| Apoprotein(a) Is
an Adhesive Protein (1991)
Rath M. Journal of Orthomolecular Medicine, 6:139-143.
Summary
In preceding publications we have shown that
apoprotein(a) [apo(a)] has important beneficial physiological
properties that by far outweigh its disadvantages. We have also
identified powerful beneficial properties of apo(a) in the defence
against the proliferation of various diseases.
Here we extend this concept and propose that apo(a)
plays a decisive physiological role as an adhesive protein. Apo(a)
contains an arginine-glycine-aspartate (RGD) tripeptide, a characteristic
sequence in adhesive proteins. Corroborating this role as an adhesive
protein is our discovery of free apo(a) in human sperm. In this
case apo(a) is not associated with apoprotein B (apoB) or low-density
lipoprotein (LDL).
Lp(a) evidently is primarily a feasible transport
form of apo(a) to the site of tissue requirement. Organs that
are largely cut off from the blood circulation such as testes
and brain have retained their autonomous apo(a) production. The
ability of such critical organs as the brain and the testes to
regulate their apo(a) supply independently of the Lp(a) production
in the liver is no coincidence.
It provides further evidence for our concept that
apo(a) plays a powerful role in health and disease. As an adhesive
protein apo(a) is involved in organising the interaction between
cellular systems and the extracellular matrix in tissue formation,
remodulation and repair. Under physiological conditions apo(a)
mediates cell adhesion and migration as well as processes like
differentiation and growth.
On the basis of these physiological properties
the importance of apo(a) increases under pathological conditions.
Here apo(a) compensates in a versatile way for ascorbate deficiency;
as an adhesive protein it particularly mediates the cellular-extracellular
interaction during chronic repair processes. The identification
of apo(a) as an adhesive protein provides new insights into these
processes. Finally, apo(a) may play a critical role in the development
and differentiation of the human body during the evolution of
man.
Full Study
Introduction
Apoprotein(a) [apo(a)] is a unique macromolecule that is synthesised
at a high rate in man and other species that have lost their ability
for endogenous ascorbate production (1). When associated with
low-density lipoprotein (LDL) to form lipoprotein(a) [LP(a)] it
becomes a primary risk factor for cardiovascular disease (CVD)
(2). The conservation of such a potentially detrimental genetic
feature during evolution deserves an explanation. Our discovery
of the ascorbate-apo(a) connection marked a turning point in research
directions. We proposed that apo(a) must have advantageous physiological
properties that by far outweigh its disadvantages.
Subsequently we identified powerful beneficial
properties of apo(a) in the defence against the proliferation
of various diseases. These properties include the stabilisation
of the extracellular matrix, the interaction with the coagulation
system, antioxidative defence, and inhibition of plasmin-induced
proteolysis. Ascorbate deficiency is the metabolic condition where
these defence mechanisms are required. Moreover, we identified
prolonged periods of ascorbate deficiency during evolution as
the life-threatening conditions that lead to the high production
of apo(a) in primates and man. The paramount importance of these
discoveries for human health is discussed in the preceding paper
(3).
Based on the conclusion that the beneficial properties
of apo(a) must be greater than its role in the defence of disease
proliferation, we now propose another, perhaps the most decisive,
function, of apo(a). We propose that apo(a) can function as an
adhesive protein. Moreover, we propose that apo(a) is critically
involved in differentiation, morphogenesis, and possibly fertility
and development of intelligence.
The apo(a) molecule contains
the arginine-glycine-aspartate sequence characteristic of adhesive
proteins
Properties such as organ morphogenesis, differentiation, and growth
have recently been discovered to be associated with a number of
proteins present in the extracellular matrix and the blood, such
as fibronectin, collagen, laminin, vitronectin, osteopontin including
also coagulation factors such as fibrinogen and von Willebrand
factor. These ‘adhesive proteins’ contain a characteristic
amino-acid sequence: arginine-glycine-aspartate (RGD), by means
of which they interact with integrins, a family of cell surface
receptors for adhesive proteins.(4,5)
Consequently we investigated the possibility that
the apo(a) molecule contains such a sequence and can function
as an adhesive protein. Sequence analysis of the apo(a) molecule
revealed an arginine-glycine-aspartate (RGD) tripeptide sequence
in the kringle-35 region. This finding confirms that apo(a) carries
the decisive tripeptide sequence that characterises the family
of adhesive proteins. Via the RGD sequence apo(a) can potentially
interact with monocytes, thrombocytes, and other cells during
pathophysiological defence processes as well as under physiological
conditions. We concluded that the role of apo(a) as an adhesive
protein would be further established if we could prove its production
independently of apoB and the Lp(a) particle.
