SlideShare a Scribd company logo

radiopaque agents.pptx

T
tujar kaso

it describes and states different radiopaque agent drugs

Education
1 of 21
Medicinal chemistry Presentation on Diagnostic agent: Radiopaque agents and classification [pharmacy department] By tujar kaso(b pharm)
Diagnostic agents  Diagnostic agents are the compounds used to detect impaired functions of the body organ or to detect abnormalities in tissue structure.  Usually they have no therapeutic value. so they do not used in the treatment of any disease.  Diagnostic agents are classified in to three heads: 1.radiopaques(x ray contrast media) e.g ioxaglate ,diatrizoate sodium 2. Cpds used to test functional capacity A. agents used to test kidney function e.g indigo carmine B. agents used to test liver function e.g rose Bengal
C. miscellaneous agents: e.g fluorescein sodium, 3. Cpds modifying physiological function: e.g alcohol Radiopaque(x ray contrast media):-  Radiopaque agents are drugs which have the ability to absorb x- rays. They are opaque to x-ray radiation so they produce lighter or whiter shadow on the x-ray film.  radiopaque agents include organic and inorganic compound which have the property of casting a shadow on x-ray film.
barium sulphate is the most inorganic compound that often used as suspension in examination of GIT.  the inorganic iodine compound which are ionized are generally toxic and they are not used clinically. But iodinated organic compounds which contain iodine bonded covalentely with carbon don’t release iodine ions readly and are less toxic. iodinated radiopaque agents They contain iodine, which blocks x-rays. Iodine is the only chemical element which combines three properties essential for the production of a successful CM:-  High contrast density  low toxicity  chemical behavior which allows firm binding to the highly variable benzene molecule
structure of iodinated radiopaque  most clinically used radiopaque contains iodine and all iodinated radiopaque contrast agents are derivative of benzoic acid. All the currently used iodinated contrast media are chemical modifications of a 2,4,6-triiodinated benzene ring.
The carbon atoms on a benzene ring are numbered clockwise from 1 to 6. Benzoic acid is produced by introducing an acid group at position 1 on the benzene ring.  This acid group permits the formation of salts or amides, which influence water solubility. 2,4,6-triiodobenzoic acid is obtained by introducing iodine atoms at positions 2, 4, and 6 on the ring.  Triiodo benzoic acid is made less toxic and less lipophilic (fat- soluble) by introducing side chains at positions 3 and 5.  The hydrogen atoms in the acid group can be replaced by a cation, such as sodium (Na) or meglumine, in which case the contrast agent is ionic.  If the hydrogen atom in the acid group is replaced instead by amine- carrying hydroxyl groups, then the compound is nonionic.
 When there is only one benzene ring in the compound, the contrast agent is a monomer; when there are two benzene rings in the compound, the contrast agent is a dimer.  The compound with 'two benzene rings contains twice the amount of iodine in the molecule compared to the monomer. Monomeric and dimeric contrast agents can be ionic or nonionic, depending on which substitutions are made at the acid group.
Structural activity relationship of iodinated radiopaque agents:  The basic structure of iodinated contrast agents is the benzene ring (Fig. 1), with its attached iodine atoms. The remaining components are the acid group and organic substitutes which influence excretion and toxicity.
All the currently used iodinated contrast media are chemical modifications of 3,5-diamino-2,4,6-triiodobenzoic acid.  all iodinated radiopaque agents contain organic amine salt group at position of R1 and R2 because amine groups are less toxic and more water soluble.
3,5-diamino-2,4,6-triiodobenzoic acid is, however, a rather unstable compound and has therefore proved unsuitable as X-ray contrast agent but acetylation of this compound yields 3,5- diacetamido-2,4,6-triiodobenzoic acid which is more stable.  The hydrogen atoms in the acid group can be replaced by a cation, such as sodium (Na) or meglumine, in which case the contrast agent is ionic.  If the hydrogen atom in the acid group is replaced instead by amine-carrying hydroxyl groups, then the compound is nonionic.  Elimination of contrast agents is dependent on organic substitutions of R1 and R2 position. If one of the organic substituents is a hydrogen atom, then the compound is excreted by the biliary system. If none of the organic substituents is a hydrogen atom on the benzene ring, then the contrast is excreted by the kidneys.
