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THE LIVER STRUCTURE AND FUNCTION

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1) The liver is both an exocrine gland, secreting bile, but also and endocrine ... An actin 'corset' prevents expansion of the canaliculi forcing the bile to flow ... – PowerPoint PPT presentation

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Title: THE LIVER STRUCTURE AND FUNCTION


1
THE LIVERSTRUCTURE AND FUNCTION
  • Richard Hinton,
  • School of Biological Sciences
  • University of Surrey

2
Functions of the Liver
  • 1) The liver is both an exocrine gland,
    secreting bile, but also and endocrine organ
    making plasma proteins
  • 2) The liver degrades worn out plasma proteins
    and red blood cells prepares hydrophobic
    materials for excretion
  • 3) The liver plays a major protective role
    preparing lipid soluble xenobiotics for
    excretion, removing particulates such as bacteria
    and viruses and synthesising protective proteins
    in theacute phase response
  • 4) The liver is the principal site for
    interconversion of fats, sugars and amino acids
    and is mainly responsible for the synthesis of,
    for example, haem and cholesterol. The liver
    also synthesises blood lipoproteins and stores
    glycogen

3
Gross anatomy of the liver
  • The liver has a dual blood supply. Only 20 of
    the blood derives from the hepatic artery, the
    remainder comes from the portal veins which drain
    the stomach and all the intestines except the
    rectum. The liver hence can remove damaging
    materials before they reach the systemic
    circulation
  • Blood leaves the liver via the hepatic veins
    which join with the ascending vena cava

4
Continued
  • The exocrine secretion of the liver, bile, is
    carried from the liver to the intestine by the
    bile duct. In most species, but not in rats or
    horses, a small sac, the gall bladder, buds off
    the upper part of the bile duct and stores and
    concentrates bile between meals. In some
    species, such as rats, pancreatic ducts fuse with
    the bile duct, in others such as humans they
    remain separate until they reach the intestine
  • Some lymph is formed in the portal tree and this
    leaves by a lymphatic. No lymph is formed in the
    parenchyma as the fenestrated endothelium means
    that proteins can pass freely from the lumen of
    the vessel to the space of Disse

5
The Internal Anatomy of the Liver
  • The portal vein, hepatic artery, bile duct and
    lymphatics enter the liver at a single point, the
    porta hepatis. Once inside the liver these
    vessels run in a connective tissue matrix and the
    assemblage is called the portal tract. This
    branches to form the portal tree. Each branch
    of the tree contains all four types of vessel

6
Continued
  • The hepatic veins also branch in a tree like
    pattern which interdigitates with the portal tree

7
Intrahepatic bile ducts
  • The bile ducts are surrounded by a network of
    small blood vessels, supplied from the hepatic
    artery. The direction of blood flow is opposite
    to that of bile so recovering low molecular
    weight materials which heve entered the bile by
    mistake

8
Structure of the hepatic parenchyma
  • ..
  • The parenchyma is the functional part of the
    gland as opposed to the supporting connective
    tissue which is termed the stroma..
  • Blood from the terminal hepatic arterioles and
    portal venules is discharged into the capillaries
    of the liver

9
Why liver capillaries are called sinusoids
  • These vessels are unusual in that their lining
    cells contain sieve plates which allow proteins
    to pass through into the Space of Disse and there
    contact the underlying hepatocytes. Because of
    this they are termed sinusoids

10
Bile Formation
  • Bile consists principally of bile acids and bile
    salts. These are detergents which assist in
    digesting fat and show entero-hepatic
    recirculation
  • Glucuronide and glutathione conjugates are also
    excreted in bile. Bile also contains lipids and
    distinctive enzymes extracted from hepatocytes
  • Bile is initially formed by transfer of bile
    acids and salts into small spaces between
    hepatocytes termed bile canaliculi. These are
    sealed by tight junctions, however these allow
    the passage of water to hydrate the secretion
  • An actin corset prevents expansion of the
    canaliculi forcing the bile to flow towards the
    portal tracts

11
Structure of hepatocytes
  • Hepatocytes are epithelial cells but, in the
    liver, there is no well defined basement membrane
    although collagen fibres are seen in the space of
    Disse and can increase in liver damage
  • Hepatocytes are large cells with central nuclei.
    Cells may be bi-nucleate or polyploid - this
    varies with species. The microtubule organising
    centre, and hence the golgi apparatus lie between
    the nucleus and the bile canaliculus. Lysosomes
    remain close to the golgi apparatus. Mitochondria
    and peroxisomes are scattered through the
    cytoplasm.

