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Primary Lymphoid Organs : Where Immune Cells Develop
• HSCs take up residence in the bone marrow, which remains the primary site of
hematopoiesis throughout adult life.
• The bone marrow supports the maturation of all erythroid and other myeloid cells and, in
humans.
• HSCs are also found in blood and may naturally recirculate between the bone marrow and
other tissues.
Stem Cells
• They have the capacity to give rise to lineages of differentiated cells, and they are self-
renewing—each division of a stem cell creates at least one stem cell.
• stem cells are classified according to their descent and developmental potential, three levels
of stem cells can be recognized: pluripotent, multipotent, and unipotent.
• Pluripotent stem cells :-
() can give rise to an entire organism.
() A fertilized egg, the zygote, is an example of such a cell.
() In humans, the initial divisions of the zygote and its descendants produce cells
that are also pluripotent.
• Multipotent stem cells :-
()These Cells arise from embryonic stem cells and can give rise to a more limited
range of cell types.
• Unipotent stem cells :-
() Further differentiation of multipotent stem cells leads to the formation of
unipotent stem cells.
() it can generate only the same cell type as themselves.
Type of Transplantations
Autologus Syngeneic Allogeneic
The Recipient is
also the Donor
The donor and recipient are
genetically identical
The donor and Recipient
are not genetically
identical
No chance of
Rejection
Low chance of Rejection
small immunosuppressant
are needed
High chance of Rejection
Life threatening Affliction
Graft Versus Host Disease
(GVHD).
Main Sources of HSCs
Bone Marrow Umblical Cord
Umbilical cord contains High frequency
of HSCs which is produced by placental
Cells
Bone Marrow the Main Site of Hematopoiesis
• It is responsible for maintaining the pool of HSCs throughout the life of an adult
vertebrate and regulating their differentiation into all blood cell types.
• outside surface of a bone is hard, the inside or marrow, also known as the medullary
cavity, is sponge-like and packed full of cells.
• The medullary cavity can be divided into the endosteal niche, lining the bone, and the
perivascular niche, lining the blood. vessels that run through the center of the bone.
• Quiescent, long-lived HSCs are found in the perivascular niche, nurtured by perivascular
and endothelial cells.
• Some HSCs remain quiescent, while others divide and differentiate into progenitors that
develop into myeloid or lymphoid lineages.
• B lymphocytes complete most of their development in the bone marrow.
• More mature B cells are found in the central sinuses of the bone marrow and exit the
bone marrow to complete the final stages of their maturation in the spleen.
• Progenitors of T lymphocytes arise from bone marrow HSCs but exit at a very immature
stage and complete their development in the thymus, the primary lymphoid organ for T-
cell maturation.
• Progenitors of T lymphocytes arise from bone marrow HSCs but exit at a very immature
stage and complete their development in the thymus, the primary lymphoid organ for T-
cell maturation
The Thymus is the Primary Lymphoid Organ Where T Cells Mature
• From initial founding regarding the Thymus it is known as Graveyard of Dead and decaying
lymphocytes.
• The cells that populated in it—small, thin-rimmed, featureless cells—looked dull and
inactive.
• But after 1960s J.F.A.P Miller and Australian Biologist Recognize it as Much more than a
Graveyard of Dead decaying lymphocytic cells.
• However, Miller proved that the thymus was the all-important site for the maturation of T
lymphocytes.
• T-cell progenitors, which still retain the ability to give rise to multiple hematopoietic cell
types, travel via the blood from the bone marrow to the thymus
• The thymus is a specialized environment where immature T cells, known as thymocytes,
mature into functional T cells
• Thymocytes ultimately generate unique antigen receptors .
• T – Cells are selected to mature on the basis of their TCR reactivity to self-peptide/MHC
complexes expressed on the surface of thymic epithelial cells.
• Thymocytes whose TCRs bind self-MHC/peptide complexes with too-high affinity are
induced to die (negative selection)
• thymocytes that bind self-MHC/peptides with intermediate affinity undergo positive
selection and mature, migrating to the thymic medulla before entering the circulation.
• The majority of cells die because they have too-low affinity for the self-peptide/MHC
combinations that they encounter on the surface of thymic epithelial cells and fail to undergo
positive selection, a process called death by neglect.
T-cell development And Thymic Microenvironment
• T-cell precursors enter the thymus in blood vessels at the corticomedullary junction between
the thymic cortex, the outer portion of the organ, and the thymic medulla, the inner portion of
the organ.
• Thymocytes first travel to the subcapsular cortex, just beneath the capsule of the thymus,
where they proliferate.
• They then travel to the cortex, where they first express mature TCRs and interact with cortical
thymic epithelial cells (cTECs)
• Thymocytes that are positively selected in the cortex continue to mature and travel to the
medulla, where they interact with medullary thymic epithelial cells (mTECs).
• Negative selection can happen in any of the microenvironments.
• Thymocytes are also distinguished by their expression of two CD antigens, CD4 and CD8
• The most immture thymocytes doesn’t express any CD antigens And they termed as Double
Negative (DN).
• After entering the cortex, thymocytes upregulate both CD4 and CD8 antigens, becoming
double positive (DP).
• As they mature, they lose one or the other CD antigen, becoming single positive (SP).
• CD4 T cells are helper cells and CD8 T cells are cytotoxic (killer) cells.
• Mature SP cells exit the thymus as they entered: via the blood vessels of the corticomedullary
junction.
• Maturation is finalized in the periphery, where these new T cells (recent thymic emigrants)
explore antigens presented in secondary lymphoid tissue, including the spleen and lymph nodes.