if there is an additional substitution of alkyl group on the amine group on one of R position, there is a difference in the solubility of the agents.  If there is di substitution of alkyl. There is a decrease in solubility of the agent. So N,N'-di-alkyl diacyl 3,5-diamino-2,4,6- triiodo-benzoic acid are useful as X-ray contrast agents in fields where insoluble compounds of high X-ray impermeability are required.  if there is mono substitution of alkyl in one of the amine group increases te solubility also it has less toxicity. So N-mono alkyl- 3,5-diacylamino-2,4,6-triiodobenzoic acids, in particular the N- methyl compound, are high water-solubility and, being of low toxicity, are especially suitable as vascular X-ray contrast agents.
classification of iodinated radiopaque agent  iodinated radiopaque agents are classified based on the:-  ionic composition Osmolar composition Water solubility viscosity  Ionicity is the characteristic of a molecule to break up into a positively charged cation and a negatively charged anion, resulting in more molecules per kilogram of water and thus increasing osmolality. Nonionic agents do not have this property and hence are less osmolar.  Ionic and nonionic contrast media may be monomeric or dimeric.
 In a solution, ionic monomers break up into their anion and cation components (increasing osmolality), delivering 3 iodine atoms (a 2:3 ratio of osmolar particles to iodine). ionic dimers would deliver 2 ionic components per 6 iodine atoms (ratio, 1:3).  Nonionic monomers do not break up in solution; a single molecule delivers 3 iodine atoms (ratio, 1:3).  a single nonionic dimer delivers 6 iodine atoms (ratio, 1:6). Thus, nonionic dimers are the most ideal contrast agents as they deliver the most iodine with the least effect on osmolality.
 based on the basis of osmolar composition iodinated radiopaque agents are classified in to:- High osmolar iodinated radiopaque agent Low osmolar iodinated radiopaque agent  iso-osmolar iodinated radiopaque agent  Osmolality indicates the concentration of all the particles dissolved in body fluid. Measures the number of molecules per kilogram of water dissolved in.  Osmolarity is a measure of the number of particles in a liter of the liquid they are dissolved in. high osmolar iodinated radiopaque agent  these agents are monomeric salt of triiodide benzoic acid. The iodine atom are attached at position 3,4,6 of the benzene ring and position 1 has a cation, either sodium or methylglucamine.
these agents contain three iodine atoms for every two osmotically active ions. These agents contain three iodine atoms for every two osmotically active ions. All ionize monomers have high osmolarity. E.g diatrizoate sodium  they are hypertonic with an osmolality(>1500mosm) which is six times higher than plasma(Normal values range from 275 to 295 mOsm/kg) , this in turn contribute to their side effect.
low osmolar iodinated radiopaque agent  these agents have three atoms of iodine for each ion. Have a ratio of 3:1,they are only two to three times of the osmolality of plasma.  these agents are either nonionic monomers or ionic dimers. And produce less allergic side effect and are less nephrotic. E.g ioxaglate, iopamidol, iohexol, ioversol.
iso-osmolar iodinated radiopaque agent  contains nonionic dimer. this class of contrast agents has osmolality similar to that of plasma. They are nonionic dimer and contains six atoms of iodine per dimer and has ratio of 6. iodixanol is the only agent in this class.
 In terms of viscosity, the larger the molecule, the more viscous is the contrast agent.  the most viscous contrast agents are the nonionic dimers, as opposed to the ionic dimers and the nonionic monomers. The least viscous are the ionic monomers.  The viscosity, however, changes with temperature. The higher the temperature, the less viscous the contrast becomes. For this reason, nonionic contrast agents are warmed to body temperature for intravenous or intraarterial injections, so as to make the injection easier and more rapid.
 based on water solubility iodinated radiopaque agents are classified in to two: 1.Water soluble iodinated radiopaque: contains agents like, diatrizoate sodium, metrizamide. Given orally or through injection.  they are mainly used for urography(examination of ureter, kidney) and angiography(examination of arterial system).  It is also used for visualizing of heart, lymph, and bile ducts. 2. water insoluble iodinated radiopaque agent: the agents are practically insoluble so there suspensions are prepared. they are mainly used for:  cholecystography(examination liver, gall bladder), bronchography(examination of bronchial tract).  contains agents like propyliodone, iopanoic acid.
techniques of administration of iodinated radiopaque agents:  the iodinated radiopaque agents are administered using two techniques: 1. In systemic procedure:- the agents are given orally or intravenously. They are used in:- A. in urography- to examine kidney B. in cholecystography- to examine gall bladder C. in roentgenography- to visualize parts the body like: urinary tract, billary tract, blood vessels, etc. 2. In retrograde procedure:- the agents are introduced by mechanical means. E.g introduced by catheter in to urinary tract through urethral orifice.

