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GMS 6551- Fundamentals Of Pharmacology: Discovery And Nomenclature Exam | Questions And Answers Latest {} A+ Graded | 100% Verified $13.48   Add to cart

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GMS 6551- Fundamentals Of Pharmacology: Discovery And Nomenclature Exam | Questions And Answers Latest {} A+ Graded | 100% Verified

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GMS 6551- Fundamentals Of Pharmacology: Discovery And Nomenclature Exam | Questions And Answers Latest {} A+ Graded | 100% Verified

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GMS 6551- Fundamentals Of Pharmacology: Discovery And Nomenclature Exam |
Questions And Answers Latest {2024- 2025} A+ Graded | 100% Verified


what do you do first when finding/developing a drug? - choose a disease:

-pharma made of companies

-tend to target diseases that have a large market

-government incentives to target orphan diseases (affects fewer than 200,000 people nationwide)



drug target - molecule the drug will interact with such as an enzyme, receptor, other protein, DNA, RNA,
etc.



selectivity - -target determines side effects

-easier to target non-human protein

-target mutated cancer protein



assay development - -in vitro

-in vivo

-ex vivo



examples of in vitro - test tube and cell culture



examples of in vivo - living animals



examples of ex vivo - tissue



what are some advantages of in vitro? - -fast - hundreds/thousands per day

-in expensive

-less red tape

-clean systems

, what are some disadvantages of in vitro? - a test tube or cell is NOT an animal



what are advantages to in vivo? - results more likely to translate to humans



what are disadvantages to in vivo? - -more expensive

-may cause suffering to animals

-regulations

-complex systems



lead compound - -first compound found that has the activity we want



how can we find a lead compound? - -natural products such as plants, algae, bacteria, fungi

-chemical banks - thousands or millions

-rational drug design- utilize side effect and alter natural ligand



computer-aided drug design/molecular docking - -crystal structures of many proteins known

-program calculates chemical attraction



what are some advantages to computer-aided drug design/molecular docking? - fast and cheap/free



what are some disadvantages to computer-aided drug design/molecular docking? - skips a lot of details
such as conformations and cell membrane



T/F: the larger release of gibbs free energy is going to predict stronger binding - True



structure activity relationships (SAR) - -optimize lead compound and functionalize

-test new compounds

-choose best compound

-functionalize new compound

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