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Summary Immunodeficient Diseases Made Simple:

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Publié le
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Écrit en
2025/2026

A concise, high-yield guide summarizing primary and secondary immunodeficiencies, directly distilled from Janeway’s Immunobiology. Covers key immune defects, affected pathways, hallmark infections, and clinical presentations. Perfect for mastering the mechanisms behind immunodeficiency disorders and understanding their diagnostic and therapeutic relevance.

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Publié le
31 octobre 2025
Nombre de pages
32
Écrit en
2025/2026
Type
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TOPIC



IMMUNO3

FAILURE OF IMMUNE HOST DEFENSES
IMMUNODEFICIENCY DISEASES
• A history of repeated infections suggests a diagnosis of immunodeficiency.

2 TYPES OF IMMUNODEFICIENCIES

1. PRIMARY à
o Caused by inherited gene defects (congenital)

o Most gene defects resulting in immunodeficiency are recessive and many caused by mutations in X
chromosome

o For example SCID caused by mutations in gene IL2RG on X. Encodes IL-2 receptor. Mutation causes problem in
signaling of all 1L-2 family cytokines

§ IL7, IL15 don’t work and so T-cells and NK don’t develop properly

§ Defects in T cell development: no Tcell dependent Ab response nor cell mediated
responses
§ They have severe combined immunodeficiency (SCID)
2. SECONDARYà

,PROPERTY OF HIGHYIELD HUB CO -DO NOT COPY
o Acquired as consequence of other diseases or result of other issues such as starvation, medical
intervention

Examples of PRIMARY IMMUNODEFICIENCIES




IMMUNODEFICIENCIE DISEASES CAN HAVE

1) DEFECTS IN T CELL DEVELOPMENT CAN RESULT IN SEVERE COMBINED IMMUNODEFICIENCIES.

2) DEFECTS IN SIGNALING T-CELL ANTIGEN RECEPTORS CAN CAUSE SEVERE IMMUNODEFICIENCY.

3) DEFECTS IN B-CELL DEVELOPMENT RESULT IN DEFICIENCIES IN ANTIBODY PRODUCTION THAT CAUSE
AN INABILITY TO CLEAR EXTRACELLULAR BACTERIA AND SOME VIRUSES.


DEFECTS IN T CELL DEVELOPMENT CAN RESULT IN SEVERE COMBINED IMMUNODEFICIENCIES
§ Pathways that lead to circulating naïve B and T cells
§ Mutations in these pathways are shown in red and are known to cause human
immunodeficiency diseases

,PROPERTY OF HIGHYIELD HUB CO -DO NOT COPY

, PROPERTY OF HIGHYIELD HUB CO -DO NOT COPY
DEFECTS IN B-CELL DEVELOPMENT RESULT IN DEFICIENCIES IN ANTIBODY PRODUCTION THAT CAUSE AN
INABILITY TO CLEAR EXTRACELLULAR BACTERIA AND SOME VIRUSES




§ Born with high level maternal IgG (moves across placenta)
§ IgG starts at 6 months; Total IgG falls because maternal IgG catabolized
§ IgG levels are low from 3months to 1 year of infant
§ After birth, IgM starts immediately


PRODUCTION OF BTK GENE IMPORTANT FOR B CELL DEVELOPMENT

§ Stimulation of the Pre B-cell receptor recruits cytoplasmic proteins including BTK (Bruton’s
tyrosine kinase) to transduce a signal that triggers B cell development


DISEASE: BRUTONS X-GAMMAGLOBINEMIA
PRO B CELL CANNOT BE CONVERTED INTO PRE B CELL IN DEVELOPMENT THEREFORE RECEPTOR IS NOT
FUNCTIONAL AND NOT ABLE TO PRODUCE APPROPRIATE SIGNAL
• X LINKED RECESSIVE (MEANING YOU NEED 2 LITTLE R’s to have disease
• In X-linked agammaglobulinema (XLA) the BTK protein gene on X chrom. is defective
• In males with XLA no signal transduced even though receptor is there
• In females half of the pre-B cells will have be expressing the defective BTK gene and will not develop
further. This is since one of the two X chromosomes in each cell is permanently inactivated early in
development
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