Recommended

Diagnostic agents
Diagnostic agentsDiagnostic agents
Diagnostic agents
Dr. Siddhartha Dutta
 
Potentiometry
PotentiometryPotentiometry
Potentiometry
Uday Deokate
 
Diagnostic agents(D. pharmacy)
Diagnostic agents(D. pharmacy)Diagnostic agents(D. pharmacy)
Diagnostic agents(D. pharmacy)
ShaikhSaniya2
 
Protectives & adsorbents
Protectives & adsorbents Protectives & adsorbents
Protectives & adsorbents
Revathi Gnanavelou
 
Non aqueous titration
Non aqueous titrationNon aqueous titration
Non aqueous titration
meraj khan
 
Diagnostic agents
Diagnostic agentsDiagnostic agents
Diagnostic agents
deepaksomavanshi
 
Radiopharmaceuticals
RadiopharmaceuticalsRadiopharmaceuticals
Radiopharmaceuticals
ESHA SHAH
 
IMIDAZOLE
IMIDAZOLE IMIDAZOLE
IMIDAZOLE
IjazHossain1
 

Recommended

Diagnostic agents
Diagnostic agentsDiagnostic agents
Diagnostic agents
Dr. Siddhartha Dutta
 
Potentiometry
PotentiometryPotentiometry
Potentiometry
Uday Deokate
 
Diagnostic agents(D. pharmacy)
Diagnostic agents(D. pharmacy)Diagnostic agents(D. pharmacy)
Diagnostic agents(D. pharmacy)
ShaikhSaniya2
 
Protectives & adsorbents
Protectives & adsorbents Protectives & adsorbents
Protectives & adsorbents
Revathi Gnanavelou
 
Non aqueous titration
Non aqueous titrationNon aqueous titration
Non aqueous titration
meraj khan
 
Diagnostic agents
Diagnostic agentsDiagnostic agents
Diagnostic agents
deepaksomavanshi
 
Radiopharmaceuticals
RadiopharmaceuticalsRadiopharmaceuticals
Radiopharmaceuticals
ESHA SHAH
 
IMIDAZOLE
IMIDAZOLE IMIDAZOLE
IMIDAZOLE
IjazHossain1
 
Complexometric titration
Complexometric titration Complexometric titration
Complexometric titration
Dr. HN Singh
 
Assay of calcium gluconate
Assay of calcium gluconateAssay of calcium gluconate
Assay of calcium gluconate
smita shelke
 
Errors
ErrorsErrors
Errors
saimuniswetha1
 
Radiopharmaceuticals
Radiopharmaceuticals Radiopharmaceuticals
Radiopharmaceuticals
Arshad Khan
 
Topical agents
Topical agentsTopical agents
Topical agents
Afroj Shaikh
 
STUDY OF FOLLOWING OFFICIAL COMPOUNDS
STUDY OF FOLLOWING OFFICIAL COMPOUNDSSTUDY OF FOLLOWING OFFICIAL COMPOUNDS
STUDY OF FOLLOWING OFFICIAL COMPOUNDS
Mr.S.SEETARAM SWAMY
 
Polarography- Pharmaceutical Analysis
Polarography- Pharmaceutical AnalysisPolarography- Pharmaceutical Analysis
Polarography- Pharmaceutical Analysis
Sanchit Dhankhar
 
Redox titration
Redox titrationRedox titration
Redox titration
Vinayaka Missions college of pharmacy
 
Adrenergic & cholinergic in Medicinal Chemistry
Adrenergic & cholinergic in Medicinal Chemistry Adrenergic & cholinergic in Medicinal Chemistry
Adrenergic & cholinergic in Medicinal Chemistry
Puja Ramu Basule
 
Radiopharmaceutical presentation
Radiopharmaceutical presentationRadiopharmaceutical presentation
Radiopharmaceutical presentation
laraib jameel
 
Radiopharmaceuticals....
Radiopharmaceuticals....Radiopharmaceuticals....
Radiopharmaceuticals....
Sandip Mavchi
 
Catheratics
CatheraticsCatheratics
Catheratics
Dipali Kulkarni
 
Cathartics
CatharticsCathartics
Cathartics
DR.Gopinathan Narasimhan
 
oxidation of drugs
oxidation of drugsoxidation of drugs
oxidation of drugs
SamawiaIqbal
 
Redox titration
Redox titration Redox titration
Redox titration
hemant Hemantch558
 
Diuretics by P.Ravisankar
Diuretics by P.RavisankarDiuretics by P.Ravisankar
Diuretics by P.Ravisankar
Dr. Ravi Sankar
 
