C as shown in Figure 1B. The C-related peak comes from the FESEM substratum.The results of the FESEM-EDXS analysis (Figure 1) showed that the nano-pure and doped HAp Ca / P ratio investigated in this study varies with an average of 1.67 between 1.46 and 2.01. The main difference between synthetic and natural hydroxyapatite is that the synthetic material showed a higher Ca/P ratio. While the former was closer to the hydroxyapatite stoichiometric. It should be noted that the semi-quantitative analysis of the Ca/P ratio of hydroxyapatite using SEM-EDXS has a technical problem. In other words, the X-ray intensity of phosphorus decreases faster than that of calcium during the analysis at a fixed current density and increasing irradiation time, resulting in an increase in the Ca / P ratio at a high dose of electron irradiation. Thus, the accelerating voltage was set at 15 kV in this study and the analysis was carried out at a low irradiation time to overcome the above problem.

 

 

Figure 2 shows SEM images of 600 oC, 800 oC, 900 oC and 1200 oC heat-treated samples respectively. The powder obtained at temperatures between 600 oC and 800 oC after heat-treatment consists of well-defined, randomly oriented elongated nanorods. As the temperature raises to 900 oC, elongated nanorod shapes are maintained, but sphere-like structures are observed for temperatures above 900 oC. Figure 2 shows the mean nanorod diameter value versus the temperature of the heat treatment. The average diameter of the nanorods takes values in a rather narrow interval for temperatures between 600 oC and 800 oC, which increases with increasing temperature. Although the average diameter shows a slight decrease at 900 oC, this is not a major problem. On the other hand, the mean diameter increases sharply for sintering temperatures above 900 oC as the temperature rises, whereby the diameter values are spreading larger. The large spread may be due, as can be observed in Figure 2, to the partial or incipient fusion of adjacent nanorod surfaces. The length of nanorods ranges from 100 nm to about 200 nm, but no correlation could be established between the length and the sintering temperature.

 

 

 

Treatment of psoriasis using (Hydroxyapatite: Silver) mixing with coaltar

Psoriasis is caused by a cause related to the immune system, specifically a specific type of white blood cell called (T cell) lymphocytes as shown in Figure 3. Normally, these cells travel throughout the body to find and control foreign substances, such as bacteria and viruses. But in psoriasis patients, these lymphocytes accidentally attack healthy skin cells. Too effective T lymphocytes provoke various reactions in the immune system, such as enlargement of blood vessels around the skin layers and increasing amounts of other blood cells that can penetrate the epidermis (thin outer layer of skin-Epidermis). As a result of these changes, the body produces more healthy skin cells, more T lymphocytes and other white blood cells. As a result, new skin cells reach the outer layer of skin very quickly in a few days, rather than weeks as is normal. But dead skin cells and white blood cells cannot rapidly fall off, so they accumulate in thick crust layers on the surface of the skin. This process can be stopped, mostly, by treatment. It is not clear exactly why T-lymphocyte activity is disrupted in psoriasis patients, and researchers believe that both genetic and environmental factors play a role.

 

 

The desired goals of psoriasis treatment using (hydroxyapatite: Ag nanoparticles mixing with coal tar)

  1. 1. Stop the process that leads to the production of excess skin cells, which reduces inflammation and the formation of layers.
  2. 2. Remove the dandruff and make the skin soft.

 

Conclusions

 

The use of a chemical method in the preparation of biological material in the form of nano-rod and mixing with coal tar and used to eliminate psoriasis in humans.

 

Authors Contribution

 

All authors contributed equally.

 

Conflict of interest

 

1- Psoriasis has increased worldwide.

2- Difficulty treating psoriasis once and for all using traditional treatments.

3- The possibility of using nanomaterials to improve the action of coal tar for the ultimate treatment of psoriasis.

