SlideShare uma empresa Scribd logo

Screening of antimalarial drugs

Transferir como PPTX, PDF
A
Anupam Prahlad

antimalarial drugs

Educação
1 de 37
SCREENING METHODS OF ANTIMALARIAL DRUGS SUBMITTED BY ANUPAM PRAHLAD DEPT.OF PHARMACOLOGY
MALARIA • Protozoal disease caused by parasites of the genus Plasmodium and transmitted to man by certain species of infected female anopheles mosquito.
• Five species of the genus Plasmodium cause nearly all malarial infections in humans. ‐ Falciparum – life threatening ‐ Vivax ‐ Ovale ‐ Malariae ‐ Knowlesi (in Southeast Asia- the monkey malaria parasite )
TREATMENT Quinolones Cinchona Biguanides Diaminopyrimidines Sulfonamides and sulfone Tetracyclines Sesquiterpine Amino alcohols Mannich base naphthoquinone
SCREENING METHODS IN VITRO METHODS 1. 3H hypoxanthine uptake 2. Giemsa stained slide method 3. Micro test 4. Flow cytometry 5. Measurement of ldh activity of p. Falciparum 6. Isobologram analysis IN VIVO METHODS 1. Plasmodium berghei 4 day suppression test 2. Hill’s test for causal prophylaxix and residual activity 3. Sporonoicidal activity testing 4. Plasmodium cynomolgi rhesus model
3H HYPOXANTHINE UPTAKE TEST • Most commonly used method for assessing antimalarial efficacy of a compound in vitro . • Hypoxanthine used by parasite for purine salvage and DNA synthesis. • Radiolabelled hypoxanthine uptake by parasite is an indicator of its growth and multiplication. • Parasites are cultured in different concentration of test compounds in media containing reduced concentration of hypoxanthine. • After which 3H Hypoxanthine is added.
• Measurement of radioactivity by a 1205 betaplate reader. • Percent reductions are measured. Evalution % reduction = (mean cpm of test samples) 3H Hypoxanthine X 100 • Percent reductions are used to plot percentage inhibition of growth as a function of drug concentration. • IC 50 are determined by linear regression analyses
GIEMSA STAINED SLIDE METHOD (MIC METHOD) • Low cost alternative for testing small number of compounds. • Parasites are incubated with test compound. • Parasitemia of control and treated groups are compared by counting Giemsa stained parasites by light microscopy. • Parasites incubated in 5% suspension of erythrocytes at 370C. • Change in the proportion of infected RBCs is assessed at end of 72 hr. at various concentrations of each drug
• Drug is dissolved in 4% sucrose and fed ad libitum to the insects following the blood meal. • The level of drug activity can be calculated from a comparison of mean oocyst counts in treated and control batches.
FLOW CYTOMETRY • Parasites are fixed after appropriate period of incubation with test compounds. • The parasite nuclei are stained with DAPI (42, 6- diamidino-2- phenylindole). • Counts of treated and control cultures are then obtained by flow cytometry.
MICRO-TEST (MARK III) • Most commonly used method for the antimalarial testing for resistance • Provides information on the quantitative drug response of P. Falciparum . • test can be carried out with several drugs, in a micro test kit with 12 X 8 wells, predosed with chloroquine , mefloquine , quinine , amodiaquine , artemisinin , sulfadoxine (SDX)/ pyrimethamine (PYR) , pyrimethamine (PYR) • Patient’s blood sample is inoculated in the wells and incubated with suitable medium. • The number of schizonts is counted and compared with control well.
• For monitoring the level and spread of resistance, molecular diagnostic methods for detecting resistant parasite have been proposed. • These molecular tools are based on the detection by PCR of point mutation in the parasite genome responsible for in vitro resistance
ADVANTAGES OF IN VITRO METHODS • Precise and efficient • Rapid • Large number of compounds can be evaluated at the same time • Synergism or antagonism with drug combinations can be studied • Better assessment of intrinsic activity of a drug.
LIMITATIONS OF IN VITRO METHODS • Drugs acting through active metabolite cannot be studied. • Non reproducibility of pharmacokinetic effects. • Toxic compounds also get selected. • Expertise and infrastructure needed • Lack of clinical correlation.
IN VIVO METHODS • Compounds effective in in-vitro screening tests are taken up for in vivo evaluation. • Plasmodium species that cause human disease are unable to infect non primate animal models, • Rodent malaria parasite. P. berghei, P. yoelii, P. chabaudi, P. vinckei have been used extensively in drug discovery and early development.
PLASMODIUM BERGHEI 4 DAY SUPPRESSION METHOD • Most widely used preliminary test. • Efficacy assessed by comparison of blood parasitemia and mouse survival time • Mice maintained at 220C at 50-70% humidity • Diet containing p-aminobenzoic acid 45 mg/kg and water ad libitum.
• On day 0, mice are injected with 0.2 ml of aliquot (2X107 parasitized erythrocytes by Plasmodium berghei) • Experimental groups are (five each) : Vehicle treated (control group) Test drug treated group. Positive control group (chloroquine,reference drug) is administered.
• On day 1 to 3, the experimental groups are treated. • On day 4, blood smears from all animals are prepared with Giemsa stain. • Parasitemia is determined microscopically by counting 4 fields of approximately 100 erythrocytes per field. • The difference between the mean value of the control group and those of the experimental groups is calculated. • Untreated control mice typically die approximately one week after infection
• For treated mice mean survival time is calculated in comparison with the untreated and standard drug treated group • Mice without parasitemia on day 30 of post-infection are considered cured. • Compounds identified as active in this test are progressed through several of the following secondary tests. • In the ‘Dose ranging full four day test’, compounds are tested at four doses, by different routes of administration, to determine ED50 value. • This test also leads to information about relative potency and bioavailability
Recrudescence test • Mice are administered with single dose of the test compound on day 3 of postinfection.  Control mice receive the suspension vehicle alone.  Blood smears are prepared at intervals of 12 h, 24h and then daily till day 33  and assessed for parasitemia • Results are expressed in terms of rapidity of onset of activity, time to onset of recrudescence, increase of parasitemia and duration of survival (in days). • Compounds are also tested for prophylactic activity by administrating them prior to infection, followed by daily examination of smears.
HILL’S TEST FOR CAUSAL PROPHYLAXIS AND RESIDUAL ACTIVITY • In this model, mice (Charles River strain) are inoculated with P. yoelii (N67 strain) sporozoites. • Each mouse receives approximately 104-105 sporozoites intravenously in a total volume of 0.2ml. • For a compound to be considered truly causal prophylactic it must pass through four different phases
PHASE 1 • Involves detection of causal prophylactic activity of the test compound in mice. • Test compound is administered 3hr after a sporozoite inoculation. • During 14 day period, blood films are taken • If parasitemia is not detected for 14 days the compound is considered to be fully protective.
PHASE 2 • Compound is then tested for residual activity directed against blood stage parasites by administrating a single dose of the test compound . • After 48hr trophozoites are injected intravenously. • If the time interval to reach 2% parasitemia is similar to that of the control group, then it is considered that no residual activity has occurred
PHASE 3 • Compounds suspected of prolonged residual activity are tested by administering sporozoites followed by the drug 3 h later. • After an additional 48h , 0.2 ml blood is and injected intraperitoneally into a clean mouse. • Blood films are examined for a 14 day . • Residual activity is noted if less than 50% of the recipients develop parasitemia . • A compound has no residual activity if 75% or more recipient mice develop patent infection.
PHASE 4 • An additional procedure to clarify whether a compound has residual effect on erythrocytic stages. • Mice are injected intravenously with trophozoites 48 h after the compound administration.
• After an additional 3-4 h, 0.2ml of blood is removed and injected to clean recipient mice. • Blood films are taken and a comparison of the time interval to reach 2% parasitemia is made with control mice • If the time interval is similar no residual activity is present
SPORONOICIDAL ACTIVITY TESTING • Albino mice are administered with Plasmodium yoelii nigeriensis N 67 parasite on day 0. • Female A. stephensi mosquitoes are placed in containers. • On third day following infection , mosquitoes were starved for 24 h are allowed to feed on mice. • Presence of mature gamets is confirmed on blood film of mice. • The mice are then anaesthetized with a single dose of 60 mg/kg of sodium pentobarbitone i.p..
• Mice laid on top of mosquito containers • Mosquitoes feed on them. • On the seventh day after the blood feed, a sample of each batch is removed and dissected. • Midguts are examined with the aid of semi-dark ground illumination and oocyst counts are made • The mean count for each batch is calculated • Drug is dissolved in 4% sucrose and fed ad libitum to the insects following the blood meal. • The level of drug activity can be calculated from a comparison of mean oocyst counts in treated and control batches
IMMUNOCOMPROMISED MICE • A new in vivo mice model for antimalarial efficacy is designed which comprises of use of immunocompromised mice. • It can support Plasmodium falciparum infection as it lacks T and Lymphokine activated killer cells. • P. falciparum parasitized human red blood cells are grafted into immunodeficient mice. • For immunomodulation dichloromethylene diphosphate (Cl2MDP) is administered for tissue macrophages.
• This is the first rodent model in which Plasmodium falciparum infection can be maintained. • Test drugs are administered when parasitemia becomes stable and smears show predominance of ring forms.
PLASMODIUM CYNOMOLGI RHESUS MODEL • This model runs a close parallel to P. vivax infection in man. • It can be used to evaluate causal prophylactic, blood schizonticidal and hypnozoitocidal activity of a test compound in one model. • Young, tuberculin negative rhesus monkeys weighing 3.5 to 6 kg are used. • Each animal receives i.v. inoculum of approximately 500,000 sporozoites in 2 ml of fluid.
• Drugs administered through a stomach tube once daily, commencing the day before infection and continuing up to day 8. • Blood films are made daily till 6 weeks • At the end of 6 weeks if the animals are still negetive, they are rechallenged with a similar inoculum to prove their susceptibility to infection. • All animals becoming infected during 4-6 weeks observation period and also infected animals from rechallenged group are further treated as soon as the parasitemia level reaches 0.1 to 0.5%. • The animals receive 7 daily oral doses of the drug and blood films are examined daily during and after therapy up to a total of 30 days.
• If still negative, the animals are then examined twice weekly until they relapse. • If the parasites are not cleared by the drug during the primary attack, the animals are given 7 daily doses of 5mg/kg of chloroquine. • If no relapse follows chloroquine administration, it indicates that the test drug has destroyed the hypnozoites. • When no relapse occurs within 8-12 weeks, the animals are splenectomized. • Failure to develop further parasitemia within 4 weeks indicates that the animals are radically cured
AVIAN MODELS • At least 447 species of birds have been found infected with malarial parasite. • The avian parasite infects nucleated erythrocytes. • The vectors of avian species are mosquitoes of the genera Aedes or Culex • Method: When only one or two birds need to be infected, parasitized blood can be obtained from the leg vein or wing vein of an infected bird.
• When large number of chicks is to be infected from a single donor, blood is aspirated directly from the neck vein or from the heart. • Drugs may be administered to chicks orally, intravenously or intramuscularly the oral route is the method used more frequently. • Experimental birds are infected intravenously and receive the first dose of drug on day 1 followed by twice daily for the next 3 days. • Blood films are made on day 4. • Parasitemia achieved on day 4 in treated and untreated control group is then compared.
THANK YOU

