Which of the following statements about the secondary immune response is false?

Immune response against a subsequent antigenic challenge is absent.

The lag period is absent or significantly shorter.

There is a negative phase in the response.

Only T-dependent antigens are recognized.

All are true regarding the development of T-cells, except?

T-cells are located in mantle layer of spleen

T-cells are formed in bone marrow

In lymph nodes, T-cells are found in paracortical area

Maturation of T-cells take place in thymus

Which of the following statements regarding rejection of solid organ transplants is true?

Hyperacute rejection begins in the operating room with reperfusion of the transplanted organ

Most immunosuppressive medications are used to prevent chronic rejection

The major cause of graft failure is acute rejection

Liver transplants are especially susceptible to hyperacute rejection

All of the following are functions of the spleen EXCEPT?

Initiation of adaptive immune response from filtration of lymph.

Clearance of damaged or aged red blood cells (RBCs) from the blood.

Extramedullary site for hematopoiesis and recycling iron.

Clearance of encapsulated bacteria from the bloodstream.

The biconcave shape of RBC is useful for all the following functions EXCEPT:

Increasing surface area for diffusion

Allows considerable alteration in cell volume

Passing easily through smaller capillaries

Immunological Memory and Tolerance for UPSC-CMS: High-Yield Physiology Lessons

Immunological Memory - Remember Me?

Immunological memory is the immune system's ability to mount an enhanced, faster, and more effective response to subsequent encounters with a previously encountered antigen.

Primary vs. Secondary Immune Response

Feature	Primary Response	Secondary Response
Speed	Slower (days to weeks)	Faster (hours to days)
Magnitude	Lower	Higher (↑100-1000x)
Predominant Ab	IgM	IgG (class switching), IgA, IgE
Antibody Affinity	Lower	Higher
Lag Phase	Longer	Shorter

Key Cells:
- Memory B cells
- Memory T cells (CD4+ & CD8+)
Hallmarks:
- Specificity
- Longevity (can be lifelong)
- Rapidity (quicker activation)
- Heightened reactivity (stronger response)

Primary vs Secondary Immune Response Kinetics

⭐ Secondary response is characterized by a rapid switch to IgG production with higher affinity antibodies due to somatic hypermutation and affinity maturation during the primary response.

Memory Cell Deep Dive - The Veteran Cells

Memory B Cells:
- Formation: Germinal centers.
- Surface marker: CD27.
- Function: Rapid differentiation to plasma cells, affinity-matured antibodies.

Memory T Cells:

General marker: CD45RO. 📌 ROund for memORy (CD45RO), RA for NAive (CD45RA).

Types:

Type	Location	Key Function(s)	Key Markers
Central ($T_{CM}$)	SLOs	Proliferate, differentiate to effectors	CCR7, CD62L
Effector ($T_{EM}$)	Periphery, blood	Rapid effector functions (cytokine release)	CCR7-, CD62L-
Tissue-Res. ($T_{RM}$)	Non-lymphoid tissues	Barrier defense, rapid local response	CD69, CD103

Survival & Self-renewal: Maintained by cytokines IL-7 and IL-15.

⭐ Central memory T cells ($T_{CM}$) primarily reside in secondary lymphoid organs, express CCR7 and L-selectin (CD62L), and have high proliferative capacity upon re-exposure to antigen.

Memory T cell subsets and characteristics

Immunological Tolerance - The Peace Treaty

Definition: Specific unresponsiveness to an antigen (especially self), preventing autoimmunity & maintaining self-non-self discrimination.
Types & Mechanisms:
- Central Tolerance:
  - Location: Thymus (T cells), Bone Marrow (B cells).
  - Key Process: Deletion (apoptosis) of self-reactive lymphocytes.
- Peripheral Tolerance:
  - Location: Secondary lymphoid organs, peripheral tissues.
  - Key Processes: Anergy, suppression by Tregs, deletion.
Factors Favoring Tolerance: High antigen dose, persistence, oral/IV route, absent co-stimulation, neonatal exposure.

⭐ The AIRE (Autoimmune Regulator) protein is crucial for expressing diverse tissue-specific antigens in the thymus, essential for central T cell tolerance.

Tolerance Mechanisms - Keeping a Lid On It

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High‑Yield Points - ⚡ Biggest Takeaways

Immunological memory underpins vaccination, causing faster, stronger secondary responses via memory cells.

Memory B cells rapidly secrete high-affinity IgG upon antigen re-encounter.

Memory T cells (TCM & TEM) provide long-term cellular immunity.

Immunological tolerance prevents autoimmunity by maintaining unresponsiveness to self-antigens.

Central tolerance eliminates self-reactive lymphocytes via negative selection in primary lymphoid organs.

Peripheral tolerance uses anergy, Treg (FoxP3+) suppression, and AICD (Activation-Induced Cell Death).

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