• DocumentCode
    3161568
  • Title

    In-vitro screening and docking study of fosinopril and its analogs

  • Author

    Kini, Suvarna ; Chaudhary, Jayant ; Arora, Sanjeev

  • Author_Institution
    Manipal Coll. of Pharm. Sci., Manipal, India
  • fYear
    2009
  • fDate
    2-4 Dec. 2009
  • Firstpage
    1
  • Lastpage
    4
  • Abstract
    Hypertension is the most common cardiovascular disease. The prevalence of hypertension increases with advancing age; for example, about 50% of people between the ages of 60 and 69 years old have hypertension, and the prevalence is further increased beyond age of 70. Many angiotensin converting enzyme (ACE) inhibitors are known to be useful in the treatment of hypertension. The search for ACE inhibitors that lacked the sulfhydryl group also leads to the investigation of phosphorus containing compounds. The phosphinic acid is capable of binding to ACE in a manner similar to enalapril. The interaction of the zinc atom with the phosphinic acid is similar that is seen with sulfhydryl groups The purpose of study is to design some derivatives of ACE Inhibitors like fosinopril, evaluate its invitro activity and carry out its docking studies to find the derivative with highest potency. Six analogs of fosinopril were given as gift samples by a pharmaceutical industry. The method of invitro study relies on spectrophotometric determination of hippuric acid, based on colorimetric reaction of hippuric acid with benzene sulfonyl chloride. Analog A2 was found to possess highest activity ( minimum IC50 value) followed by Fosinopril, Al, A4, A3, A5, and A6 respectively. GRIP batch docking study for all six compounds was carried out by using crystal structure of ACE as receptor, to screen them based on the dock score using the software vLife MDS 3.0. Analog A2 was found to have minimum dock score ( binding with the receptor by minimum energy) indicating highest activity.
  • Keywords
    biochemistry; crystal structure; drugs; enzymes; inhibitors; molecular biophysics; spectrochemical analysis; spectrophotometry; Fosinopril; GRIP batch docking study; angiotensin converting enzyme inhibitors; benzene sulfonyl chloride; cardiovascular disease; colorimetric reaction; crystal structure; hippuric acid; hypertension; in vitro screening; minimum dock score; pharmaceutical industry; phosphinic acid; spectrophotometry; sulfhydryl group; vLife MDS 3.0 software; Biochemistry; Cardiovascular diseases; Educational institutions; Hydrogen; Hypertension; In vitro; Inhibitors; Laboratories; Pharmaceuticals; Zinc;
  • fLanguage
    English
  • Publisher
    ieee
  • Conference_Titel
    Biomedical and Pharmaceutical Engineering, 2009. ICBPE '09. International Conference on
  • Conference_Location
    Singapore
  • Print_ISBN
    978-1-4244-4763-3
  • Electronic_ISBN
    978-1-4244-4764-0
  • Type

    conf

  • DOI
    10.1109/ICBPE.2009.5384099
  • Filename
    5384099