Recomendados

Pharmacological screening of Anti-psychotic agents
Pharmacological screening of Anti-psychotic agentsPharmacological screening of Anti-psychotic agents
Pharmacological screening of Anti-psychotic agentsAbin Joy
 
Screening of antimalarial drugs
Screening of antimalarial drugsScreening of antimalarial drugs
Screening of antimalarial drugsHarsh Yadav
 
Screening of antiparkinsonian agents
Screening of antiparkinsonian agentsScreening of antiparkinsonian agents
Screening of antiparkinsonian agentsDr. Mallappa Shalavadi
 
Preclinical screening methods of Sedative and hypnotics by syed
Preclinical screening methods of Sedative and hypnotics by syedPreclinical screening methods of Sedative and hypnotics by syed
Preclinical screening methods of Sedative and hypnotics by syedMubasheer syed
 
Screening Models of Anti-Inflammatory Drugs
Screening Models of Anti-Inflammatory DrugsScreening Models of Anti-Inflammatory Drugs
Screening Models of Anti-Inflammatory DrugsAnupam dubey
 
Screening of antipyretic drugs
Screening of antipyretic drugsScreening of antipyretic drugs
Screening of antipyretic drugsSindhoora Shetty
 
SCREENING OF ANTI CANCER DRUGS
SCREENING OF ANTI CANCER DRUGSSCREENING OF ANTI CANCER DRUGS
SCREENING OF ANTI CANCER DRUGSRafa Zubair
 