 

REFRENCES

 

  • Boehncke WH, Schön MP (2015). Psoriasis. Lancet (London, England). 386: 983–94.  PMID 26025581. https://doi.org/10.1016/S0140-6736(14)61909-7
  • Colledge NR, Walker BR, Ralston SH (2010). Davidson’s principles and practice of medicine. (21st ed.). Edinburgh: Churchill Livingstone/Elsevier. pp. 1260–1. ISBN 978-0-7020-3084-0. https://doi.org/10.1016/B978-0-7020-3085-7.00007-9
  • Ely JW, Seabury SM (2010). The generalized rash: part II. Diagnostic approach. Am. Fam. Physician. 81(6): 735–9. PMID 20229972.
  • Gelmetti C (2009). Therapeutic moisturizers as adjuvant therapy for psoriasis patients. Am. J. Clin. Dermatol. 10(Suppl 1): 7–12. PMID 19209948. https://doi.org/10.2165/0128071-200910001-00002
  • Gudjonsson JE, Elder JT, Goldsmith LA, Katz SI, Gilchrest BA, Paller AS, Leffell DJ, Wolff K (2012). “18: Psoriasis”. Fitzpatrick’s Dermatology in General Medicine (8th ed.). McGraw-Hill. ISBN 0-07-166904-3.
  • Jain S (2012). Dermatology: Illustrated study guide and comprehensive board review. Springer. pp. 83–87. ISBN 978-1-4419-0524-6.
  • James W, Berger T, Elston D (2005). Andrews’ diseases of the skin: Clinical Dermatology (10th ed.). Saunders. pp. 191–7. ISBN 0-7216-2921-0.
  • Jones D, Roach P, Hartmann J, Setter J (2003). English pronouncing dictionary, Cambridge: Cambridge University Press, ISBN 3-12-539683-2.
  • Jump (2013). Questions and answers about psoriasis. Nat. Inst. Arthritis Musculoskeletal Skin Dis. Retrieved 1 July 2015.
  • Menter A, Gottlieb A, Feldman SR, Van Voorhees AS, Leonardi CL, Gordon KB, Lebwohl M, Koo JY, Elmets CA, Korman NJ, Beutner KR, Bhushan R (2008). Guidelines of care for the management of psoriasis and psoriatic arthritis: Section 1. Overview of psoriasis and guidelines of care for the treatment of psoriasis with biologics. J. Am. Acad. Dermatol. 58(5): 826–850. https://doi.org/10.1016/j.jaad.2008.02.039
  • Palfreeman AC, McNamee KE, McCann FE (2013). New developments in the management of psoriasis and psoriatic arthritis: a focus on apremilast. Drug. Des. Dev. Ther. 7: 201–210. PMC 3615921. PMID 23569359. https://doi.org/10.2147/DDDT.S32713
  • Parisi R, Symmons DP, Griffiths CE, Ashcroft DM (2013). Identification and management of psoriasis and associated comorbidity (IMPACT) project team. Global epidemiology of psoriasis: a systematic review of incidence and prevalence. J. Invest. Dermatol. 133(2): 377–85. PMID 23014338. https://doi.org/10.1038/jid.2012.339
  • Raychaudhuri SK, Maverakis E, Raychaudhuri SP (2014). Diagnosis and classification of psoriasis. Autoimmun. Rev. 13: 490–5. PMID 24434359. https://doi.org/10.1016/j.autrev.2014.01.008
  • Robinson A, Van Voorhees AS, Hsu S, Korman NJ, Lebwohl MG, Bebo BF, Kalb RE (2012). Treatment of pustular psoriasis: From the medical board of the national psoriasis foundation. J. Am. Acad. Dermatol. 67(2): 279–88. PMID 22609220. https://doi.org/10.1016/j.jaad.2011.01.032
  • Ship, Martin S, Greenberg, Michael G, Jonathan A (2008). Burket’s oral medicine (11th ed.). Hamilton, Ont.: BC Decker. pp. 103–104. ISBN 1-55009-345-2.
  • Stanway A (2014). Erythrodermic psoriasis. Derm. Net. NZ. Retrieved 16 March 2014.
  • Tamparo C (2011). Fifth edition: Diseases of the human body. Philadelphia, PA: F.A. Davis. pp. 180. ISBN 978-0-8036-2505-1.
  • Weigle N, McBane S (2013). Psoriasis. Am. Fam. Physician. 87(9): 626–633. PMID 23668525.
  • Yesudian PD, Chalmers RJ, Warren RB, Griffiths CE (2012). In search of oral psoriasis. Arch. Dermatol. Res. 304(1): 1–5. PMID 21927905. https://doi.org/10.1007/s00403-011-1175-3
  • Zattra E, Fortina BA, Peserico A, Alaibac M (2012). Erythroderma in the era of biological therapies. Eur. J. Dermatol. 22(2): 167–71. PMID 22321651. https://doi.org/10.1684/ejd.2011.1569
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