Local antiinfective agents
Local antiinfective agentsLocal antiinfective agents
Local antiinfective agents
kencha swathi
 
TITLE -Radiopaque contrast media/PHARMACEUTICAL CHEMISTRY
TITLE -Radiopaque contrast media/PHARMACEUTICAL CHEMISTRYTITLE -Radiopaque contrast media/PHARMACEUTICAL CHEMISTRY
TITLE -Radiopaque contrast media/PHARMACEUTICAL CHEMISTRY
SUSHANT OJHA
 
Pharmaceutical impurities
Pharmaceutical impuritiesPharmaceutical impurities
Pharmaceutical impurities
Mahima Dubey
 
UNIT II: DRUGS ACTING ON AUTONOMIC NERVOUS SYSTEM
UNIT II: DRUGS ACTING ON AUTONOMIC NERVOUS SYSTEMUNIT II: DRUGS ACTING ON AUTONOMIC NERVOUS SYSTEM
UNIT II: DRUGS ACTING ON AUTONOMIC NERVOUS SYSTEM
SONALI PAWAR
 
Radiographic contrast media (urology)
Radiographic contrast media (urology)Radiographic contrast media (urology)
Radiographic contrast media (urology)
Deepesh Kalra
 
Contrast media 3
Contrast media 3 Contrast media 3
Contrast media 3
Behzad Ommani
 

More Related Content

What's hot

Polarography- Pharmaceutical Analysis
Polarography- Pharmaceutical AnalysisPolarography- Pharmaceutical Analysis
Polarography- Pharmaceutical Analysis
Sanchit Dhankhar
 

What's hot (20)

Complexometric titration
Complexometric titration Complexometric titration
Complexometric titration
 
Assay of calcium gluconate
Assay of calcium gluconateAssay of calcium gluconate
Assay of calcium gluconate
 
Errors
ErrorsErrors
Errors
 
Radiopharmaceuticals
Radiopharmaceuticals Radiopharmaceuticals
Radiopharmaceuticals
 
Topical agents
Topical agentsTopical agents
Topical agents
 
STUDY OF FOLLOWING OFFICIAL COMPOUNDS
STUDY OF FOLLOWING OFFICIAL COMPOUNDSSTUDY OF FOLLOWING OFFICIAL COMPOUNDS
STUDY OF FOLLOWING OFFICIAL COMPOUNDS
 
Polarography- Pharmaceutical Analysis
Polarography- Pharmaceutical AnalysisPolarography- Pharmaceutical Analysis
Polarography- Pharmaceutical Analysis
 
Redox titration
Redox titrationRedox titration
Redox titration
 
Adrenergic & cholinergic in Medicinal Chemistry
Adrenergic & cholinergic in Medicinal Chemistry Adrenergic & cholinergic in Medicinal Chemistry
Adrenergic & cholinergic in Medicinal Chemistry
 
Radiopharmaceutical presentation
Radiopharmaceutical presentationRadiopharmaceutical presentation
Radiopharmaceutical presentation
 
Radiopharmaceuticals....
Radiopharmaceuticals....Radiopharmaceuticals....
Radiopharmaceuticals....
 
Catheratics
CatheraticsCatheratics
Catheratics
 
Cathartics
CatharticsCathartics
Cathartics
 
oxidation of drugs
oxidation of drugsoxidation of drugs
oxidation of drugs
 
Redox titration
Redox titration Redox titration
Redox titration
 
Diuretics by P.Ravisankar
Diuretics by P.RavisankarDiuretics by P.Ravisankar
Diuretics by P.Ravisankar
 
Local antiinfective agents
Local antiinfective agentsLocal antiinfective agents
Local antiinfective agents
 
TITLE -Radiopaque contrast media/PHARMACEUTICAL CHEMISTRY
TITLE -Radiopaque contrast media/PHARMACEUTICAL CHEMISTRYTITLE -Radiopaque contrast media/PHARMACEUTICAL CHEMISTRY
TITLE -Radiopaque contrast media/PHARMACEUTICAL CHEMISTRY
 
Pharmaceutical impurities
Pharmaceutical impuritiesPharmaceutical impurities
Pharmaceutical impurities
 
UNIT II: DRUGS ACTING ON AUTONOMIC NERVOUS SYSTEM
UNIT II: DRUGS ACTING ON AUTONOMIC NERVOUS SYSTEMUNIT II: DRUGS ACTING ON AUTONOMIC NERVOUS SYSTEM
UNIT II: DRUGS ACTING ON AUTONOMIC NERVOUS SYSTEM
 