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Primary lymphatic organs system of human

  • 1. Primary Lymphoid Organs : Where Immune Cells Develop • HSCs take up residence in the bone marrow, which remains the primary site of hematopoiesis throughout adult life. • The bone marrow supports the maturation of all erythroid and other myeloid cells and, in humans. • HSCs are also found in blood and may naturally recirculate between the bone marrow and other tissues.
  • 2. Stem Cells • They have the capacity to give rise to lineages of differentiated cells, and they are self- renewing—each division of a stem cell creates at least one stem cell. • stem cells are classified according to their descent and developmental potential, three levels of stem cells can be recognized: pluripotent, multipotent, and unipotent. • Pluripotent stem cells :- () can give rise to an entire organism. () A fertilized egg, the zygote, is an example of such a cell. () In humans, the initial divisions of the zygote and its descendants produce cells that are also pluripotent. • Multipotent stem cells :- ()These Cells arise from embryonic stem cells and can give rise to a more limited range of cell types. • Unipotent stem cells :- () Further differentiation of multipotent stem cells leads to the formation of unipotent stem cells. () it can generate only the same cell type as themselves.
  • 3. Type of Transplantations Autologus Syngeneic Allogeneic The Recipient is also the Donor The donor and recipient are genetically identical The donor and Recipient are not genetically identical No chance of Rejection Low chance of Rejection small immunosuppressant are needed High chance of Rejection Life threatening Affliction Graft Versus Host Disease (GVHD).
  • 4. Main Sources of HSCs Bone Marrow Umblical Cord Umbilical cord contains High frequency of HSCs which is produced by placental Cells
  • 5. Bone Marrow the Main Site of Hematopoiesis • It is responsible for maintaining the pool of HSCs throughout the life of an adult vertebrate and regulating their differentiation into all blood cell types. • outside surface of a bone is hard, the inside or marrow, also known as the medullary cavity, is sponge-like and packed full of cells. • The medullary cavity can be divided into the endosteal niche, lining the bone, and the perivascular niche, lining the blood. vessels that run through the center of the bone. • Quiescent, long-lived HSCs are found in the perivascular niche, nurtured by perivascular and endothelial cells. • Some HSCs remain quiescent, while others divide and differentiate into progenitors that develop into myeloid or lymphoid lineages. • B lymphocytes complete most of their development in the bone marrow. • More mature B cells are found in the central sinuses of the bone marrow and exit the bone marrow to complete the final stages of their maturation in the spleen. • Progenitors of T lymphocytes arise from bone marrow HSCs but exit at a very immature stage and complete their development in the thymus, the primary lymphoid organ for T- cell maturation. • Progenitors of T lymphocytes arise from bone marrow HSCs but exit at a very immature stage and complete their development in the thymus, the primary lymphoid organ for T- cell maturation
  • 6. The Thymus is the Primary Lymphoid Organ Where T Cells Mature • From initial founding regarding the Thymus it is known as Graveyard of Dead and decaying lymphocytes. • The cells that populated in it—small, thin-rimmed, featureless cells—looked dull and inactive. • But after 1960s J.F.A.P Miller and Australian Biologist Recognize it as Much more than a Graveyard of Dead decaying lymphocytic cells. • However, Miller proved that the thymus was the all-important site for the maturation of T lymphocytes. • T-cell progenitors, which still retain the ability to give rise to multiple hematopoietic cell types, travel via the blood from the bone marrow to the thymus • The thymus is a specialized environment where immature T cells, known as thymocytes, mature into functional T cells • Thymocytes ultimately generate unique antigen receptors . • T – Cells are selected to mature on the basis of their TCR reactivity to self-peptide/MHC complexes expressed on the surface of thymic epithelial cells. • Thymocytes whose TCRs bind self-MHC/peptide complexes with too-high affinity are induced to die (negative selection) • thymocytes that bind self-MHC/peptides with intermediate affinity undergo positive selection and mature, migrating to the thymic medulla before entering the circulation. • The majority of cells die because they have too-low affinity for the self-peptide/MHC combinations that they encounter on the surface of thymic epithelial cells and fail to undergo positive selection, a process called death by neglect.
  • 7.
  • 8. T-cell development And Thymic Microenvironment • T-cell precursors enter the thymus in blood vessels at the corticomedullary junction between the thymic cortex, the outer portion of the organ, and the thymic medulla, the inner portion of the organ. • Thymocytes first travel to the subcapsular cortex, just beneath the capsule of the thymus, where they proliferate. • They then travel to the cortex, where they first express mature TCRs and interact with cortical thymic epithelial cells (cTECs) • Thymocytes that are positively selected in the cortex continue to mature and travel to the medulla, where they interact with medullary thymic epithelial cells (mTECs). • Negative selection can happen in any of the microenvironments. • Thymocytes are also distinguished by their expression of two CD antigens, CD4 and CD8 • The most immture thymocytes doesn’t express any CD antigens And they termed as Double Negative (DN). • After entering the cortex, thymocytes upregulate both CD4 and CD8 antigens, becoming double positive (DP).
  • 9. • As they mature, they lose one or the other CD antigen, becoming single positive (SP). • CD4 T cells are helper cells and CD8 T cells are cytotoxic (killer) cells. • Mature SP cells exit the thymus as they entered: via the blood vessels of the corticomedullary junction. • Maturation is finalized in the periphery, where these new T cells (recent thymic emigrants) explore antigens presented in secondary lymphoid tissue, including the spleen and lymph nodes.