Assignment on Preclinical and clinical screening of anti cancer drugs
Assignment on Preclinical and clinical screening of anti cancer drugsAssignment on Preclinical and clinical screening of anti cancer drugs
Assignment on Preclinical and clinical screening of anti cancer drugsDeepak Kumar
 

Recomendados

Pharmacological screening of Anti-psychotic agents
Pharmacological screening of Anti-psychotic agentsPharmacological screening of Anti-psychotic agents
Pharmacological screening of Anti-psychotic agentsAbin Joy
 
Screening of antimalarial drugs
Screening of antimalarial drugsScreening of antimalarial drugs
Screening of antimalarial drugsHarsh Yadav
 
Screening of antiparkinsonian agents
Screening of antiparkinsonian agentsScreening of antiparkinsonian agents
Screening of antiparkinsonian agentsDr. Mallappa Shalavadi
 
Preclinical screening methods of Sedative and hypnotics by syed
Preclinical screening methods of Sedative and hypnotics by syedPreclinical screening methods of Sedative and hypnotics by syed
Preclinical screening methods of Sedative and hypnotics by syedMubasheer syed
 
Screening Models of Anti-Inflammatory Drugs
Screening Models of Anti-Inflammatory DrugsScreening Models of Anti-Inflammatory Drugs
Screening Models of Anti-Inflammatory DrugsAnupam dubey
 
Screening of antipyretic drugs
Screening of antipyretic drugsScreening of antipyretic drugs
Screening of antipyretic drugsSindhoora Shetty
 
SCREENING OF ANTI CANCER DRUGS
SCREENING OF ANTI CANCER DRUGSSCREENING OF ANTI CANCER DRUGS
SCREENING OF ANTI CANCER DRUGSRafa Zubair
 
Assignment on Preclinical and clinical screening of anti cancer drugs
Assignment on Preclinical and clinical screening of anti cancer drugsAssignment on Preclinical and clinical screening of anti cancer drugs
Assignment on Preclinical and clinical screening of anti cancer drugsDeepak Kumar
 
Screening antianginal (1)
Screening antianginal (1)Screening antianginal (1)
Screening antianginal (1)Dr Roohana Hasan
 
Screening models of antiepileptic and nootropic drugs
Screening models of antiepileptic and nootropic drugsScreening models of antiepileptic and nootropic drugs
Screening models of antiepileptic and nootropic drugsHimikaRathi
 
Screening of Local Anaesthestics
Screening of Local AnaesthesticsScreening of Local Anaesthestics
Screening of Local AnaesthesticsTulasi Raman
 
Acute dermal irritation/corrosion: OECD 404
Acute dermal irritation/corrosion: OECD 404Acute dermal irritation/corrosion: OECD 404
Acute dermal irritation/corrosion: OECD 404Dr Ajay Mandal
 
Screening method of nootropics vikas malik
Screening method of nootropics vikas malikScreening method of nootropics vikas malik
Screening method of nootropics vikas malikVikasMalik68
 
Assignment on Preclinical Screening of Immunomodulators
Assignment on Preclinical Screening of ImmunomodulatorsAssignment on Preclinical Screening of Immunomodulators
Assignment on Preclinical Screening of ImmunomodulatorsDeepak Kumar
 
Screening of antipyretic drugs
Screening of antipyretic drugsScreening of antipyretic drugs
Screening of antipyretic drugsdrarunsingh4
 
Screening models for immunomodulator
Screening models for immunomodulatorScreening models for immunomodulator
Screening models for immunomodulatorMr. MOHD FAHAD
 
Antipsychotic screening- Dr Divya Krishnan
Antipsychotic screening- Dr Divya Krishnan Antipsychotic screening- Dr Divya Krishnan
Antipsychotic screening- Dr Divya Krishnan Divya Krishnan
 
Preclinical Screening for Alzheimer's
Preclinical Screening for Alzheimer'sPreclinical Screening for Alzheimer's
Preclinical Screening for Alzheimer'sDrx Burade
 
Screening hypnotic activity
Screening hypnotic activityScreening hypnotic activity
Screening hypnotic activityDr. Pooja
 
screening of antiulcer agents
screening of antiulcer agentsscreening of antiulcer agents
screening of antiulcer agentsUttara Joshi
 
Screening of centrally acting muscle relaxant agents
Screening of centrally acting muscle relaxant agentsScreening of centrally acting muscle relaxant agents
Screening of centrally acting muscle relaxant agentsDeepmalya Ghosh
 
Screening models for inflammatory drugs
Screening models for inflammatory drugsScreening models for inflammatory drugs
Screening models for inflammatory drugsMy_VivJaan
 
Safety pharmacology
Safety pharmacologySafety pharmacology
Safety pharmacologyRamavath Aruna
 
Anti-diarrhoeal screening models and methods
Anti-diarrhoeal screening models and methodsAnti-diarrhoeal screening models and methods
Anti-diarrhoeal screening models and methodsPervej Alom
 
pre clinical Screening for anti asthmatic drugs
pre clinical Screening for anti asthmatic drugspre clinical Screening for anti asthmatic drugs
pre clinical Screening for anti asthmatic drugsDHINESHKUMAR V
 
Screening of anti-emetic drugs
Screening of anti-emetic drugsScreening of anti-emetic drugs
Screening of anti-emetic drugsDr. Prashant Shukla
 
Alternative methods to animal toxicity testing
Alternative methods to animal toxicity testingAlternative methods to animal toxicity testing
Alternative methods to animal toxicity testingSanchit Dhankhar
 
Screening of antihypertensive agents
Screening of antihypertensive agentsScreening of antihypertensive agents
Screening of antihypertensive agentsKanthlal SK
 
Anti- Tumor assay / Screening of Anticancer Drugs
Anti- Tumor assay / Screening of Anticancer DrugsAnti- Tumor assay / Screening of Anticancer Drugs
Anti- Tumor assay / Screening of Anticancer DrugsPratik Parikh
 
Recent advances in treatment of malaria
Recent advances in treatment of malaria Recent advances in treatment of malaria
Recent advances in treatment of malaria Naser Tadvi
 

Mais conteúdo relacionado

Mais procurados

Screening models of antiepileptic and nootropic drugs
Screening models of antiepileptic and nootropic drugsScreening models of antiepileptic and nootropic drugs
Screening models of antiepileptic and nootropic drugsHimikaRathi
 