Similar to radiopaque agents.pptx

Testing the degradation of ascorbic acid by tlc
Testing the degradation of ascorbic acid by tlcTesting the degradation of ascorbic acid by tlc
Testing the degradation of ascorbic acid by tlc
ceutics1315
 

Similar to radiopaque agents.pptx (20)

Radiographic contrast media (urology)
Radiographic contrast media (urology)Radiographic contrast media (urology)
Radiographic contrast media (urology)
 
Contrast media 3
Contrast media 3 Contrast media 3
Contrast media 3
 
CONTRAST MEDIA in diagnostic radiography
CONTRAST MEDIA in diagnostic radiographyCONTRAST MEDIA in diagnostic radiography
CONTRAST MEDIA in diagnostic radiography
 
Contrast agents used in radiology
Contrast agents used in radiologyContrast agents used in radiology
Contrast agents used in radiology
 
Contrast media berry^Jrsna ^JAjr.pptx
Contrast media berry^Jrsna ^JAjr.pptxContrast media berry^Jrsna ^JAjr.pptx
Contrast media berry^Jrsna ^JAjr.pptx
 
Molecular spectroscopy notes
Molecular spectroscopy notesMolecular spectroscopy notes
Molecular spectroscopy notes
 
Basics of contrast media
Basics of contrast mediaBasics of contrast media
Basics of contrast media
 
basics of contrastmedia-171027192651.pdf
basics of contrastmedia-171027192651.pdfbasics of contrastmedia-171027192651.pdf
basics of contrastmedia-171027192651.pdf
 
diazotisation reaction and synthesis of azodyes
diazotisation reaction and synthesis of azodyes diazotisation reaction and synthesis of azodyes
diazotisation reaction and synthesis of azodyes
 
Susmita contrast media presentation
Susmita contrast media presentationSusmita contrast media presentation
Susmita contrast media presentation
 
Testing the degradation of ascorbic acid by tlc
Testing the degradation of ascorbic acid by tlcTesting the degradation of ascorbic acid by tlc
Testing the degradation of ascorbic acid by tlc
 
Radioisotopes -B for nuclear Engineering Course.pptx
Radioisotopes -B for nuclear Engineering Course.pptxRadioisotopes -B for nuclear Engineering Course.pptx
Radioisotopes -B for nuclear Engineering Course.pptx
 
Alkaloids
AlkaloidsAlkaloids
Alkaloids
 
Chemistry of natural products "alkaloids"
Chemistry of natural products "alkaloids"Chemistry of natural products "alkaloids"
Chemistry of natural products "alkaloids"
 
Detergents(1)
Detergents(1)Detergents(1)
Detergents(1)
 
Water Analysis through High Performance Liquid Chromotography, Ion Exchange R...
Water Analysis through High Performance Liquid Chromotography, Ion Exchange R...Water Analysis through High Performance Liquid Chromotography, Ion Exchange R...
Water Analysis through High Performance Liquid Chromotography, Ion Exchange R...
 
Gallery (2).pptx
Gallery (2).pptxGallery (2).pptx
Gallery (2).pptx
 
INTRAVASCULAR CONTRAST MEDIA [Autosaved].pptx
INTRAVASCULAR CONTRAST MEDIA [Autosaved].pptxINTRAVASCULAR CONTRAST MEDIA [Autosaved].pptx
INTRAVASCULAR CONTRAST MEDIA [Autosaved].pptx
 
Copy of CONTRAST MEDIA WEEK 1.pdf
Copy of CONTRAST MEDIA WEEK 1.pdfCopy of CONTRAST MEDIA WEEK 1.pdf
Copy of CONTRAST MEDIA WEEK 1.pdf
 
INTRAVASCULAR CONTRAST MEDIA.pptx
INTRAVASCULAR CONTRAST MEDIA.pptxINTRAVASCULAR CONTRAST MEDIA.pptx
INTRAVASCULAR CONTRAST MEDIA.pptx
 

Recently uploaded

Making communications land - Are they received and understood as intended? we...
Making communications land - Are they received and understood as intended? we...Making communications land - Are they received and understood as intended? we...
Making communications land - Are they received and understood as intended? we...
Association for Project Management
 

Recently uploaded (20)

Introduction to Nonprofit Accounting: The Basics
Introduction to Nonprofit Accounting: The BasicsIntroduction to Nonprofit Accounting: The Basics
Introduction to Nonprofit Accounting: The Basics
 
Unit-IV- Pharma. Marketing Channels.pptx
Unit-IV- Pharma. Marketing Channels.pptxUnit-IV- Pharma. Marketing Channels.pptx
Unit-IV- Pharma. Marketing Channels.pptx
 
Towards a code of practice for AI in AT.pptx
Towards a code of practice for AI in AT.pptxTowards a code of practice for AI in AT.pptx
Towards a code of practice for AI in AT.pptx
 
Single or Multiple melodic lines structure
Single or Multiple melodic lines structureSingle or Multiple melodic lines structure
Single or Multiple melodic lines structure
 
Making communications land - Are they received and understood as intended? we...
Making communications land - Are they received and understood as intended? we...Making communications land - Are they received and understood as intended? we...
Making communications land - Are they received and understood as intended? we...
 
