5. Endothelium is thin layer of cells which lies the interior
surface of blood vessels and lymphatic vessels
Cells which form endothelium are called endothelial cells
(EC’s)
Mesodermal in origin
It forms an interface between circulating blood/lymph in
the lumen and rest of the vessel wall
Most quiescent & genetically stable cells of the body-
turnover time usually 100 days
6. HISTORY
Endothelium- 1st described by Virchow in capillaries
as a simple membrane with flattened nuclei
Swiss Anatomist Wilhelm His- introduced the term
“endothelium”
Waldayer -suggested the term restricting to those
cells that make up the innermost layer of blood
vessels and lymph vessels & posterior lining of cornea
1st pro-angiogenic factor (bFGF)- purified in 1984
from tumor cells by Sching & Klagsbrun
11. Earliest blood vessels develop from Blood islands
(insulae sanguineae) which appear in mesoderm
surrounding the wall of the yolk sac at 3 weeks of
development
12. Centre of blood islands form
Hematopoeitic stem cells
( Precursor of all blood cells)
Peripheral hemangioblasts form
Mesodermal cells
HEMANGIOBLAST
ANGIOBLAST(Precursor
of blood vessels
FGF- 2
VEGF
13. Angioblasts proliferate and eventually induced to form
EC’s (by VEGF, secreted by surrounding mesoderm cells)
Once process of vasculogenesis estalishes a primary
vascular bed, additional vasculature is added by
angiogenesis, the sprouting of new vessels (by VEGF)
Maturation & modeling of the vasculature is regulated
by other GF’s ( PDGF, TGF-b )
17. VEGF
Receptor
KDR ( kinase insert domain
receptor 2)- It is human gene
encoding Flk-1
VEGFR-2
KDR is designated as
CD 309
Flk -1
(fetal liver
kinase 1)
18. Expression of flk-1 represents the earliest marker of
the developing endothelial lineage during
vasculogenesis
SCL (Stem cell leukaemia) transcription factor/
TAL- 1 i.e T-cell acute lymphocytic leukaemia=
crucial for the development of blood cells and blood
vessels
AC 133 / / Prominin - 1= Useful marker for
isolation of hematopoeitic & endothelial progenitor cell
(homeobox gene)- marker for both
hemangioblast and angioblast
present only in endothelial precursors
flk-1
SCL
CD 133
Hex
19.
20.
21. CD133 is absent on mature endothelial cells and monocytic cells
22.
23. Microvasculature (Capillaries & post capillary venules
EC’s Pericytes
• Contractile function
• Multipotential capabilities- differentiate
to adipocytes, osteoblasts, phagocytes,
SMC’s
• Pericytes & SMC’s recruit to form
periendothelial layer- for vessel
maturation & stabilisation
• Imp for BBB formation
/ Mural /Rouget cells
24. STRUCTURE
Epithelial lining of the vascular system
Almost always Simple squamous epithelium
EC’s are very flat and elongate, have central nucleus,
thickness is maximum at the level of nucleus(2-3 µm),
10-20 µm in diameter
Elsewhere-thinner and laminar; in capillaries as thin as
0.2 µm
Elongated in the direction of the blood flow, especially
in arteries
25. Cytoplasm is relatively simple with few organelles;
mostly concentrated in the perinuclear zone
At ultra structural level, they have few characteristic
organelle
e.g.1) transcytotic/ pinocytotic vesicle
2) caveole
3) Weibel-Palade body
26. TRANSCYTOTIC VESICLE :
- in all ECs but particularly present in exchange vessels
- shuttle small amount of extracellular fluid or blood
plasma across the endothelial cytoplasm
-facilitates bulk exchange of dissolved gases, metabolites
and nutrients
-E.g. in the lung capillaries where there is very efficient
movement of gases (carbon dioxide, oxygen and
anaesthetics etc)
.