Screening of Local Anaesthestics
Screening of Local AnaesthesticsScreening of Local Anaesthestics
Screening of Local AnaesthesticsTulasi Raman
 
Acute dermal irritation/corrosion: OECD 404
Acute dermal irritation/corrosion: OECD 404Acute dermal irritation/corrosion: OECD 404
Acute dermal irritation/corrosion: OECD 404Dr Ajay Mandal
 
Screening method of nootropics vikas malik
Screening method of nootropics vikas malikScreening method of nootropics vikas malik
Screening method of nootropics vikas malikVikasMalik68
 
Assignment on Preclinical Screening of Immunomodulators
Assignment on Preclinical Screening of ImmunomodulatorsAssignment on Preclinical Screening of Immunomodulators
Assignment on Preclinical Screening of ImmunomodulatorsDeepak Kumar
 
Screening of antipyretic drugs
Screening of antipyretic drugsScreening of antipyretic drugs
Screening of antipyretic drugsdrarunsingh4
 
Screening models for immunomodulator
Screening models for immunomodulatorScreening models for immunomodulator
Screening models for immunomodulatorMr. MOHD FAHAD
 
Antipsychotic screening- Dr Divya Krishnan
Antipsychotic screening- Dr Divya Krishnan Antipsychotic screening- Dr Divya Krishnan
Antipsychotic screening- Dr Divya Krishnan Divya Krishnan
 
Preclinical Screening for Alzheimer's
Preclinical Screening for Alzheimer'sPreclinical Screening for Alzheimer's
Preclinical Screening for Alzheimer'sDrx Burade
 
Screening hypnotic activity
Screening hypnotic activityScreening hypnotic activity
Screening hypnotic activityDr. Pooja
 
screening of antiulcer agents
screening of antiulcer agentsscreening of antiulcer agents
screening of antiulcer agentsUttara Joshi
 
Screening of centrally acting muscle relaxant agents
Screening of centrally acting muscle relaxant agentsScreening of centrally acting muscle relaxant agents
Screening of centrally acting muscle relaxant agentsDeepmalya Ghosh
 
Screening models for inflammatory drugs
Screening models for inflammatory drugsScreening models for inflammatory drugs
Screening models for inflammatory drugsMy_VivJaan
 
Anti-diarrhoeal screening models and methods
Anti-diarrhoeal screening models and methodsAnti-diarrhoeal screening models and methods
Anti-diarrhoeal screening models and methodsPervej Alom
 
pre clinical Screening for anti asthmatic drugs
pre clinical Screening for anti asthmatic drugspre clinical Screening for anti asthmatic drugs
pre clinical Screening for anti asthmatic drugsDHINESHKUMAR V
 
Alternative methods to animal toxicity testing
Alternative methods to animal toxicity testingAlternative methods to animal toxicity testing
Alternative methods to animal toxicity testingSanchit Dhankhar
 
Screening of antihypertensive agents
Screening of antihypertensive agentsScreening of antihypertensive agents
Screening of antihypertensive agentsKanthlal SK
 

Mais procurados (20)

Screening antianginal (1)
Screening antianginal (1)Screening antianginal (1)
Screening antianginal (1)
 
Screening models of antiepileptic and nootropic drugs
Screening models of antiepileptic and nootropic drugsScreening models of antiepileptic and nootropic drugs
Screening models of antiepileptic and nootropic drugs
 
Screening of Local Anaesthestics
Screening of Local AnaesthesticsScreening of Local Anaesthestics
Screening of Local Anaesthestics
 
Acute dermal irritation/corrosion: OECD 404
Acute dermal irritation/corrosion: OECD 404Acute dermal irritation/corrosion: OECD 404
Acute dermal irritation/corrosion: OECD 404
 
Screening method of nootropics vikas malik
Screening method of nootropics vikas malikScreening method of nootropics vikas malik
Screening method of nootropics vikas malik
 
Assignment on Preclinical Screening of Immunomodulators
Assignment on Preclinical Screening of ImmunomodulatorsAssignment on Preclinical Screening of Immunomodulators
Assignment on Preclinical Screening of Immunomodulators
 
Screening of antipyretic drugs
Screening of antipyretic drugsScreening of antipyretic drugs
Screening of antipyretic drugs
 
Screening models for immunomodulator
Screening models for immunomodulatorScreening models for immunomodulator
Screening models for immunomodulator
 
Antipsychotic screening- Dr Divya Krishnan
Antipsychotic screening- Dr Divya Krishnan Antipsychotic screening- Dr Divya Krishnan
Antipsychotic screening- Dr Divya Krishnan
 
Preclinical Screening for Alzheimer's
Preclinical Screening for Alzheimer'sPreclinical Screening for Alzheimer's
Preclinical Screening for Alzheimer's
 
Screening hypnotic activity
Screening hypnotic activityScreening hypnotic activity
Screening hypnotic activity
 
screening of antiulcer agents
screening of antiulcer agentsscreening of antiulcer agents
screening of antiulcer agents
 
Screening of centrally acting muscle relaxant agents
Screening of centrally acting muscle relaxant agentsScreening of centrally acting muscle relaxant agents
Screening of centrally acting muscle relaxant agents
 
Screening models for inflammatory drugs
Screening models for inflammatory drugsScreening models for inflammatory drugs
Screening models for inflammatory drugs
 
Safety pharmacology
Safety pharmacologySafety pharmacology
Safety pharmacology
 
Anti-diarrhoeal screening models and methods
Anti-diarrhoeal screening models and methodsAnti-diarrhoeal screening models and methods
Anti-diarrhoeal screening models and methods
 
pre clinical Screening for anti asthmatic drugs
pre clinical Screening for anti asthmatic drugspre clinical Screening for anti asthmatic drugs
pre clinical Screening for anti asthmatic drugs
 
Screening of anti-emetic drugs
Screening of anti-emetic drugsScreening of anti-emetic drugs
Screening of anti-emetic drugs
 
Alternative methods to animal toxicity testing
Alternative methods to animal toxicity testingAlternative methods to animal toxicity testing
Alternative methods to animal toxicity testing
 
Screening of antihypertensive agents
Screening of antihypertensive agentsScreening of antihypertensive agents
Screening of antihypertensive agents
 

Semelhante a Screening of antimalarial drugs

Anti- Tumor assay / Screening of Anticancer Drugs
Anti- Tumor assay / Screening of Anticancer DrugsAnti- Tumor assay / Screening of Anticancer Drugs
Anti- Tumor assay / Screening of Anticancer DrugsPratik Parikh
 