How to Create and Manage Wizard in Odoo 17
How to Create and Manage Wizard in Odoo 17How to Create and Manage Wizard in Odoo 17
How to Create and Manage Wizard in Odoo 17
 
Sociology 101 Demonstration of Learning Exhibit
Sociology 101 Demonstration of Learning ExhibitSociology 101 Demonstration of Learning Exhibit
Sociology 101 Demonstration of Learning Exhibit
 
HMCS Max Bernays Pre-Deployment Brief (May 2024).pptx
HMCS Max Bernays Pre-Deployment Brief (May 2024).pptxHMCS Max Bernays Pre-Deployment Brief (May 2024).pptx
HMCS Max Bernays Pre-Deployment Brief (May 2024).pptx
 
SOC 101 Demonstration of Learning Presentation
SOC 101 Demonstration of Learning PresentationSOC 101 Demonstration of Learning Presentation
SOC 101 Demonstration of Learning Presentation
 
TỔNG ÔN TẬP THI VÀO LỚP 10 MÔN TIẾNG ANH NĂM HỌC 2023 - 2024 CÓ ĐÁP ÁN (NGỮ Â...
TỔNG ÔN TẬP THI VÀO LỚP 10 MÔN TIẾNG ANH NĂM HỌC 2023 - 2024 CÓ ĐÁP ÁN (NGỮ Â...TỔNG ÔN TẬP THI VÀO LỚP 10 MÔN TIẾNG ANH NĂM HỌC 2023 - 2024 CÓ ĐÁP ÁN (NGỮ Â...
TỔNG ÔN TẬP THI VÀO LỚP 10 MÔN TIẾNG ANH NĂM HỌC 2023 - 2024 CÓ ĐÁP ÁN (NGỮ Â...
 
On National Teacher Day, meet the 2024-25 Kenan Fellows
On National Teacher Day, meet the 2024-25 Kenan FellowsOn National Teacher Day, meet the 2024-25 Kenan Fellows
On National Teacher Day, meet the 2024-25 Kenan Fellows
 
ComPTIA Overview | Comptia Security+ Book SY0-701
ComPTIA Overview | Comptia Security+ Book SY0-701ComPTIA Overview | Comptia Security+ Book SY0-701
ComPTIA Overview | Comptia Security+ Book SY0-701
 
2024-NATIONAL-LEARNING-CAMP-AND-OTHER.pptx
2024-NATIONAL-LEARNING-CAMP-AND-OTHER.pptx2024-NATIONAL-LEARNING-CAMP-AND-OTHER.pptx
2024-NATIONAL-LEARNING-CAMP-AND-OTHER.pptx
 
How to Give a Domain for a Field in Odoo 17
How to Give a Domain for a Field in Odoo 17How to Give a Domain for a Field in Odoo 17
How to Give a Domain for a Field in Odoo 17
 
Application orientated numerical on hev.ppt
Application orientated numerical on hev.pptApplication orientated numerical on hev.ppt
Application orientated numerical on hev.ppt
 
Understanding Accommodations and Modifications
Understanding Accommodations and ModificationsUnderstanding Accommodations and Modifications
Understanding Accommodations and Modifications
 
Unit-IV; Professional Sales Representative (PSR).pptx
Unit-IV; Professional Sales Representative (PSR).pptxUnit-IV; Professional Sales Representative (PSR).pptx
Unit-IV; Professional Sales Representative (PSR).pptx
 
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
 
Food safety_Challenges food safety laboratories_.pdf
Food safety_Challenges food safety laboratories_.pdfFood safety_Challenges food safety laboratories_.pdf
Food safety_Challenges food safety laboratories_.pdf
 
