Lecture 12: Viral Protection and Therapeutics Flashcards
Why are most antibiotics ineffective at targeting viruses?
Most antibiotics inhibit the ribosome, which viruses do not have.
How does AZT work as an anti-viral therapeutic?
AZT is a nucleoside analog that has an azide group (N3) in place of the hydroxyl group (OH). This inhibits DNA chain extension during transcription. AZT = DNA CHAIN TERMINATOR
What is the effect of a missing dose of antiviral drug?
Partially-resistant virus will have time to develop a second mutation to become fully drug resistant.
How can multi-drug antiviral therapy help prevent viral resistance?
Multiple drugs can target different viral proteins at once so it can never become a fully resistant virus (ie. HAART therapy).
How can monoclonal antibodies be used as an antiviral therapeutic via humanizing a mouse?
Mice can be humanized. Immune system destroyed via irradiation and its bone marrow re-populated with human hematopoietic stem cells. Recover B cells from this mouse.
How are monoclonal antibodies made in the lab for therapeutics?
Synthesize a mouse antibody capable of targeting the chosen antigen in the lab. Chimerize the variable (Fab) region of a mouse antibody with the constant (Fc) region of a human antibody to get a human antibody that can recognize said target antigen. Express the chimeric antibody in a bacteria cell to multiply, harvest, and purify. Inject the final product directly into patient bloodstream to generate immediate immunity/therapeutic effects.
What are nanobodies? How can nanobodies be used in antiviral therapeutics?
Nanobodies are the first domain of only one chain of the variable (Fab) region of an antibody. This singular domain can be used to hit valleys/nooks in the virus surface. Then, nanobodies can be detected by another antibody, making easier to target the virus.
What is a soluble decoy receptor? How do immunotoxins and immunoadhesins act as soluble decoy receptors?
Soluble decoy receptors are soluble versions of the same receptor that the virus would usually bind to. That way, virus binds to these and not actual human cells. Link it to a toxin, and the toxin can kill infected cells. Link it to an adhesin or Fc portion of an antibody, and virus opsonization will induce macrophage phagocytosis.
What is the difference between prevention and treatment?
Prevention occurs before acquiring the pathogen (ie. vaccination). Exception: pre-exposure drugs. Treatment occurs after contracting the pathogen (ie. drugs and therapeutic antibodies). Exception: Some treatments can consist of injecting a vaccine if the virus has a long incubation period.
What is the host response to a vaccine?
Antibody production, leading to cell-mediated immunity
When did smallpox (Variola) first get treated? What was the change in case fatality?
First treated in 900 Ad via nasal insufflation (grind healing scabs and snort up nose). 30-40% fatality dropped to 1%
How did Jenner invent the smallpox vaccine in 1796?
In 1796, he inoculated boy’s arm with pus from healing cow pock.
What was significant about milkmaids?
Milkmaids infected with cowpox never got smallpox.
What are the 8 strategies for vaccine development? Which method is mostly a therapeutic and not so much a prevention method?
- Use harmless ANIMAL VIRUS in a different host
- Use ATTENUATED viruses, can be to the point it its unable to replicate
- Genetically engineer an ATTENUATED virus
- Use INACTIVATED/killed viruses
- Use SUBUNIT viruses, consists of just protein, peptide, or empty capsid
- DNA or RNA-BASED vaccine
- Engineer a live virus by INSERTING ANTIGEN GENE from a different virus.
- Adoptive transfer with mAbs, or Abs. [Therapeutic mostly]
Describe how the live-attentuated vaccine strategy was created.
Pasteur took serially passaged saliva from rabid dog into the brains of live rabbits. After doing this multiple times, he dried, ground up, and inocculated the rabbit’s spinal cord into a dog and human, which gave both immune protection.