Recent advances in treatment of malaria
Recent advances in treatment of malaria Recent advances in treatment of malaria
Recent advances in treatment of malaria Naser Tadvi
 
A review on stages of drug development and alternative methods for animal stu...
A review on stages of drug development and alternative methods for animal stu...A review on stages of drug development and alternative methods for animal stu...
A review on stages of drug development and alternative methods for animal stu...Frinto Francis
 
pharmacology practice school report.pptx
pharmacology practice school report.pptxpharmacology practice school report.pptx
pharmacology practice school report.pptxPharama slide share
 
pharmacologypracticeschoolreport-221219060301-1ca27004 (1).pdf
pharmacologypracticeschoolreport-221219060301-1ca27004 (1).pdfpharmacologypracticeschoolreport-221219060301-1ca27004 (1).pdf
pharmacologypracticeschoolreport-221219060301-1ca27004 (1).pdfManishJaat9
 
assswwwdocxxxxxxxdoc.pptx
assswwwdocxxxxxxxdoc.pptxassswwwdocxxxxxxxdoc.pptx
assswwwdocxxxxxxxdoc.pptxAbrhamKali
 
Pharmacological screening2 & tox. studies
Pharmacological screening2 & tox. studiesPharmacological screening2 & tox. studies
Pharmacological screening2 & tox. studiesNoor Alam
 
Evaluation of anticancer agents final
Evaluation of anticancer agents finalEvaluation of anticancer agents final
Evaluation of anticancer agents finalDr.Anup Thorat
 
BioSafety merged projects e budget.pptx
BioSafety merged projects e budget.pptxBioSafety merged projects e budget.pptx
BioSafety merged projects e budget.pptxHafezHawas1
 
Techniques for identification of bacterial and viral pathogens
Techniques for identification of bacterial and viral pathogensTechniques for identification of bacterial and viral pathogens
Techniques for identification of bacterial and viral pathogensAmbica Bora
 
animal toxicity studies.pptx
animal toxicity studies.pptxanimal toxicity studies.pptx
animal toxicity studies.pptxDrRenuYadav2
 
Current Guidelines on Malaria In Children
Current Guidelines on Malaria In ChildrenCurrent Guidelines on Malaria In Children
Current Guidelines on Malaria In ChildrenDr Anand Singh
 
Screening models for acute eye irritation & skin sentization
Screening models for acute eye irritation & skin sentizationScreening models for acute eye irritation & skin sentization
Screening models for acute eye irritation & skin sentizationpradnya Jagtap
 
Evaluation of Bactericidal and Bacteriostatic (Disinfectant). PHARMACEUTICAL ...
Evaluation of Bactericidal and Bacteriostatic (Disinfectant). PHARMACEUTICAL ...Evaluation of Bactericidal and Bacteriostatic (Disinfectant). PHARMACEUTICAL ...
Evaluation of Bactericidal and Bacteriostatic (Disinfectant). PHARMACEUTICAL ...Ms. Pooja Bhandare
 
Experimental Techniques For Evaluation Of New Drugs.ppt
Experimental Techniques For Evaluation Of New Drugs.pptExperimental Techniques For Evaluation Of New Drugs.ppt
Experimental Techniques For Evaluation Of New Drugs.pptKarabiAdak
 
Schedule y for toxicity studies
Schedule y for toxicity studiesSchedule y for toxicity studies
Schedule y for toxicity studiesKrushangiShah233
 

Semelhante a Screening of antimalarial drugs (20)

Anti- Tumor assay / Screening of Anticancer Drugs
Anti- Tumor assay / Screening of Anticancer DrugsAnti- Tumor assay / Screening of Anticancer Drugs
Anti- Tumor assay / Screening of Anticancer Drugs
 
Recent advances in treatment of malaria
Recent advances in treatment of malaria Recent advances in treatment of malaria
Recent advances in treatment of malaria
 
OECD Guidelines
OECD GuidelinesOECD Guidelines
OECD Guidelines
 
A review on stages of drug development and alternative methods for animal stu...
A review on stages of drug development and alternative methods for animal stu...A review on stages of drug development and alternative methods for animal stu...
A review on stages of drug development and alternative methods for animal stu...
 
pharmacology practice school report.pptx
pharmacology practice school report.pptxpharmacology practice school report.pptx
pharmacology practice school report.pptx
 
pharmacologypracticeschoolreport-221219060301-1ca27004 (1).pdf
pharmacologypracticeschoolreport-221219060301-1ca27004 (1).pdfpharmacologypracticeschoolreport-221219060301-1ca27004 (1).pdf
pharmacologypracticeschoolreport-221219060301-1ca27004 (1).pdf
 
assswwwdocxxxxxxxdoc.pptx
assswwwdocxxxxxxxdoc.pptxassswwwdocxxxxxxxdoc.pptx
assswwwdocxxxxxxxdoc.pptx
 
Pharmacological screening2 & tox. studies
Pharmacological screening2 & tox. studiesPharmacological screening2 & tox. studies
Pharmacological screening2 & tox. studies
 
Evaluation of anticancer agents final
Evaluation of anticancer agents finalEvaluation of anticancer agents final
Evaluation of anticancer agents final
 
OECD Guidelines
OECD GuidelinesOECD Guidelines
OECD Guidelines
 
BioSafety merged projects e budget.pptx
BioSafety merged projects e budget.pptxBioSafety merged projects e budget.pptx
BioSafety merged projects e budget.pptx
 
dermal toxicity.pptx
dermal toxicity.pptxdermal toxicity.pptx
dermal toxicity.pptx
 
Techniques for identification of bacterial and viral pathogens
Techniques for identification of bacterial and viral pathogensTechniques for identification of bacterial and viral pathogens
Techniques for identification of bacterial and viral pathogens
 
animal toxicity studies.pptx
animal toxicity studies.pptxanimal toxicity studies.pptx
animal toxicity studies.pptx
 
Current Guidelines on Malaria In Children
Current Guidelines on Malaria In ChildrenCurrent Guidelines on Malaria In Children
Current Guidelines on Malaria In Children
 
Screening models for acute eye irritation & skin sentization
Screening models for acute eye irritation & skin sentizationScreening models for acute eye irritation & skin sentization
Screening models for acute eye irritation & skin sentization
 
Evaluation of Bactericidal and Bacteriostatic (Disinfectant). PHARMACEUTICAL ...
Evaluation of Bactericidal and Bacteriostatic (Disinfectant). PHARMACEUTICAL ...Evaluation of Bactericidal and Bacteriostatic (Disinfectant). PHARMACEUTICAL ...
Evaluation of Bactericidal and Bacteriostatic (Disinfectant). PHARMACEUTICAL ...
 