Accessible Digital Futures project (20/03/2024)
Accessible Digital Futures project (20/03/2024)Accessible Digital Futures project (20/03/2024)
Accessible Digital Futures project (20/03/2024)
 

radiopaque agents.pptx

  • 1. Medicinal chemistry Presentation on Diagnostic agent: Radiopaque agents and classification [pharmacy department] By tujar kaso(b pharm)
  • 2. Diagnostic agents  Diagnostic agents are the compounds used to detect impaired functions of the body organ or to detect abnormalities in tissue structure.  Usually they have no therapeutic value. so they do not used in the treatment of any disease.  Diagnostic agents are classified in to three heads: 1.radiopaques(x ray contrast media) e.g ioxaglate ,diatrizoate sodium 2. Cpds used to test functional capacity A. agents used to test kidney function e.g indigo carmine B. agents used to test liver function e.g rose Bengal
  • 3. C. miscellaneous agents: e.g fluorescein sodium, 3. Cpds modifying physiological function: e.g alcohol Radiopaque(x ray contrast media):-  Radiopaque agents are drugs which have the ability to absorb x- rays. They are opaque to x-ray radiation so they produce lighter or whiter shadow on the x-ray film.  radiopaque agents include organic and inorganic compound which have the property of casting a shadow on x-ray film.
  • 4. barium sulphate is the most inorganic compound that often used as suspension in examination of GIT.  the inorganic iodine compound which are ionized are generally toxic and they are not used clinically. But iodinated organic compounds which contain iodine bonded covalentely with carbon don’t release iodine ions readly and are less toxic. iodinated radiopaque agents They contain iodine, which blocks x-rays. Iodine is the only chemical element which combines three properties essential for the production of a successful CM:-  High contrast density  low toxicity  chemical behavior which allows firm binding to the highly variable benzene molecule
  • 5. structure of iodinated radiopaque  most clinically used radiopaque contains iodine and all iodinated radiopaque contrast agents are derivative of benzoic acid. All the currently used iodinated contrast media are chemical modifications of a 2,4,6-triiodinated benzene ring.
  • 6. The carbon atoms on a benzene ring are numbered clockwise from 1 to 6. Benzoic acid is produced by introducing an acid group at position 1 on the benzene ring.  This acid group permits the formation of salts or amides, which influence water solubility. 2,4,6-triiodobenzoic acid is obtained by introducing iodine atoms at positions 2, 4, and 6 on the ring.  Triiodo benzoic acid is made less toxic and less lipophilic (fat- soluble) by introducing side chains at positions 3 and 5.  The hydrogen atoms in the acid group can be replaced by a cation, such as sodium (Na) or meglumine, in which case the contrast agent is ionic.  If the hydrogen atom in the acid group is replaced instead by amine- carrying hydroxyl groups, then the compound is nonionic.
  • 7.  When there is only one benzene ring in the compound, the contrast agent is a monomer; when there are two benzene rings in the compound, the contrast agent is a dimer.  The compound with 'two benzene rings contains twice the amount of iodine in the molecule compared to the monomer. Monomeric and dimeric contrast agents can be ionic or nonionic, depending on which substitutions are made at the acid group.
  • 8. Structural activity relationship of iodinated radiopaque agents:  The basic structure of iodinated contrast agents is the benzene ring (Fig. 1), with its attached iodine atoms. The remaining components are the acid group and organic substitutes which influence excretion and toxicity.
  • 9. All the currently used iodinated contrast media are chemical modifications of 3,5-diamino-2,4,6-triiodobenzoic acid.  all iodinated radiopaque agents contain organic amine salt group at position of R1 and R2 because amine groups are less toxic and more water soluble.
  • 10. 3,5-diamino-2,4,6-triiodobenzoic acid is, however, a rather unstable compound and has therefore proved unsuitable as X-ray contrast agent but acetylation of this compound yields 3,5- diacetamido-2,4,6-triiodobenzoic acid which is more stable.  The hydrogen atoms in the acid group can be replaced by a cation, such as sodium (Na) or meglumine, in which case the contrast agent is ionic.  If the hydrogen atom in the acid group is replaced instead by amine-carrying hydroxyl groups, then the compound is nonionic.  Elimination of contrast agents is dependent on organic substitutions of R1 and R2 position. If one of the organic substituents is a hydrogen atom, then the compound is excreted by the biliary system. If none of the organic substituents is a hydrogen atom on the benzene ring, then the contrast is excreted by the kidneys.
