Anaemia of Chronic Disorders (ACD) Lecture Notes PDF

Summary

This document is an academic lecture on anaemia of chronic disorders (ACD), detailing its definition, causes, pathogenesis, laboratory investigation, and treatment. The lecture is focused on explaining the clinical aspects of ACD and its associated systemic disorders.

Full Transcript

Anaemia of chronic disorders
(ACD)

by
Dr. Teeb M. Jaafar
MBCh.B / F.I.C.M.S. (Path)
 Topics

Definition of anemia of chronic disorders.
Causes
Pathogenesis
Laboratory investigation
Differential diagnosis
Peripheral blood smear and bone marrow study
ESR and CRP comparison
Treatment
 Objectives

At the end of the lecture you will be able to :

Define anemia of chronic disorders and enumerate its causes.
Explain its pathogenesis.
Mention its important lab. Investigation.
Differentiate between it and similar conditions.
Enumerate the peripheral blood and bone marrow finding in each causative
underlying disease.
Compare between ESR and CRP.
Summarize its treatment.
 Anaemia of chronic disorders (ACD)

Many of the anemias seen in clinical practice occur in patients with systemic
disorders and are the result of a number of contributing factors. The anaemia of
chronic disorders (ACD) is of central importance and occurs in patients with a
variety of chronic inflammatory and malignant diseases.
Usually, both the erythrocyte sedimentation rate (ESR) and C‐reactive protein
(CRP) are raised.
It may be complicated by additional hematological changes due to the disease
such as anemias from other causes (e.g. iron or folate deficiency, bone marrow
infiltration, hypersplenism or endocrine abnormality).
 Causes
Chronic inflammatory diseases

 Infectious (e.g. pulmonary abscess, tuberculosis, osteomyelitis, pneumonia, bacterial
endocarditis and some viral and parasitic infection)
 Non‐infectious (e.g. rheumatoid arthritis, systemic lupus erythematosus and other
connective tissue diseases, sarcoid, Crohn’s disease and liver cirrhosis)

Malignant disease
(e.g. carcinoma, lymphoma, sarcoma, myeloma).

Chronic Renal failure.
Chronic Liver diseases
 Pathogenesis
1. Decreased release of iron from macrophages to plasma because of raised serum hepcidin
levels:

Hepcidin is a polypeptide produced by liver cells. It is the major hormonal regulator of iron
homeostasis. It inhibits iron release from macrophages and from intestinal epithelial cells by
its interaction with the transmembrane iron exporter, ferroportin. It accelerates degradation
of ferroportin mRNA. Raised hepcidin levels therefore profoundly affect iron metabolism by
reducing its absorption and release from macrophages.

When iron stores are adequate or high, increased hepcidin expression inhibits:
1. intestinal iron absorption.
2. release of recycled iron from macrophages.
3. its transport across the placenta.
Hepcidin synthesis is increased by:
a. transferrin saturation.
b. Inflammation.
while hepcidin synthesis is reduced by:
a. Increased erythropoiesis.
b. Erythropoietin.
c. Hypoxia.
d. Matriptase.

2. Reduced red cell lifespan.

3. An inadequate erythropoietin response to anaemia caused by the effects of cytokines and tumor
necrosis factor (TNF) on erythropoiesis :

The plasma levels of various cytokines, especially interleukin (IL – 1& IL – 6) and tumor necrosis factor
(TNF) are raised and reduce erythropoietin secretion.
 Clinical features
These patients usually presented with signs and symptoms of anemia (pallor,
dizziness, tiredness, palpitation, etc.) in addition to signs and symptoms of the
underlying disease.
 Lab. Findings
1. Mild to moderate anaemia (hemoglobin rarely