Which of the following vaccines is currently used as a live attenuated vaccine in routine immunization programs?

Inactivated Polio Vaccine (IPV)

The following statements are true about DPT vaccine except

Presence of acellular pertussis component increases its immunogenicity

Whole killed bacteria of Bordetella pertussis has an adjuvant effect

Aluminium salt has an adjuvant effect

Presence of Hemophilus influenza type B component increases the immunogenicity of pertussis component

Live vaccines are contraindicated in all except:

Patients on high-dose immunosuppressants

True about chicken pox -

Caused by varicella-zoster virus

Types of Vaccines for NEET-PG: High-Yield Microbiology Lessons

Overview of Vaccine Types - Immune Kickstarters

Principle: Stimulate adaptive immunity (B-cells, T-cells, memory) to a pathogen without causing disease. Mimics natural infection.
Broad Categories:
- Live-attenuated (e.g., MMR, BCG)
- Inactivated/Killed (e.g., Salk Polio, Rabies)
- Subunit (Protein, Polysaccharide, Conjugate) (e.g., Hep B)
- Toxoid (e.g., Tetanus, Diphtheria)
- Viral Vector (Recombinant) (e.g., some COVID-19)
- Nucleic Acid (mRNA, DNA) (e.g., some COVID-19)

⭐ Live attenuated vaccines generally induce robust, long-lasting immunity (cellular & humoral) often with a single dose.

Live Attenuated Vaccines - Weakened Warriors

Contain weakened (attenuated) live organisms; mimic natural infection to induce robust immunity.
Immunity: Potent, long-lasting (humoral & cellular). Often lifelong with 1-2 doses (except oral).
Advantages: Strong immune response, fewer doses needed.
Disadvantages:
- Potential reversion to virulence (rare).
- ⚠️ Contraindicated: Immunocompromised individuals, pregnancy (most).
- Circulating antibody interference.
- Strict cold chain essential.
📌 Mnemonic: BOY TRICS GETS MMR (BCG, OPV, Yellow fever, Typhoid oral, Rotavirus, Influenza intranasal, Chickenpox, Smallpox, MMR).

⭐ OPV (Sabin) provides strong intestinal immunity (IgA) but carries a risk of Vaccine-Associated Paralytic Poliomyelitis (VAPP) (approx. 1 in 2.7 million first doses).

Inactivated (Killed) Vaccines - Neutralized Foes

Whole bacteria/viruses killed by heat/chemicals (e.g., formalin, β-propiolactone); non-infectious.
Key Features:
- Cannot replicate or cause disease; no reversion to virulence.
- Safer profile, suitable for immunocompromised individuals.
Immune Response:
- Mainly humoral (antibody) immunity; less cell-mediated response.
- Less immunogenic than live vaccines.
- Requires multiple doses (priming, boosters) & often adjuvants.
Examples:
- Viral: Influenza (shot), Polio (Salk/IPV), Rabies, Hepatitis A.
- Bacterial: Pertussis (wP), Typhoid (parenteral), Cholera.

⭐ Salk vaccine (IPV), an inactivated polio vaccine, prevents poliomyelitis without risk of vaccine-associated paralytic polio (VAPP).

Component Vaccines - Purified Parts

Uses specific antigenic components of pathogens, not whole organisms.
Advantages: ↓ reactogenicity, ↑ safety, suitable for immunocompromised (if not live).

Polysaccharide Vaccines
- Capsular polysaccharides (e.g., Pneumococcal - PPSV23, Vi Typhoid).
- T-cell independent response; poor in <2 yrs age.
Conjugate Vaccines
- Polysaccharide + protein carrier (e.g., Hib, Pneumococcal - PCV13, MenC).
- T-cell dependent response; effective in infants.
Recombinant Protein Vaccines
- Gene for antigen inserted into host (e.g., yeast for Hep B surface Ag - HBsAg; HPV vaccine - L1 protein).
Toxoid Vaccines
- Inactivated bacterial toxins (e.g., Tetanus, Diphtheria).
- Immunity to toxin, not organism.

Polysaccharide vs. Protein-Polysaccharide Conjugate Vaccines

⭐ Hepatitis B vaccine is a classic example of a recombinant subunit vaccine, produced by inserting the gene for HBsAg into yeast cells (e.g., Saccharomyces cerevisiae).

Newer Vaccine Technologies - Cutting-Edge Shields

mRNA Vaccines: mRNA (antigen-coding) → host cell production → immunity.
- Rapid development. E.g., Pfizer, Moderna (COVID-19).
Viral Vector Vaccines: Harmless virus delivers pathogen genes.
- E.g., AstraZeneca (Adenovirus), rVSV-ZEBOV (Ebola).
DNA Vaccines: Plasmid DNA (antigen gene) → host cell expression.
- Strong T-cell response.
VLPs (Virus-Like Particles): Non-infectious viral protein shells.
- Highly immunogenic. E.g., HPV.

Conventional and Nucleic Acid Vaccine Types

⭐ mRNA vaccines: rapid development, potent humoral & cellular immunity.

High‑Yield Points - ⚡ Biggest Takeaways

Live attenuated: Strongest immunity (IgA/IgG), risk reversion; contraindicated: immunocompromised (BCG, OPV, MMR).

Killed/Inactivated: Safer, humoral immunity, need boosters (IPV, Rabies, Influenza shot).

Toxoids: Inactivated bacterial toxins (Tetanus, Diphtheria), form antitoxin antibodies.

Subunit/Acellular: Use specific purified antigens (Hepatitis B, acellular Pertussis).

Conjugate: Link polysaccharide to protein carrier for T-cell response in infants (PCV, Hib).

Recombinant vaccines: Produced by genetic engineering (e.g., Hepatitis B, HPV).

mRNA/DNA vaccines: Deliver genetic material for host cells to synthesize antigens.

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Types of Vaccines