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Title: Introduction to Haematopoiesis
Description: 2nd Year Biomedical Science Degree. An introduction to different haematopoeitic stem cells and processes.
Description: 2nd Year Biomedical Science Degree. An introduction to different haematopoeitic stem cells and processes.
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L1 Introduction and Haematopoiesis
Body maintains output of blood cells through haematopoietic stem cells – HSCs in bone marrow
HSCs are multipotent – can form several cell types
HSCs can give rise to all blood cell types
Control of HSCs numbers
HSCs are self-renewing and proliferative – asymmetric division
Long term HSCs (LT-HSC) can self-renew – symmetric division
ST-HSC have limited self-renewal is more committed down a lineage
...
These then populate the foetal liver, thymus, spleen which take oer
haematopoiesis
This process is called definitive haematopoiesis
HSCs capable of reconstituting adult bone marrow (LT-HSCs) are first found in the foetal liver
Towards the end of gestation, LT-HSCs populate the bone marrow which becomes the primary source of
haematopoiesis in adults
The haematopoietic stem cell niche
At all stages of primitive and definitive haematopoiesis, the environment in which the HSC finds itself is
important for proper function
E
...
in the transition from primitive to definite haematopoiesis, the environment of the AGM is important for
formation of LT-HSCs
The bone marrow niche, which supports self-renewal and commitment to differentiation has several
components
o Cellular components
o Molecular components
Secreted ligands and their receptors
The extracellular matrix
Adhesion molecules
Chemical gradients
Bone marrow niche is vital for the proper regulation and function of HSCs
Cytokines, signalling molecules and transcription factors drive lineage specific differentiation
Megakaryocytes
A highly specialised cell that is responsible for
the production of platelets and their release into
the blood
They develop in the bone marrow from
haematopoietic stem cells and undergo
characteristic changes as they develop into
mature megs
Under times of high demand, platelet
production can increase by up to 20x
Cytokines: TPO
o Binding of TPO to cMpl drives a
signalling pathway which leads to the
proliferation and differentiation of
megakaryocytes and platelet production
o Liver and kidney produces TPO
o LOOK @ HANDOUT
TFs: GATA-1, FOG-1 & FLI-1
Signalling molecules: c-MPL
Many TFs are common to both megs and erythroid differentiation
But they have a couple specific factors the cause them to commit to one path
...
o Binding of FLI-1 to FOG via protein-protein interactions represses transcription on erythroid promoter
EKLF = erythroid lineage determining
o Binding of EKLF via DNA binding domain to erythroid promoter activates transcription downstream of
GATA/FOG
o Binding of EKLF to FOG via protein-proteins interaction represses transcription on meg promoter
TPO induced signalling and gene regulation that drives Meg/platelet production causes:
o Mature megakaryocyte to become polyploidy – this occurs by endomitosis, the replication of DNA
without cell division = cell gets really big
o Cytoplasmic maturation – the cytoplasm of mature megakaryocytes fills up with membranes, organells
and platelets specific proteins ready for packing into platelets
Platelets are anucleated cell fragments of megakaryocytes
However, all platelets are very consistent in their size shape and composition – platelet formation is highly
regulation -elegant process known as Proplatelet formation
Title: Introduction to Haematopoiesis
Description: 2nd Year Biomedical Science Degree. An introduction to different haematopoeitic stem cells and processes.
Description: 2nd Year Biomedical Science Degree. An introduction to different haematopoeitic stem cells and processes.