27. CAVEOLE :
- special type of transcytotic vesicle
- typical in vessels of smooth muscle cells
- vesicular invagination of cell surface
- associated with receptors, enzymes and ion channels
28. WEIBEL-PALADE BODY :
-also known as rod-shaped (micro) tubulated bodies
-characterizes EC’s
- elongated cytoplasmic vesicle(3 x 0.1) µm
single membrane; dense interior,
-stores adhesion molecule,
P- selectin
Von Willebrand factor( vWF )
30. Formed by
Cadherin-
trans membrane gp
Cell to cell
contact & with
cytoskeleton
Cadherin 5/
VE cadherin/
Endothelial
specific cadherin
31. In large arteries &
brain vessels
Composed of-
Occludin,
Claudin 5,
JAM’s( Junctional
adhesion molecules
Present more at
the apical region
of the cell
Function-Seals
neighboring cells
together to prevent
leakage of molecules
between them
32. c/o Connexons-
mainly of 37, 40, 43
(detected in EC’s)
Function-cell to cell
junction allowing
passage of small
water soluble ions &
molecules
33. ENDOTHELIAL HETEROGEINITY
EC’s exhibit different phenotype- both in structure & function
heterogeneity is linked to both intrinsic, i.e., genetic factor, and
extrinsic factors
Structural heterogeneity- obtained following electron microscopy
observations where differences in intercellular junctions led to the
classification of-
# continuous endothelium
# fenestrated endothelium
# discontinuous endothelium
35. Specialized EC’s of post capillary venules
plump cuboidal morphology, have large no. of lymphocytes
within their walls, basal lamina is continuous, 7-30µm
A) High Endothelial Venules (HEV)-
HEVs are found in all secondary lymphoid organs except spleen
HEVs enable lymphocytes to move in and out of the lymph
nodes from the circulatory system
HEV-expresses addressins (specific adhesion molecules)
eg CD34
Mad CAM1
Attaches to
L-selectin on
Lymphocytes
36. BLOOD BRAIN BARRIER:BBB-
It is highly selective permeability barrier that prevent the entry of
lipid insoluble substances to enter brain, SC & peripheral nerve
BBB is formed by capillary EC’s which are connected by tight
junctions & relative lack of transcytotic vesicle
Tightness of barrier depends upon the close apposition of
astrocytes (astrocyte cell projections surround the EC’s of BBB)
Circumventricular organs lack it.
37. LUNG :
respiratory membrane
have a selective phagocytic activity & are able to extract
substances from blood
KIDNEY :
finely fenestrated : functions as a selective filter
Principle barrier(≈33µm)--is the BM, the fused endothelium &
podocyte basal lamina
And allows the passage of water, small molecules & ions; but not
larger & those with -ve charge
42. CLINICAL ASSESSMENT OF ENDOTHELIAL
FUNCTION
by both invasively and non- invasively
involves evaluating measure of endothelial cell behavior
in vivo viz endothelium dependent vasodilatation
done using either pharmacological or mechanical
agonist that stimulates endothelium to release effector
molecules that alter underlying SM cell tone.
43. INVASIVE PROCEDURE :
agonist that stimulate release of endothelial NO is
used e.g. acetyl choline & methacholine (short lived
rapidly acting )
intracoronary infusion is given
Change in coronary diameter is measured
44. NON- INVASIVE PROCEDURE :
Assessed in the forearm circulation
Brachial artery blood flow is occluded with a BP cuff
Then cuff is deflated
change in blood flow and diameter is measured ultrasonographically
depends upon -
-shear stress-dependent changes in endothelial release of NO
following restoration of blood flow &
-the effect of transient adenosine released from ischemic tissue.
45. RESULTS:
Normally the change is approx. 10%
Endothelial dysfunction( ED) is defined by- smaller
change & in extreme cases ,a paradoxical
vasoconstriction effect is also seen.
Occurs due to direct effect of cholinergic agonist on
vascular SMC
ED seen in pat with atherosclerosis & risk factors(HTN,
↑cholesterolemia, DM, smoking etc.)
46.