Detection of apo(a) in human
sperm
When human sperm was analysed in our laboratory, both the seminal
plasma and the cellular fraction were found to contain apo(a).
We could not detect any apo B associated with this apo(a). The
detection of apo(a) in human sperm is the proof that isolated
apo(a) is actually produced and secreted into a body fluid independently
of apoB and lipoprotein particles. Two years ago Richard Lawn
and co-workers screened the organs of rhesus monkeys for their
content of apo(a) mRNA. Beside in the liver, apo(a) mRNA was also
found in the testes and the brain (6). Until now these observations
have remained unexplained. The proposed function of apo(a) as
an adhesive protein offers this explanation. After our discovery
of apo(a) in the sperm it is likely that apo(a) will also be found
in the cerebrospinal fluid. Both organs are largely separated
from the bloodstream by blood-organ barriers. The detection of
an autonomous production of apo(a) I these organs leads to important
conclusions. The role of apo(a) in human metabolism is obviously
so important that virtually no organ can afford to be cut off
from the apo(a) supply. Moreover, those organs that are cut off
from this apo(a) supply via the circulatory Lp(a) have maintained
the ability for autonomous apo(a) production.
Lp(a), the transport form
of the adhesive protein apo(a)
So far much interest in Lp(a) has derived from its association
with lipoprotein metabolism, in particular its close relation
to the LDL particle. On the basis of our recent discoveries and
the role of apo(a) as an adhesive protein we conclude that this
associations rather the means than the end. The Lp(a) lipoprotein
particles secreted from the liver into the plasma are the transport
form of apo(a). Via this backpacking mechanism apo(a) can be carried
to almost all sites of the body under physiological and pathophysiological
conditions. Goldstein and Brown suggested that apo(a) may target
the LDL particle to the sites of wound-healing (7). We, however,
propose in the light of the concept presented here that the apo(a)
molecule rather than the LDL molecule is the more important partner
in this metabolic co-operation. Thus the LDL particle is rather
the means, i.e. a convenient transport vehicle, than the end,
lipid substrate supply for tissue repair. A closer look on the
amount of LDL and Lp(a) and their relation as part of the individual
plasma confirms this concept: apo(a), not LDL, is the limiting
partner. We do not, of course, exclude that the availability of
lipid substrates at the site of tissue growth or repair may be
an additional advantage for the combination of apo(a) with LDL.
The role of the adhesive
protein apo(a) under physiological conditions
Elevated plasma Lp(a) concentrations have been detected in new-borns
as well as during periods of increased growth.8 It is thus conceivable
that the primary role of the adhesive protein apo(a) is during
development and differentiation of the human body and its organs.
Those organs unable to synthesize apo(a) are supplied via Lp(a)
from the circulation. Those organs separated from the circulation
by a blood-organ barrier would depend on their own production.
In this respect the ability of the brain to produce
apo(a) deserves particular attention. It has been shown by in
vitro studies with other adhesive proteins that the RGD tripeptide
is critically involved in the differentiation and morphogenesis
of the central and peripheral nervous system as well as the binding
of oligodendrocytes to various components of the glial-derived
matrix (9). It is therefore conceivable that the adhesive protein
apo(a) is involved in the development and differentiation of the
brain.
Similarly the presence of apo(a) in the seminal
fluid suggests a specific role for apo(a). The RGD sequences have
been shown to be essential for the formation of Sertoli cell cords.
Moreover, during conception the RGD sequence is involved in sperm-oolemmal
adhesion and egg penetration. Both the formation of Sertoli cell
cords and the fertilisation itself have been successfully inhibited
by synthetic peptides containing the RGD sequence.10 The detection
of apo(a) in human sperm suggests a role of apo(a) in fertility
and conception.
The role of the adhesive protein apo(a) under pathological conditions
The importance of apo(a) as an adhesive protein increases under
pathological conditions and ascorbate deficiency. Apo(a) co-ordinates
the interaction between cellular systems and the extracellular
matrix during repair processes. Apo(a) is involved in tissue reformation
during acute repair processes such as wound-healing and Lp(a)
plasma levels are known to be elevated during the post operative
phase.