OECD GUIDELINES.pptx
OECD GUIDELINES.pptxOECD GUIDELINES.pptx
OECD GUIDELINES.pptx
 
Experimental Techniques For Evaluation Of New Drugs.ppt
Experimental Techniques For Evaluation Of New Drugs.pptExperimental Techniques For Evaluation Of New Drugs.ppt
Experimental Techniques For Evaluation Of New Drugs.ppt
 
Schedule y for toxicity studies
Schedule y for toxicity studiesSchedule y for toxicity studies
Schedule y for toxicity studies
 

Último

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_.pdfSherif Taha
 
1029 - Danh muc Sach Giao Khoa 10 . pdf
1029 - Danh muc Sach Giao Khoa 10 . pdf1029 - Danh muc Sach Giao Khoa 10 . pdf
1029 - Danh muc Sach Giao Khoa 10 . pdfQucHHunhnh
 
Fostering Friendships - Enhancing Social Bonds in the Classroom
Fostering Friendships - Enhancing Social Bonds in the ClassroomFostering Friendships - Enhancing Social Bonds in the Classroom
Fostering Friendships - Enhancing Social Bonds in the ClassroomPooky Knightsmith
 
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).pptxVishalSingh1417
 
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 17Celine George
 
Understanding Accommodations and Modifications
Understanding Accommodations and ModificationsUnderstanding Accommodations and Modifications
Understanding Accommodations and ModificationsMJDuyan
 
FSB Advising Checklist - Orientation 2024
FSB Advising Checklist - Orientation 2024FSB Advising Checklist - Orientation 2024
FSB Advising Checklist - Orientation 2024Elizabeth Walsh
 
Micro-Scholarship, What it is, How can it help me.pdf
Micro-Scholarship, What it is, How can it help me.pdfMicro-Scholarship, What it is, How can it help me.pdf
Micro-Scholarship, What it is, How can it help me.pdfPoh-Sun Goh
 
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).pptxEsquimalt MFRC
 
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.pptxJisc
 
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 FellowsMebane Rash
 
Vishram Singh - Textbook of Anatomy Upper Limb and Thorax.. Volume 1 (1).pdf
Vishram Singh - Textbook of Anatomy Upper Limb and Thorax.. Volume 1 (1).pdfVishram Singh - Textbook of Anatomy Upper Limb and Thorax.. Volume 1 (1).pdf
Vishram Singh - Textbook of Anatomy Upper Limb and Thorax.. Volume 1 (1).pdfssuserdda66b
 
General Principles of Intellectual Property: Concepts of Intellectual Proper...
General Principles of Intellectual Property: Concepts of Intellectual Proper...General Principles of Intellectual Property: Concepts of Intellectual Proper...
General Principles of Intellectual Property: Concepts of Intellectual Proper...Poonam Aher Patil
 
Python Notes for mca i year students osmania university.docx
Python Notes for mca i year students osmania university.docxPython Notes for mca i year students osmania university.docx
Python Notes for mca i year students osmania university.docxRamakrishna Reddy Bijjam
 
Unit-IV- Pharma. Marketing Channels.pptx
Unit-IV- Pharma. Marketing Channels.pptxUnit-IV- Pharma. Marketing Channels.pptx
Unit-IV- Pharma. Marketing Channels.pptxVishalSingh1417
 
How to Manage Global Discount in Odoo 17 POS
How to Manage Global Discount in Odoo 17 POSHow to Manage Global Discount in Odoo 17 POS
How to Manage Global Discount in Odoo 17 POSCeline George
 
SOC 101 Demonstration of Learning Presentation
SOC 101 Demonstration of Learning PresentationSOC 101 Demonstration of Learning Presentation
SOC 101 Demonstration of Learning Presentationcamerronhm
 
Dyslexia AI Workshop for Slideshare.pptx
Dyslexia AI Workshop for Slideshare.pptxDyslexia AI Workshop for Slideshare.pptx
Dyslexia AI Workshop for Slideshare.pptxcallscotland1987
 

Último (20)

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
 
Mehran University Newsletter Vol-X, Issue-I, 2024
Mehran University Newsletter Vol-X, Issue-I, 2024Mehran University Newsletter Vol-X, Issue-I, 2024
Mehran University Newsletter Vol-X, Issue-I, 2024
 
1029 - Danh muc Sach Giao Khoa 10 . pdf
1029 - Danh muc Sach Giao Khoa 10 . pdf1029 - Danh muc Sach Giao Khoa 10 . pdf
1029 - Danh muc Sach Giao Khoa 10 . pdf
 
Fostering Friendships - Enhancing Social Bonds in the Classroom
Fostering Friendships - Enhancing Social Bonds in the ClassroomFostering Friendships - Enhancing Social Bonds in the Classroom
Fostering Friendships - Enhancing Social Bonds in the Classroom
 
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
 
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
 
Spatium Project Simulation student brief
Spatium Project Simulation student briefSpatium Project Simulation student brief
Spatium Project Simulation student brief
 
Understanding Accommodations and Modifications
Understanding Accommodations and ModificationsUnderstanding Accommodations and Modifications
Understanding Accommodations and Modifications
 
FSB Advising Checklist - Orientation 2024
FSB Advising Checklist - Orientation 2024FSB Advising Checklist - Orientation 2024
FSB Advising Checklist - Orientation 2024
 
Micro-Scholarship, What it is, How can it help me.pdf
Micro-Scholarship, What it is, How can it help me.pdfMicro-Scholarship, What it is, How can it help me.pdf
Micro-Scholarship, What it is, How can it help me.pdf
 
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
 
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
 
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
 
Vishram Singh - Textbook of Anatomy Upper Limb and Thorax.. Volume 1 (1).pdf
Vishram Singh - Textbook of Anatomy Upper Limb and Thorax.. Volume 1 (1).pdfVishram Singh - Textbook of Anatomy Upper Limb and Thorax.. Volume 1 (1).pdf
Vishram Singh - Textbook of Anatomy Upper Limb and Thorax.. Volume 1 (1).pdf
 
General Principles of Intellectual Property: Concepts of Intellectual Proper...
General Principles of Intellectual Property: Concepts of Intellectual Proper...General Principles of Intellectual Property: Concepts of Intellectual Proper...
General Principles of Intellectual Property: Concepts of Intellectual Proper...
 