47. PERMEABILITY BARRIER & TRANSPORT
provide barrier between the blood and rest of the body
tissues
Simple diffusion- O2, CO2
Active transport- Glucose, AA’s, electrolytes
Pinocytosis- small molecules, soluble proteins
Receptor mediated endocytosis (clathrin dependent
process)-
GF’s, Antibodies, LDL, Transferrin, MHC complexes
48. SYNTHESIS OF-
Role in VASOMOTION-
1. Prostacyclin (PGI2)
2. Endothelium derived hyperpolarizing factor( EDHF)
3. Nitric oxide (NO)/ (EDRF)
Vasodilator
factors
1. Endothelin-1
2. Thromboxane (TXA2)
3. Angiotensin II
Vasoconstrictive
factors
NOS 3 subtype present in EC’s
49. Secretes ECM protein-
1. Basal lamina- collagen, laminin, elastin, fibronectin
2. Glycocalyx - Proteoglycans
• Smoothness of endothelial surface- due to glycocalyx
• Negative charge on EC’s – due to GAG’s (mainly heparan
SO4)
(EC’s binds to ECM via Integrin)
Secretion of growth stimulating factors-PDGF, FGF, GM-
CSF
Secretion of growth inhibiting factors- heparin, TGF- β
Secretion of IL-1, IL-6, IL-8
50. PECAM 1 (CD31)-
found on the surface of endothelial cell intercellular junctions,
platelets, monocytes, neutrophils, macrophages,
lymphocytes, megakaryocytes
involved in leukocyte transmigration, angiogenesis
& integrin activation
VCAM-1 (CD106)-
expressed on both large and small blood vessels only after EC’s are
stimulated by cytokines
mediates the adhesion of lymphocytes, monocytes, eosinophil,
and basophils to vascular endothelium
Major BM addressin for hematopoeitic progenitor cells expressing
VLA-4 / integrin α4β4
51. ICAM (CD54)-
is expressed by the vascular endothelium, macrophages,
and lymphocytes.
is a ligand for LFA-1 (integrin) , a receptor found on
leukocytes.
stabilizing cell-cell interactions and facilitating leukocyte
endothelial transmigration
53. Anticoagulants- production of Thrombomodulin (CD141)-
(co-factor for thrombin)
Anti thrombogenic agents- production of prostacyclin,
heparin, t PA, anti thrombin III
Pro thrombogenic agents( released after damage to cells)-
# tissue thromboplastin, vWF, PAI
Clotting
Role in CLOTTING-
55. INFLAMMATION
Leucocyte normally repelled by endothelium(for free
flow of blood )
Inflammatory states - leucocytes are attracted to the
endothelium by leucocyte adhesion molecules( expressed
on EC’s)- leucocyte Margination
They leucocyte pass by diapedesis
Hallmark of inflammation- Increased vascular permeability
→ edema
Vascular leakage occurs due to contraction of EC (M.C.)
56.
57. ENDOTHELIUM AS AN ORGAN
1-2 trillion EC’s, forming an almost 1.5 kgs organ
Uniquely contains Weibel-palade bodies (stores vWF)
Not only a permeability barrier, also multifunctional
paracrine & endocrine organ
Involved in-
immune response,
growth regulation, coagulation
production of extracellular matrix components
modulator of blood flow & blood vessel tone
58. ROLE IN DISEASE
Oxidative Stress leads to Endothelial dysfunction (ED)
ED- 1) decreased NO
2) increased Endothelin ( ET-1 binds to Endothelin A and
B receptors in pulmonary vascular bed- potent vasoconstrictor)
It is also a physiological process
Takes place gradually by age and menopause.
61. Disease of large & medium sized muscular arteries
Characterized by-
1. ED
2. vascular inflammation
3. Atheroma's/atherosclerotic plaque--build up of
cholesterol, lipids, cellular debris, calcium & fibrin within the
intima.intima
62.
63. Angiotensin-converting-enzyme(ACE) is an endothelial
enzyme
Converts angiotensinogen I to angiotensinogen II
A II is a potent vasoconstrictor: important in
pathogenesis of hypertension
Hypertension
64. SMOKING
Nicotine- opens up intercellular junction & allow large
molecules to pass through the wall
Such toxins can potentiate degenerative changes in
the blood vessels & lead to vascular disease
Prolonged( years ) smoking of one pack of cigarettes
daily or more –daily, increase death rate from IHD by
200%
Smoking cessation decreases that risk substantially
65. ENDOTHELIUM & STROKE
Production of EDCF- counteracts the normal dilator
effect of NO
Reduced activity of NO synthase
Presence of Hemoglobin in SAH-
# inhibition of NO- vasospasm
69. TTP & HUS are caused by insult that activates platelets
& deposited as thrombi in microcirculation
Superimposition of endothelial injury may further
promote platelet micro aggregate formation : initiate
or exacerbate
Thrombotic microangiopathies
73. In disease , EC growth supports metabolic requirement
of tumor beyond few mm : growth of primary &
metastatic tumor
Several steps=
-stimulation of EC
-degradation of ECM
-proliferation of EC & migration into tumor
-Formation of new capillary tubes
Tumor vessels are=
-tortuous
-dilated, uneven diameter
-excessive branching &shunting
-lack perivascular cells
74. ANTIANGIOGENIC THERAPY
Acquired drug résistance of tumor – due to high intrinsic
mutation rate -- major cause of treatment failure
But ECs are genetically stable ; ECs apoptosis pathway
is intact
EC provides nourishment to many tumor cells; tumor
growth dependent on angiogenesis
blockade of a single GF (e.g. VEGF) may inhibit tumor
induced vascular growth
75.