12
Continued
  • Hepatocytes contain a lot of rough endoplasmic
    reticulum which may form small stacks or be
    looped around mitochondria
  • Smooth endoplasmic reticulum is in the form of
    small tubules and may be difficult to distinguish
    in the normal cell. It tends to localise, along
    with glycogen granules in the central part of the
    cell.
  • There is a well developed cytoskeleton with
    microtubules transporting material between the
    sinusoidal surface of the cell and the peri-golgi
    zone
  • Both the sinusoidal and bile canalicular faces of
    the cell have stubby microvilli

13
Circulatory Zones in the Liver
  • As blood flows from the portal tract to the
    hepatic venules it gradually loses oxygen.
    Although the hepatocytes in the well oxygenated
    periportal zone look similar to hepatocyes
    around hepatic veins (the centrilobular zone)
    their enzymology is different. Cells in the
    intermediate (midzonal) area are - intermediate
  • Synthesis of blood proteins and gluconeogenesis
    occur principally in the periportal zone

Most isoforms of cytochrome P450 concentrate in
the centrilobular zone. Cells in this area are
also especially rich in peroxysomes
14
The differences between the circulatory zones are
difficult to spot in control livers but show up
clearly in damaged livers
15
Kuppfer cells
  • We have already mentioned the sinusoid
    endothelial cell and its sieve plates. Like
    other endothelial cells it appears to be involved
    in message passing.
  • Kupffer cells are fixed macrophages which live
    within the sinusoids and throw processes across
    the vessel. Their job is to remove particulate
    materials picked up in the intestine and worn out
    red blood cells. They are also very heavily
    involved in message passing

16
The cells with every name
  • Fat storing cells (also known as Ito or stellate
    cells) store retinoic acid and are also heavily
    involved in message passing. They are modified
    fibroblasts and, in the damaged liver, revert to
    type
  • The very scarce pit cells are probably resident
    NK cells

17
Control of the Liver
  • The size of the liver is very carefully
    controlled and is regulated by the weight of the
    animal. Cells may be added by mitosis or removed
    by apoptosis. Normally turnover is slow (several
    months in rats)
  • As the centre of intermediary metabolism the
    liver has receptors for a very large number of
    hormones including peptide hormones such as
    insulin and glucogon and nuclear-acting hormones
    such as steroids
  • The liver is only lightly innervated and such
    innervation as there is does not seem to play a
    significant role - as witnessed by the normal
    function of the liver transplant

18
Cross talk between liver cells
  • All the major cell types of liver are capable of
    secreting cytokines which act on other liver
    cells. These are known to affect both the
    addition of cells by mitosis and the removal of
    cells by apoptosis.
  • Mitosis of hepatocytes may be stimulated by TGF?,
    which is an autocrine factor made in hepatocytes
    and acting on hepatocytes and by HGF which is
    formed by fat storing cells.
  • Once the liver cell number has reached the target
    size then division is halted by negative growth
    factors such as TGF?.

19
Continued
  • Transformation of fat storing cells into more
    typical fibrocytes appears to be due to the
    effect of factors released from Kupffer cells.
  • It now seems that apoptosis in the liver is due
    to the interaction of a range of factors.
    Sporadic apoptosis is observed throughout life,
    the factors triggering this are unknown.
    Apoptosis is observed following treatment with a
    range of toxins and may be prevented by factors
    which cause loss of Kupffer cell function .
    However there seem to be other cases where
    Kupffer cells are not involved.

20
Development of the Liver
  • The liver develops from a pair of buds from the
    primitive gut. The liver develops rapidly for it
    several functions vital to the developing. In
    particular it makes blood proteins and is
    colonised by haematopoietic cells. In rats and
    mice the latter role continues for the first 3
    weeks of life.
  • It would seem that hepatocytes, bile duct lining
    cells and the epithelial cells of the endocrine
    and exocrine pancreas have a common origin, their
    development being determined by their environment.

21
Repair of the liver
  • The liver has an immense capacity for
    regeneration. Repair is normally by division of
    hepatocytes drawn from all parts of the liver.
  • If, for some reason, hepatocytes cannot divide
    (eg in galactosamine toxicity) small cells,
    thought to derive from a population on the edge
    of the portal tract divide and differentiate into
    hepatocytes. These oval cells are stem cells
    capable of differentiating into both liver and
    pancreas
  • Repeated damage to the liver or haemorrhagic
    necrosis then the liver may repair by fibrosis
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