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NURS 6501N Week 10 Case Study: Chlamydia Pathophysiology & Immune Evasion.

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NURS 6501N Week 10 Case Study: Chlamydia Pathophysiology & Immune Evasion.

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July 21, 2025
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2024/2025
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WK10ASSGMENT - WEEK 10 ASSIGNMENT




NURS 6501N Week 10 Case Study : Chlamydia Pathophysiology & Immune
Evasion.


Week 10 Case Study Assignment




®™

, WK10ASSGMENT - WEEK 10 ASSIGNMENT


Week 10 Case Study Assignment

The pathophysiologic process of chlamydia, Intracellular development, and immune
evasion.

Chlamydia, an intracellular pathogen, is intricately dependent on host cells for vital

nutrients, particularly adenosine triphosphate (ATP), which is indispensable for its energy

generation and overall survival (Wang et al., 2024). To flourish within its host environment,

Chlamydia has a range of complex strategies to elude the innate immune system, and this

adaptation not only enhances its ability to acquire essential nutrients but also allows it to

manipulate immune responses, particularly in times of nutritional scarcity (Wang et al., 2024).

Chlamydia muridarum predominantly infects rodents, while Chlamydia psittaci targets avian

species and humans. Chlamydia pneumoniae, which is associated with respiratory infections, and

Chlamydia trachomatis (CT) are recognized as leading culprits behind sexually transmitted

infections (STIs) and a significant cause of preventable blindness, clinically presenting with

minimal or no symptoms (Jury et al., 2023).

According to Wang et al. (2024), CD4+ Th1 cytokine responses are vital in establishing

protective immunity against C. trachomatis infections and reinfections, whereas CD8+ T cells

play a relatively minor role in this critical immune defense. Upon entering host cells, C.

trachomatis is met by an innate immune response that acts as the body's vigilant "guards." Mast

cells, the frontline defenders, attempt to engulf and eliminate the invading pathogen, which

triggers dendritic cells to process and present antigens from C. trachomatis to T cells, the

"commanders" of the adaptive immune response, utilizing MHC-I and MHC-II molecules (Wang

et al., 2024). Additionally, interferon-gamma (IFN-γ) produced by activated T cells and natural

killer (NK) cells bolsters macrophage activation, transforming them into the "combat troops" that

ensure enhanced immunity against C. trachomatis both locally within tissues and throughout the




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