76. von Willebrand disease
vWF required for interaction & adhesion of platelets to
ECM
Genetic absence of this factor( AD, rare AR)→von
Willebrand disease
77. The WHO classification of vascular tumors
A)Benign=
1) Hemangiomas
-sub cut/deep
-capillary
-cavernous
-arteriovenous
-Venous
-intramuscular
-synovial
2) Epitheloid Hemangiomas
3) Angiomatosis
4) Lymphangioma
TUMOR OF ENDOTHELIAL CELLS
78. B) Intermediate (locally aggressive)
-Kaposiform hemangioendothelioma
C) Intermediate (rarely metastasizing)
-retiform hemangioendothelioma
-papillary intralymphatic angioendothelioma
-composite hemangioendothelioma
-kaposi sarcoma
D) Malignant
-Epitheloid hemangioendothelioma
-Angiosarcoma of soft tissue
79. EC’s play a vital role in health and integrity of every
tissue of the body because
apart from cartilage, every cell lies within a few µm
of a capillary
The diffusion limit of oxygen in tissue is only ≈
100µm,and can not cross blood vessel thicker than that
fine capillaries ( 10-15 µm ) & consist merely of
endothelial cells and a very fine basal lamina, thus helps
in providing oxygen, nutrients & metabolites.
Summary
80. adjust their number & arrangement to accommodate
local requirement
Thus, they are life-support tissue extending & remodeling
the network of blood vessels to enable tissue growth,
motion & repair.
Dysfunction of EC has been implicated in virtually
every type vascular disease( Atherosclerosis,HTN etc.)
and hence integrity & proper function of EC is
essential for proper organ function and good health.
81. Pathological basis of disease : Robbins & Cotran,8th e
Harrison’s internal medicine: 17th e
WHO classification: tumors of soft tissue and bone
Hematology : Basic Principles & Practise,5th e( Hoffman)
Hemostasis and Thrombosis –Basic Principles & Practice, 5th e(
Colman , Goldhaber )
Internet sites
References
An epithelium is any type of tissue ----line the surface or cavity of any structure in the body.
Epithelium is one of the four primary tissue types in the human body, the others being connective tissue, nervous tissue, and muscle tissue.
T. Media thicker in arteries and thinner in veins
Blood islands arise from mesodermal cells( induced by FGF-2 )-to form hemangioblasts, a common precursor for vessel and blood cells formation
Fenestrated capillaries hav diaphragm dat cover the pores
But discontinuous capillaries donot have the diaphragm & js hav an open pore
MadCAM1 (mucosal addressin cellular adhesion molecules 1)- on endothelium of mesentric l. node & peyers patches
functions
NOS 1- brain/SC/neuronal cells/platelets…..constitutive
NOS 2-nucleated cells, Ca independent,,inducible by inflammation
PECAM 1-platelet endothelial cell adhesion molecule-found in vascular tumors
VCAM 1- vascular cell adhesion molecule- express in Atherosclerosis, RA, Melanoma
VLA-4 ( very late antigen 4/ integrin α4β4
ICAM-1( Intercellualr adhesion molecule 1)- increased in subarachnoid hemorrhage (SAH), causes vasospasm,
expressed by respiratory epithelial cells is also the binding site for rhinovirus
PAI- plasminogen activator inhibitor
Rho A/ Rho A kinase-present on EC’s and corpus cavernosa of SMC……smooth muscle contract
