All of the following are features of Lymph node histology except:

Red pulp and White pulp are present

Both Efferent and Afferent are present

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

Cells and Organs of Immune System for UPSC-CMS: High-Yield Microbiology Lessons

Primary Lymphoid Organs - Immune Cell Nurseries

Primary Lymphoid Organs (PLOs) are sites where lymphocytes develop and mature from progenitor cells, becoming immunocompetent.

Bone Marrow (BM)
- Central site for hematopoiesis; origin of all immune cells (lymphoid and myeloid progenitors).
- Maturation site for B-lymphocytes and Natural Killer (NK) cells.
- Contains Hematopoietic Stem Cells (HSCs).
Thymus
- Bi-lobed organ in anterior superior mediastinum; crucial for T-cell maturation & selection.
- Structure: Outer cortex (densely packed immature thymocytes, positive selection) and inner medulla (mature thymocytes, negative selection, Hassall's corpuscles).
- Undergoes age-related involution (atrophy).
- 📌 Selection Mnemonic: "Be Positive you can bind MHC in the Cortex; Be Negative about self-reactivity in the Medulla."

Comparison: Bone Marrow vs. Thymus

Feature	Bone Marrow	Thymus
Primary Role	Hematopoiesis; B-cell & NK cell maturation	T-cell maturation & selection
Key Output	Naive B-cells, Immature T-cells (pro-T)	Mature, self-tolerant Naive T-cells

⭐ DiGeorge Syndrome (chromosome 22q11.2 deletion) is characterized by thymic aplasia/hypoplasia, leading to deficient T-cell mediated immunity and recurrent infections.

Secondary Lymphoid Organs - Battlegrounds & Hubs

Organ	Key Features / Zones	Main Functions
Lymph Nodes	Cortex (B-cell follicles), Paracortex (T-cells, HEVs), Medulla	Filter lymph, Ag presentation, activate lymphocytes
Spleen	White Pulp (PALS: T-cells; Follicles: B-cells), Red Pulp	Filter blood, respond to blood-borne Ags, remove old RBCs
MALT (e.g., Peyer's Patches)	Submucosal lymphoid aggregates, M-cells for Ag uptake	Mucosal immunity, local Ag sampling

HEVs (High Endothelial Venules) in LNs facilitate lymphocyte entry.
M-cells in MALT transport luminal antigens.
⭐ > Post-splenectomy: ↑ risk of sepsis from encapsulated bacteria (S. pneumoniae, H. influenzae, N. meningitidis). 📌 SHiN.

Innate Immune Cells - First Responders

Rapid, non-specific defense. Key players include:

Cell Type	Key Features & Functions	Key Markers
Neutrophils	Most abundant phagocyte; multi-lobed nucleus; NETosis; acute inflammation.	CD15, CD16b, MPO
Macrophages	Phagocytosis; antigen presentation; cytokine production (TNF-α, IL-1, IL-6); tissue repair.	CD14, CD68, CD11b
Dendritic Cells	Potent APCs; link innate & adaptive immunity; initiate T-cell response.	CD11c, MHC-II, CD80/86
NK Cells	Kill virus-infected/tumor cells (perforin, granzymes); ADCC; no antigen-specific receptor.	CD16, CD56

-   **Mast Cells:** Release histamine; allergy, anaphylaxis.
-   **Eosinophils:** Combat parasitic infections; allergic reactions. Markers: MBP.
-   **Basophils:** Release histamine, heparin; allergic inflammation. Markers: CD203c.

⭐ Toll-Like Receptors (TLRs) on macrophages and dendritic cells recognize Pathogen-Associated Molecular Patterns (PAMPs), initiating innate immune responses.

Immune Cell Lineage and Surface Markers

Adaptive Immune Cells - Specialized Forces

T-lymphocytes (T-cells): Cell-mediated immunity. Mature in Thymus.
- Helper T (Th): CD4+. Orchestrate response. Subsets: Th1 (IFN-γ), Th2 (IL-4, IL-5), Th17 (IL-17).
- Cytotoxic T (CTL): CD8+. Kill infected & tumor cells.
- Regulatory T (Treg): CD4+, CD25+, FOXP3+. Suppress immunity, maintain tolerance.
- 📌 Rule of 8: $CD4 \times MHCII = 8$; $CD8 \times MHCI = 8$.
B-lymphocytes (B-cells): Humoral immunity. Mature in Bone marrow.
- Differentiate: Plasma cells (Antibody factories: IgM, IgG, IgA, IgE) & Memory B-cells (rapid recall).
- Markers: CD19, CD20, CD21.

⭐ IL-2, from activated T-cells, is vital for T-cell proliferation & differentiation.

T-cell subsets and their roles in immune responses and B-cell differentiation into plasma and memory cells)

High‑Yield Points - ⚡ Biggest Takeaways

Primary lymphoid organs are Bone Marrow (B-cell maturation) and Thymus (T-cell maturation).

Secondary lymphoid organs (Spleen, Lymph Nodes, MALT) are sites of antigen encounter and immune response initiation.

T-cell education in the thymus involves positive selection (MHC restriction) and negative selection (self-tolerance).

B-cell maturation in bone marrow involves negative selection to eliminate self-reactive B cells.

CD4+ T-cells (Helper T cells) recognize MHC Class II; CD8+ T-cells (Cytotoxic T cells) recognize MHC Class I.

Dendritic cells are the most potent professional Antigen Presenting Cells (APCs).

Natural Killer (NK) cells mediate innate immunity against virally infected/tumor cells and perform ADCC (Antibody-Dependent Cell-mediated Cytotoxicity).

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