Repair Dr Heyam Awad FRCPath. Tissue repair Restoration of tissue architecture and function after injury. Two types : 1) regeneration. 2) scar formation.

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Presentation transcript:

Repair Dr Heyam Awad FRCPath

Tissue repair Restoration of tissue architecture and function after injury. Two types : 1) regeneration. 2) scar formation.

Regeneration Replacement of damaged cells and restoration of normal function. Happens by proliferation of residual, uninjured cells that can replicate and by tissue replacement from stem cells.

Scar formation = repair by fibrous tissue, resulting in a scar. Happens if the injured tissue unable to replicate or the supportive structures of the tissue are severely injured. The scar cannot perform the lost function but it gives structural support.

In many situation … both, regeneration and scar formation contribute to repair.

Cell and tissue regeneration Cells that replicate during repair: 1. Remnant of injured tissue. 2. Endothelial cells. 3. Fibroblasts. The proliferation of all these cells is controlled by growth factors.

Normal size of cell population is controlled by a balance between: Cell proliferation Cell death by apoptosis Formation of new differentiated cells from stem cells.

Cell cycle

Non dividing cells are arrested in G1 phase or exited the cell cycle at G0 phase. Growth factors.. Stimulate transition from G0 to G1 and beyond into S phase, G2 and M phase. This progression is regulated by cyclins that are regulated by cyclin dependent kinases.

Proliferation capacities of tissues Labile cells Stable cells Permeant cells

Labile tissue Labile tissue= continuously dividing tissue. continously lost and replaced by proliferation of mature cells and by maturation from stem cells. Examples: Hematopietic cells, skin and surface epithelium

Stable tissue Quiescent, inactive cells Minimal replicative activity in the normal state. Can proliferate in response to injury Examples: Parenchyma of solid organs, Endothelial cells, Fibroblasts, Smooth muscle cells. Stable tissue,except the liver, has limited capacity to regenerate.

Permanent tissue Permanent tissue: terminally differentiated and non proliferative. Neurons and cardiac muscle Limited stem cell replication and differentiation occur in some areas of the adult brain Cardiac stem cells may proliferate. Skeletal muscle usually classified as permanent but stellate cells provide some regeneration.

Stem cells Self renewal capacity Asymmetric replication

Stem cells 1. embryonic stem cells. 2. adult stem cells.

Embryonic stem cells Undifferentiated. Extensive cell renewal capacity. Can differentiate to the three germ cell layers.

Adult stem cells Less undifferentiated. Their lineage potential restricted to the differentiated cells in the organ they are found in. Important in maintaining tissue size and in repair.

Tissue (adult) stem cell use in medicine Restricted by: 1. Difficulty in isolating them to purity 2. They are present in stem cell niches… without which they cannot function properly.

Stem cell niches microenvironment, within the specific anatomic location where stem cells are found, which interacts with stem cells to regulate cell fate.

Stem cell niches

Tissue stem cells uses Treatment of certain diseases…. Leukaemia and lymphoma….. By hematopoietic stem cells. Regenerative medicine… to regenerate damaged tissues……… difficult because of the problems mentioned previously !

Embryonic stem cells uses Regenerative medicine.. Problem: immunologic rejection. Solution: tried to generate stem cells from patients’ own cells = iPS.

iPS = induced pleuripotent stem cells. How? By identifying certain genes needed for stem-cell-ness These genes are introduced in differentiated cells… this causes reprogramming of somatic cell nucleus.. It acquires properties of embryonic stem cells. Clinical usefulness???

iPS

Growth factors Proteins that stimulate cell survival and proliferation. They can also promote migration, differentiation and other cellular responses. derived from macrophages, endothelial cells, mesenchymal and many other cells.

GFs EPIDERMAL GROWTH FACTOR TGF ALPHA TGF BETA HEPATOCYTE GF PDGF KERATINOCYTE GF VEGF

GF GF stimulate cell growth by: 1. promote entry to cell cycle. 2.releive blocks on cell cycle progression. 3.Prevent apoptosis. 4. increase protein synthesis

Signalling mechanisms of GFs GFs function through receptors…. And trigger biochemical signals … which stimulate or repress gene expression

GF signalling Can be Autocrine.. On the same cell that produced the factor Paracrine… between adjacent cells Endocrine.. Through blood.

GF receptors Receptors with intrinsic kinase activity. G protein coupled receptors Receptors without intrinsic enzymatic activity.

Receptors with intrinsic kinase activity Ligand binds to receptor… dimerization and phosphorylation of the receptor subunits…. Phosphorylated receptor… bind and activate intracellular proteins ….cell proliferation.

G coupled proteins Seven transmembrane alpha helices, coupled with G protein (GTP binding protein). Ligand binding: GDP in the G protein changes to GTP… receptor activated. Signal transduction through second messengers including cAMP.

G protein- coupled receptors

Receptors without intrinsic enzymatic activity Ligand.. Conformational change of receptor intracellular domain…. So it can bind to intracytoplasmic kinase (Janus kinases = JAKs). Now receptor activated… stimulation of STATs (signal transducers and activators of transcription)…. goes to nucleus… induces transcription