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International journal of clinical and experimental pathology
2024;17 (10): 317-328.

Therapeutic and toxicological assessment of hydroethanolic leaf extracts of in apparently healthy rats.

Yibala Ibor Oboma, Sylvanus Beredugo, Clement Nyenke, Yakubu Sunday Bot, Charles Iyore Idehen, Letticia Ikiomoye Beredugo
Author Information
  1. Yibala Ibor Oboma: Department of Medical Laboratory Science, School of Allied Health Sciences, Kampala International University, Western Campus P.O. Box 20000, Bushenyi, Uganda.
  2. Sylvanus Beredugo: Department of Medical Laboratory Science, Faculty of Basic Medical Sciences, Niger Delta University Wilberforce Island, P.O. Box 076, Bayelsa State, Nigeria.
  3. Clement Nyenke: Department of Medical Laboratory Sciences, Faculty of Allied Health Sciences, PAMO University of Medical Sciences (PUMS) Port-Harcourt, Rivers State, Nigeria.
  4. Yakubu Sunday Bot: Department of Medical Laboratory Science, School of Allied Health Sciences, Kampala International University, Western Campus P.O. Box 20000, Bushenyi, Uganda.
  5. Charles Iyore Idehen: Department of Medical Laboratory Science, School of Allied Health Sciences, Kampala International University, Western Campus P.O. Box 20000, Bushenyi, Uganda.
  6. Letticia Ikiomoye Beredugo: Department of Community Health Nursing, Faculty of Nursing Sciences, Niger Delta University Wilberforce Island, P.O. Box 076, Bayelsa State, Nigeria.
PMID: 39544712 DOI: 10.62347/SYZP2468

Abstract

The use of medicinal plants in the management or prevention of diseases is one of the oldest human medicinal practices worldwide. and are widely reported for their use in the management of blood disorders, hypertension, and diabetes.
OBJECTIVE: The study aimed at evaluating the effects of hydroethanolic leaf extracts of and on the biochemical, hematological, and histological parameters of apparently healthy rats.
METHODOLOGY: Thirty adult rats (n = 30) with an average weight of 153 g were randomly divided into six groups (A-F). Group A: negative control; Group B: positive control; Group C: (low dose); Group D: (high dose); Group E: (low dose); and Group F: (high dose). Standard and scientifically approved methods were used for sacrifice and laboratory diagnosis.
RESULTS: The study shows a significant increase in body weight across groups administered with the leaf extracts. Elevated levels of serum creatinine were recorded in rats administered with both extracts, indicating nephrotoxicity. The study also observed an increase in alanine aminotransferase, aspartate aminotransferase, and alkaline phosphatase across groups, indicating hepatotoxicity. Both extracts caused an increase in white blood cell count and hemoglobin concentration, a significant reduction in bleeding time, increased prothrombin time, and partial thromboplastin time at high dosages. Total iron binding capacity and serum ferritin values were increased in high doses and were statistically significant at P<0.05. Histomorphology of both extracts shows hepatorenal toxicity at high concentrations and none in the lungs or heart. Oral administration of and extracts at high concentrations is not safe for the liver and kidneys.
CONCLUSION: Biochemical parameters should be monitored regularly in humans exposed to both plants. Therefore, this study scientifically confirms and supports the traditional use of the leaves of and to enhance hematological parameters.

Keywords

Jatropha Justicia Kampala therapeutic toxicology

References

  1. J Dent Hyg. 2003 Winter;77(1):37-46 [PMID: 12704968]
  2. Helicobacter. 2017 Feb;22(1): [PMID: 27411077]
  3. J Thromb Haemost. 2005 Aug;3(8):1773-82 [PMID: 16102044]
  4. Vitam Horm. 2005;72:505-35 [PMID: 16492481]
  5. Nutrients. 2014 Mar 13;6(3):1080-102 [PMID: 24633395]
  6. Afr J Tradit Complement Altern Med. 2011 Oct 02;9(1):81-7 [PMID: 23983324]
  7. J Ethnopharmacol. 2013 Mar 7;146(1):40-61 [PMID: 23286904]
  8. Malays J Nutr. 2002 Sep;8(2):179-89 [PMID: 22692476]
  9. Radiat Res. 2008 Apr;169(4):384-96 [PMID: 18363433]
  10. J Med Food. 2005 Winter;8(4):539-44 [PMID: 16379569]
  11. J Dent Hyg. 2007 Summer;81(3):67 [PMID: 17908423]
  12. Pak J Biol Sci. 2009 Aug 1;12(15):1063-8 [PMID: 19943462]
  13. J Ethnopharmacol. 2003 Nov;89(1):101-5 [PMID: 14522439]
  14. J Indian Soc Periodontol. 2013 Jul;17(4):411-6 [PMID: 24174716]
  15. Transfus Apher Sci. 2009 Oct;41(2):121-5 [PMID: 19699685]
  16. Best Pract Res Clin Obstet Gynaecol. 2014 Jan;28(1):3-12 [PMID: 24140480]
  17. J Ethnopharmacol. 2004 Jan;90(1):11-5 [PMID: 14698501]
  18. Acta Sci Pol Technol Aliment. 2017 Apr-Jun;16(2):217-230 [PMID: 28703962]
  19. Int J Mol Sci. 2011;12(5):2958-71 [PMID: 21686161]
Journal Article

Word Cloud

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