Chronic repair processes are characteristic for
all pathological states and they are sustained by chronic ascorbate
deficiency. In this situation adhesive proteins play a particular
role. They interact specifically with cellular systems such as
monocytes, T cells as well as thrombocytes and thereby play a
critical role in inflammatory, infectious, hemostatic and many
other processes (4,5).
The adhesive protein apo(a), on the basis of its
physiological properties, may play an important role in disease
containment, tissue reorganisation and chronic repair processes
in general. The elevation of Lp(a) plasma levels as established
for cancer, cardiovascular, inflammatory and many other diseases
is additional confirmation for this concept.
In this context it is noteworthy that apo(a) can
interact with a variety of other adhesive proteins, such as fibrinogen,
collagen, and fibronectin. The interaction of apo(a) with fibronectin
is of particular interest.
Apo(a) and fibronectin
Fibronectin is one of the best-characterised adhesive proteins.
It is present in plasma and other body fluids, with a particularly
high concentration in the seminal fluid. Fibronectin is involved
in cellular migration during embryogenesis, morphogenesis, differentiation,
and growth of many systems. In particular it has been shown to
be involved in development and differentiation of the brain and
the peripheral nervous system. Other functions comprise platelet
aggregation, thrombus formation, and wound healing (5).
Apo(a) and fibronectin share common structural
and functional properties. Both molecules consist of numerous
repeated segments, including kringle structures, and possibly
share common ancestral genes. Both apo(a) and fibronectin can
bind to fibrin and collagen. A particularly well-characterised
region is the cell-binding region of fibronectin, which contains
an RGD sequence and is critically involved in the interaction
of fibronectin with integrins and different cell systems.
It has been reported that apo(a) not only can
bind to fibronectin but also cleaves this molecule. This observation
has been interpreted as an indication for the pathogenic role
of apo(a) (11). An alternative interpretation is presented here:
the coexistence of apo(a) and fibronectin e.g. in plasma, the
seminal fluid, and other body fluids in relatively high concentrations
largely excludes a genuine hostile interaction of these two proteins.
It is rather likely that apo(a) and fibronectin
share several common functions. This conclusion is supported by
the fact that an increase in plasma fibronectin is found almost
immediately at sites of wound healing and cell repair (12). Lp(a),
however, in trauma patients reaches its maximum in plasma only
after one week. Thus a replacement of the short-term adhesive
protein fibronectin by apo(a), a long-term adhesive molecule with
superior functions, is conceivable.
The adhesive protein apo(a) and its possible
role in the evolution of man
The role of adhesive proteins in morphogenesis and organ differentiation
is well established, yet little is known about the potential role
of adhesive proteins in the differentiation of species during
evolution. This in part reflects the fact that the adhesive proteins
discovered so far, including fibronectin, are highly conserved
throughout the animal word. Therefore it is difficult to study
their role in relation to the differentiation between species.
This is not the case for the adhesive protein apo(a). Apo(a) has
become a major constituent of the metabolism mainly in primates
and man.
Thus, apo(a), on the basis of other evolutionary
advantages achieved during primate evolution, may have become
an additional important metabolic element towards the evolution
of man. The production of apo(a) in testes and the brain could
be interpreted as additional evidence. These organs have determined
critical evolutionary advantages: Fertility and intelligence.
Conclusion
We propose that apo(a) is an adhesive protein. We provide several
lines of evidence. The apo(a) molecule contains an RGD tripeptide
sequence, a characteristic peptide sequence of adhesive proteins.
Consequently, apo(a) is proposed to interact with integrin receptor
systems on the surface of thrombocytes, monocytes, and other cells
under physiological and pathophysiological conditions. Corroborating
the role of apo(a) is the detection of apo(a) in human organs
that do not have access to apo(a) supply via the Lp(a) particle
in the circulation is a remarkable fact. It suggests that virtually
all organs of the human body are critically dependent on apo(a)
supply.
With our discovery of the ascorbate-apo(a) connection
it became immediately evident that apo(a) exerts powerful beneficial
properties in health and disease. With the recognition of apo(a)
as an adhesive protein we continue to elucidate these properties.
With confirmatory evidence for the role of apo(a) as an adhesive
protein, the implications of this discovery may be far-reaching.
We propose that apo(a) participates in a comprehensive coordinative
way in the morphogenesis and differentiation of organs as well
as in body growth. Moreover, the preferential production of apo(a)
in primates and man and its autonomous production in those organs
critical for intelligence and reproduction provide yet another
clue: apo(a) may turn out to be an important piece of the metabolic
mosaic towards evolution of man during the remarkably short time
in which he became the dominant species on earth.
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