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Document Description
Title
Calcitonin
modulates
skeletal
mineral
loss
during
lactation
through
interactions
in
mammary
tissue
and
directly
through
osteoclasts
in
bone
Author
Woodrow
,
Janine
P.
Description
Thesis
(Ph.D.)--Memorial
University
of
Newfoundland
,
2009.
Medicine
Date
2009
Pagination
xviii, 227 leaves : ill. (chiefly col.)
Subject
Bone
densitometry;
Calcitonin--Physiological
effect;
Lactation--Nutritional
aspects;
Mice--Reproduction;
Minerals
in the
body;
Bone
Density--physiology;
Calcitonin;
Lactation--physiology;
Mice;
Degree
Ph.D.
Degree Grantor
Memorial University of Newfoundland. Faculty of Medicine
Discipline
Medicine
Language
Eng
Notes
Includes
bibliographical
references
(leaves
189-210)
Abstract
The
physiological
role
of
calcitonin
in
mammals
has been in
question
since
it
discovery.
Many
have
speculated
that the
calcitonin/calcitonin
gene-related
peptide
(ctcgrp)
gene
has
endured
simply
because
of its
alternate
mRNA
pathway
to
produce
calcitonin
gene-related
peptide-cx
(CGRP-cx)
in
neural
tissue.
Nevertheless
, a
few
studies
have
persisted
in
suggesting
that
mammalian
calcitonin
is
vital
in
times
of
increased
calcium
demand
,
such
as
during
lactation.
Unfortunately
, these
surgical
based
studies
were
fraught
with
experimental
problems
stemming
from
lack
of
true
absence
of
calcitonin
and
confounding
effects
of
thyroid
ablation.
This
doctoral
work
,
therefore
, was
carried
out
to
test
the
theses
that:
calcitonin
is
required
physiologically
during
lactation
to
protect
the
maternal
skeleton
against
excessive
resorption
of
mineral
and that
lactational
bone
losses
in the
absence
of
calcitonin
involve
a
complex
physiological
circuitry
between
the
breast
,
bone
and
brain.
Studies
were
carried
out
using
the
murine
ctcgrp
null
mouse
model
,
which
is
completely
void
of
calcitonin
from
conception
onwards.
Ctcgrp
nulls
were
compared
to the
normal
,
wild-type
(WT)
siblings
as
controls.
--
We
have
demonstrated
that
although
calcitonin
is
unnecessary
during
pregnancy
and the
post-weaning
period
,
it
is
indeed
required
physiologically
during
lactation
since
in its
absence
over
half
(51.
6%
±
4.6%)
of the
vertebral
bone
mineral
content
(BMC)
is
lost
versus
that
seen
in the
WT
(24.4%
±
5.4%).
BMC
losses
were also
significant
within
the
hindlimb
region
and at the
total
body
level.
Loss
of
calcitonin
during
lactation
is
associated
with
increased
trabecular
thinning
and
separation.
Despite
these
significant
architectural
changes
,
however
,
bone
strength
is
no
different
in the
ctcgrp
null
versus
WT
,
likely
due
to a
higher
baseline
bone
volume
in the
ctcgrp
null.
--
Mechanisms
underlying
significant
BMC
losses
in the
ctcgrp
null
versus
the
WT
include
increased
mammary
production
of
PTHrP
,
increased
circulating
PTH
and
increased
bone
resorption.
Pituitary
contributions
to
bone
loss
appear
to be
less
significant.
Excess
calcium
lost
during
lactation
does
not
occur
as a
result
of
compromised
intestinal
absorption
or
increased
urinary
excretion
but
is
most
likely
lost
in the
milk
supply.
--
Our
studies
therefore
confirm
an
important
physiological
role
of
calcitonin
in
protecting
the
maternal
skeleton
against
excessive
resorption
during
lactation.
Important
physiological
pathways
regulating
bone
resorption
at this
time
include
the
breast
and
bone
, with
potential
contributions
coming
from the
brain.
Furthermore
, the
post-weaning
ctcgrp
null
skeleton
may
offer
an
ideal
context
in
which
skeletal
recovery
could
be
examined
because
anabolic
mechanisms
are
likely
upregulated.
Type
Text
Resource Type
Electronic
thesis
or
dissertation
Format
Image/jpeg;
Application/pdf
Source
Paper copy kept in the Centre for Newfoundland Studies, Memorial University Libraries
Local Identifier
a3241924
Rights
The author retains copyright ownership and moral rights in this thesis. Neither the thesis nor substantial extracts from it may be printed or otherwise reproduced without the author's permission.
Collection
Electronic
Theses
and
Dissertations
Scanning Status
Completed
PDF File
(28.49
MB)
--
http://collections.mun.ca/PDFs/theses/Woodrow_JanineP.pdf
CONTENTdm file name
34180.cpd