Python Notes for mca i year students osmania university.docx
Python Notes for mca i year students osmania university.docxPython Notes for mca i year students osmania university.docx
Python Notes for mca i year students osmania university.docx
 
Unit-IV- Pharma. Marketing Channels.pptx
Unit-IV- Pharma. Marketing Channels.pptxUnit-IV- Pharma. Marketing Channels.pptx
Unit-IV- Pharma. Marketing Channels.pptx
 
How to Manage Global Discount in Odoo 17 POS
How to Manage Global Discount in Odoo 17 POSHow to Manage Global Discount in Odoo 17 POS
How to Manage Global Discount in Odoo 17 POS
 
SOC 101 Demonstration of Learning Presentation
SOC 101 Demonstration of Learning PresentationSOC 101 Demonstration of Learning Presentation
SOC 101 Demonstration of Learning Presentation
 
Dyslexia AI Workshop for Slideshare.pptx
Dyslexia AI Workshop for Slideshare.pptxDyslexia AI Workshop for Slideshare.pptx
Dyslexia AI Workshop for Slideshare.pptx
 

Screening of antimalarial drugs

  • 1. SCREENING METHODS OF ANTIMALARIAL DRUGS SUBMITTED BY ANUPAM PRAHLAD DEPT.OF PHARMACOLOGY
  • 2. MALARIA • Protozoal disease caused by parasites of the genus Plasmodium and transmitted to man by certain species of infected female anopheles mosquito.
  • 3. • Five species of the genus Plasmodium cause nearly all malarial infections in humans. ‐ Falciparum – life threatening ‐ Vivax ‐ Ovale ‐ Malariae ‐ Knowlesi (in Southeast Asia- the monkey malaria parasite )
  • 4.
  • 6. SCREENING METHODS IN VITRO METHODS 1. 3H hypoxanthine uptake 2. Giemsa stained slide method 3. Micro test 4. Flow cytometry 5. Measurement of ldh activity of p. Falciparum 6. Isobologram analysis IN VIVO METHODS 1. Plasmodium berghei 4 day suppression test 2. Hill’s test for causal prophylaxix and residual activity 3. Sporonoicidal activity testing 4. Plasmodium cynomolgi rhesus model
  • 7. 3H HYPOXANTHINE UPTAKE TEST • Most commonly used method for assessing antimalarial efficacy of a compound in vitro . • Hypoxanthine used by parasite for purine salvage and DNA synthesis. • Radiolabelled hypoxanthine uptake by parasite is an indicator of its growth and multiplication. • Parasites are cultured in different concentration of test compounds in media containing reduced concentration of hypoxanthine. • After which 3H Hypoxanthine is added.
  • 8. • Measurement of radioactivity by a 1205 betaplate reader. • Percent reductions are measured. Evalution % reduction = (mean cpm of test samples) 3H Hypoxanthine X 100 • Percent reductions are used to plot percentage inhibition of growth as a function of drug concentration. • IC 50 are determined by linear regression analyses
  • 9. GIEMSA STAINED SLIDE METHOD (MIC METHOD) • Low cost alternative for testing small number of compounds. • Parasites are incubated with test compound. • Parasitemia of control and treated groups are compared by counting Giemsa stained parasites by light microscopy. • Parasites incubated in 5% suspension of erythrocytes at 370C. • Change in the proportion of infected RBCs is assessed at end of 72 hr. at various concentrations of each drug
  • 10. • Drug is dissolved in 4% sucrose and fed ad libitum to the insects following the blood meal. • The level of drug activity can be calculated from a comparison of mean oocyst counts in treated and control batches.
  • 11. FLOW CYTOMETRY • Parasites are fixed after appropriate period of incubation with test compounds. • The parasite nuclei are stained with DAPI (42, 6- diamidino-2- phenylindole). • Counts of treated and control cultures are then obtained by flow cytometry.
  • 12. MICRO-TEST (MARK III) • Most commonly used method for the antimalarial testing for resistance • Provides information on the quantitative drug response of P. Falciparum . • test can be carried out with several drugs, in a micro test kit with 12 X 8 wells, predosed with chloroquine , mefloquine , quinine , amodiaquine , artemisinin , sulfadoxine (SDX)/ pyrimethamine (PYR) , pyrimethamine (PYR) • Patient’s blood sample is inoculated in the wells and incubated with suitable medium. • The number of schizonts is counted and compared with control well.
  • 13. • For monitoring the level and spread of resistance, molecular diagnostic methods for detecting resistant parasite have been proposed. • These molecular tools are based on the detection by PCR of point mutation in the parasite genome responsible for in vitro resistance
  • 14. ADVANTAGES OF IN VITRO METHODS • Precise and efficient • Rapid • Large number of compounds can be evaluated at the same time • Synergism or antagonism with drug combinations can be studied • Better assessment of intrinsic activity of a drug.
  • 15. LIMITATIONS OF IN VITRO METHODS • Drugs acting through active metabolite cannot be studied. • Non reproducibility of pharmacokinetic effects. • Toxic compounds also get selected. • Expertise and infrastructure needed • Lack of clinical correlation.
  • 16. IN VIVO METHODS • Compounds effective in in-vitro screening tests are taken up for in vivo evaluation. • Plasmodium species that cause human disease are unable to infect non primate animal models, • Rodent malaria parasite. P. berghei, P. yoelii, P. chabaudi, P. vinckei have been used extensively in drug discovery and early development.
  • 17. PLASMODIUM BERGHEI 4 DAY SUPPRESSION METHOD • Most widely used preliminary test. • Efficacy assessed by comparison of blood parasitemia and mouse survival time • Mice maintained at 220C at 50-70% humidity • Diet containing p-aminobenzoic acid 45 mg/kg and water ad libitum.
  • 18. • On day 0, mice are injected with 0.2 ml of aliquot (2X107 parasitized erythrocytes by Plasmodium berghei) • Experimental groups are (five each) : Vehicle treated (control group) Test drug treated group. Positive control group (chloroquine,reference drug) is administered.
  • 19. • On day 1 to 3, the experimental groups are treated. • On day 4, blood smears from all animals are prepared with Giemsa stain. • Parasitemia is determined microscopically by counting 4 fields of approximately 100 erythrocytes per field. • The difference between the mean value of the control group and those of the experimental groups is calculated. • Untreated control mice typically die approximately one week after infection
  • 20. • For treated mice mean survival time is calculated in comparison with the untreated and standard drug treated group • Mice without parasitemia on day 30 of post-infection are considered cured. • Compounds identified as active in this test are progressed through several of the following secondary tests. • In the ‘Dose ranging full four day test’, compounds are tested at four doses, by different routes of administration, to determine ED50 value. • This test also leads to information about relative potency and bioavailability
