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(Section
2b. Phases
of Cutaneous Wound Healing continued)
-
Cellular Proliferation Phase
(Begins Day 2)
Cellular proliferation involves three key
processes, angiogenesis, fibroblast,
proliferation
and epithelial cell proliferation
(all require energy, protein synthesis and
anabolism).
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Components:
-
Angiogenesis
- Fibroblast
proliferation
- Epithelial
cell proliferation
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Angiogenesis:
The
wound surface or edge is relatively ischemic
and healing cannot effectively proceed until
sufficient blood flow is restored to allow
delivery of nutrients.
Macrophages secrete a substance known
as angiogenesis factor, which is felt to be a
chemo-attractant for mesothelial and vascular
endothelial cells.
The remarkable process of neo-vascularization
or angiogenesis begins in the first several
days although the process is delayed if a
thick layer of surface necrosis is present.
Endothelial cells proliferate and form
capillary buds at the wound surface.
The buds form a network of loops which
fuse with other buds forming a new capillary
bed. If
the wound edges are approximated, the
capillaries can bridge the wound. |
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Impairment:
Excess Inflammation
- Surface
dead tissue
- Wound
exudates
- Decreased
perfusion
- Corticosteriods
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Fibroblast
Proliferation: The
fibroblast begins to appear in the wound about
2 days after injury.
The initial cells on the scene appear
to migrate from nearby connective tissue.
The stimulus for subsequent fibroblast proliferation as well as subsequent
collagen synthesis appears to be growth factors from platelets and macrophages.
The fibroblasts migrate into the wound
along local fibrin strands from the initial
wound coagulation as well as any remaining
collagen strands.
The fibroblasts, being metabolically
active, depend on the adequacy of local O2 supply and the
adequacy of neo-vascularization for continued
proliferation. |
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Impairment:
- Decreased
perfusion
- Inadequate
nutrients
- Decreased
anabolic activity
- Corticosteriods
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Epithelialization:
The epidermal lining of skin is in a
continual state of proliferation and
desquamation as opposed to the more dormant
mesenchymal tissues.
With loss of the epidermis, adjacent
cells become reprogrammed.
They appear detached from their
basement membrane, divide, and migrate toward
and across the wound, first forming a single
cell layer.
Various epidermal growth factors
released from the macrophage and platelet,
initiate the response.
This process, however, is quite limited
and any dead tissue on the surface will retard
epithelialization.
Also the cell distance traveled is
limited to about 3 cm from the wound edge.
The re-epithelialization process can be
rapid, i.e., 3 to 5 days in a superficial
injury or several months, depending on the
size of the defect, the nutrient supply, the
number of remaining basal cells, and the wound
environment
Once a single layer develops,
additional layers form from mitotic division. |
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Impairment:
- Desiccation
- Destruction
by excessive proteases
- Excess
inflammation
- Impaired
perfusion
- Lack
of adequate nutrients
- Corticosteriods
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| Figure
4: (2-4 days) |
Figure
5: Angiogenesis |
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| New
vessel formation, increased fibroblasts,
epithelial cell migration, macro phages,
O2 in wounds. |
New capillaries wound surface. |
| Figure
6: Fibroblast
Proliferation |
Figure
7: Epithelial
clusters |
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| Numerous fibroblasts now
present. |
White
areas enlarging and
merging close to the wound. |
| Figure
8: Epithelial
Cell Proliferation |
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Epithelial
cells are proliferating and migrating towards
each other close to the partial thickness
wound.
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