  • 11. if there is an additional substitution of alkyl group on the amine group on one of R position, there is a difference in the solubility of the agents.  If there is di substitution of alkyl. There is a decrease in solubility of the agent. So N,N'-di-alkyl diacyl 3,5-diamino-2,4,6- triiodo-benzoic acid are useful as X-ray contrast agents in fields where insoluble compounds of high X-ray impermeability are required.  if there is mono substitution of alkyl in one of the amine group increases te solubility also it has less toxicity. So N-mono alkyl- 3,5-diacylamino-2,4,6-triiodobenzoic acids, in particular the N- methyl compound, are high water-solubility and, being of low toxicity, are especially suitable as vascular X-ray contrast agents.
  • 12. classification of iodinated radiopaque agent  iodinated radiopaque agents are classified based on the:-  ionic composition Osmolar composition Water solubility viscosity  Ionicity is the characteristic of a molecule to break up into a positively charged cation and a negatively charged anion, resulting in more molecules per kilogram of water and thus increasing osmolality. Nonionic agents do not have this property and hence are less osmolar.  Ionic and nonionic contrast media may be monomeric or dimeric.
  • 13.  In a solution, ionic monomers break up into their anion and cation components (increasing osmolality), delivering 3 iodine atoms (a 2:3 ratio of osmolar particles to iodine). ionic dimers would deliver 2 ionic components per 6 iodine atoms (ratio, 1:3).  Nonionic monomers do not break up in solution; a single molecule delivers 3 iodine atoms (ratio, 1:3).  a single nonionic dimer delivers 6 iodine atoms (ratio, 1:6). Thus, nonionic dimers are the most ideal contrast agents as they deliver the most iodine with the least effect on osmolality.
  • 14.
  • 15.  based on the basis of osmolar composition iodinated radiopaque agents are classified in to:- High osmolar iodinated radiopaque agent Low osmolar iodinated radiopaque agent  iso-osmolar iodinated radiopaque agent  Osmolality indicates the concentration of all the particles dissolved in body fluid. Measures the number of molecules per kilogram of water dissolved in.  Osmolarity is a measure of the number of particles in a liter of the liquid they are dissolved in. high osmolar iodinated radiopaque agent  these agents are monomeric salt of triiodide benzoic acid. The iodine atom are attached at position 3,4,6 of the benzene ring and position 1 has a cation, either sodium or methylglucamine.
  • 16. these agents contain three iodine atoms for every two osmotically active ions. These agents contain three iodine atoms for every two osmotically active ions. All ionize monomers have high osmolarity. E.g diatrizoate sodium  they are hypertonic with an osmolality(>1500mosm) which is six times higher than plasma(Normal values range from 275 to 295 mOsm/kg) , this in turn contribute to their side effect.
  • 17. low osmolar iodinated radiopaque agent  these agents have three atoms of iodine for each ion. Have a ratio of 3:1,they are only two to three times of the osmolality of plasma.  these agents are either nonionic monomers or ionic dimers. And produce less allergic side effect and are less nephrotic. E.g ioxaglate, iopamidol, iohexol, ioversol.
  • 18. iso-osmolar iodinated radiopaque agent  contains nonionic dimer. this class of contrast agents has osmolality similar to that of plasma. They are nonionic dimer and contains six atoms of iodine per dimer and has ratio of 6. iodixanol is the only agent in this class.
  • 19.  In terms of viscosity, the larger the molecule, the more viscous is the contrast agent.  the most viscous contrast agents are the nonionic dimers, as opposed to the ionic dimers and the nonionic monomers. The least viscous are the ionic monomers.  The viscosity, however, changes with temperature. The higher the temperature, the less viscous the contrast becomes. For this reason, nonionic contrast agents are warmed to body temperature for intravenous or intraarterial injections, so as to make the injection easier and more rapid.
  • 20.  based on water solubility iodinated radiopaque agents are classified in to two: 1.Water soluble iodinated radiopaque: contains agents like, diatrizoate sodium, metrizamide. Given orally or through injection.  they are mainly used for urography(examination of ureter, kidney) and angiography(examination of arterial system).  It is also used for visualizing of heart, lymph, and bile ducts. 2. water insoluble iodinated radiopaque agent: the agents are practically insoluble so there suspensions are prepared. they are mainly used for:  cholecystography(examination liver, gall bladder), bronchography(examination of bronchial tract).  contains agents like propyliodone, iopanoic acid.
  • 21. techniques of administration of iodinated radiopaque agents:  the iodinated radiopaque agents are administered using two techniques: 1. In systemic procedure:- the agents are given orally or intravenously. They are used in:- A. in urography- to examine kidney B. in cholecystography- to examine gall bladder C. in roentgenography- to visualize parts the body like: urinary tract, billary tract, blood vessels, etc. 2. In retrograde procedure:- the agents are introduced by mechanical means. E.g introduced by catheter in to urinary tract through urethral orifice.