  • 21. Recrudescence test • Mice are administered with single dose of the test compound on day 3 of postinfection.  Control mice receive the suspension vehicle alone.  Blood smears are prepared at intervals of 12 h, 24h and then daily till day 33  and assessed for parasitemia • Results are expressed in terms of rapidity of onset of activity, time to onset of recrudescence, increase of parasitemia and duration of survival (in days). • Compounds are also tested for prophylactic activity by administrating them prior to infection, followed by daily examination of smears.
  • 22. HILL’S TEST FOR CAUSAL PROPHYLAXIS AND RESIDUAL ACTIVITY • In this model, mice (Charles River strain) are inoculated with P. yoelii (N67 strain) sporozoites. • Each mouse receives approximately 104-105 sporozoites intravenously in a total volume of 0.2ml. • For a compound to be considered truly causal prophylactic it must pass through four different phases
  • 23. PHASE 1 • Involves detection of causal prophylactic activity of the test compound in mice. • Test compound is administered 3hr after a sporozoite inoculation. • During 14 day period, blood films are taken • If parasitemia is not detected for 14 days the compound is considered to be fully protective.
  • 24. PHASE 2 • Compound is then tested for residual activity directed against blood stage parasites by administrating a single dose of the test compound . • After 48hr trophozoites are injected intravenously. • If the time interval to reach 2% parasitemia is similar to that of the control group, then it is considered that no residual activity has occurred
  • 25. PHASE 3 • Compounds suspected of prolonged residual activity are tested by administering sporozoites followed by the drug 3 h later. • After an additional 48h , 0.2 ml blood is and injected intraperitoneally into a clean mouse. • Blood films are examined for a 14 day . • Residual activity is noted if less than 50% of the recipients develop parasitemia . • A compound has no residual activity if 75% or more recipient mice develop patent infection.
  • 26. PHASE 4 • An additional procedure to clarify whether a compound has residual effect on erythrocytic stages. • Mice are injected intravenously with trophozoites 48 h after the compound administration.
  • 27. • After an additional 3-4 h, 0.2ml of blood is removed and injected to clean recipient mice. • Blood films are taken and a comparison of the time interval to reach 2% parasitemia is made with control mice • If the time interval is similar no residual activity is present
  • 28. SPORONOICIDAL ACTIVITY TESTING • Albino mice are administered with Plasmodium yoelii nigeriensis N 67 parasite on day 0. • Female A. stephensi mosquitoes are placed in containers. • On third day following infection , mosquitoes were starved for 24 h are allowed to feed on mice. • Presence of mature gamets is confirmed on blood film of mice. • The mice are then anaesthetized with a single dose of 60 mg/kg of sodium pentobarbitone i.p..
  • 29. • Mice laid on top of mosquito containers • Mosquitoes feed on them. • On the seventh day after the blood feed, a sample of each batch is removed and dissected. • Midguts are examined with the aid of semi-dark ground illumination and oocyst counts are made • The mean count for each batch is calculated • Drug is dissolved in 4% sucrose and fed ad libitum to the insects following the blood meal. • The level of drug activity can be calculated from a comparison of mean oocyst counts in treated and control batches
  • 30. IMMUNOCOMPROMISED MICE • A new in vivo mice model for antimalarial efficacy is designed which comprises of use of immunocompromised mice. • It can support Plasmodium falciparum infection as it lacks T and Lymphokine activated killer cells. • P. falciparum parasitized human red blood cells are grafted into immunodeficient mice. • For immunomodulation dichloromethylene diphosphate (Cl2MDP) is administered for tissue macrophages.
  • 31. • This is the first rodent model in which Plasmodium falciparum infection can be maintained. • Test drugs are administered when parasitemia becomes stable and smears show predominance of ring forms.
  • 32. PLASMODIUM CYNOMOLGI RHESUS MODEL • This model runs a close parallel to P. vivax infection in man. • It can be used to evaluate causal prophylactic, blood schizonticidal and hypnozoitocidal activity of a test compound in one model. • Young, tuberculin negative rhesus monkeys weighing 3.5 to 6 kg are used. • Each animal receives i.v. inoculum of approximately 500,000 sporozoites in 2 ml of fluid.
  • 33. • Drugs administered through a stomach tube once daily, commencing the day before infection and continuing up to day 8. • Blood films are made daily till 6 weeks • At the end of 6 weeks if the animals are still negetive, they are rechallenged with a similar inoculum to prove their susceptibility to infection. • All animals becoming infected during 4-6 weeks observation period and also infected animals from rechallenged group are further treated as soon as the parasitemia level reaches 0.1 to 0.5%. • The animals receive 7 daily oral doses of the drug and blood films are examined daily during and after therapy up to a total of 30 days.
  • 34. • If still negative, the animals are then examined twice weekly until they relapse. • If the parasites are not cleared by the drug during the primary attack, the animals are given 7 daily doses of 5mg/kg of chloroquine. • If no relapse follows chloroquine administration, it indicates that the test drug has destroyed the hypnozoites. • When no relapse occurs within 8-12 weeks, the animals are splenectomized. • Failure to develop further parasitemia within 4 weeks indicates that the animals are radically cured
  • 35. AVIAN MODELS • At least 447 species of birds have been found infected with malarial parasite. • The avian parasite infects nucleated erythrocytes. • The vectors of avian species are mosquitoes of the genera Aedes or Culex • Method: When only one or two birds need to be infected, parasitized blood can be obtained from the leg vein or wing vein of an infected bird.
  • 36. • When large number of chicks is to be infected from a single donor, blood is aspirated directly from the neck vein or from the heart. • Drugs may be administered to chicks orally, intravenously or intramuscularly the oral route is the method used more frequently. • Experimental birds are infected intravenously and receive the first dose of drug on day 1 followed by twice daily for the next 3 days. • Blood films are made on day 4. • Parasitemia achieved on day 4 in treated and untreated control group is then compared.