Progeria (pronunciation: /proʊˈdʒɪəriə/) (Hutchinson–Gilford
progeria syndrome, HGPS, progeria syndrome) is an extremely
rare genetic disorder
wherein symptoms resembling aspects of aging are manifested at a very early age.
Progeria is one of several progeroid syndromes.
The word progeria comes from the Greek words "pro" (πρό), meaning "before" or
"premature", and "gēras" (γῆρας),
meaning "old age". The disorder has a very low incidence rate,
occurring in an estimated 1 per 8 million live births. Those born with
progeria typically live to their mid teens to early twenties. It is a genetic
condition that occurs as a new mutation, and is rarely
inherited, as patients usually do not live to reproduce. Although the term
progeria applies strictly speaking to all diseases characterized by premature
aging symptoms, and is often used as such, it is often applied specifically in
reference to Hutchinson–Gilford progeria syndrome (HGPS).
Scientists are particularly
interested in progeria because it might reveal clues about the normal process
of aging Progeria was first described in 1886 by Jonathan Hutchinson.
It was also described independently in 1897 by Hastings Gilford. The condition was later named
Hutchinson–Gilford progeria syndrome.
pictures of kids with progeria.
Signs
and symptoms
Children with progeria usually
develop the first symptoms during their first few months of life. The earliest
symptoms may include a failure to thrive
and a localized scleroderma-like skin
condition. As a child ages past
infancy, additional conditions become apparent usually around 18–24 months. Limited growth, full-body alopecia, and a distinctive appearance (a small face with a shallow recessed jaw, and a pinched nose) are all characteristics of progeria. Signs and symptoms of this progressive disease tend to become more marked as the child ages. Later, the condition causes wrinkled skin, atherosclerosis, kidney failure, loss of eyesight, and cardiovascular problems. Scleroderma, a hardening and tightening of the skin on trunk and extremities of the body, is prevalent. People diagnosed with this disorder usually have small, fragile bodies, like those of elderly people. The face is usually wrinkled, with a larger head in relation to the body, a narrow face and a beak nose. Prominent scalp veins are noticeable (made more obvious by alopecia), as well as prominent eyes. Musculoskeletal degeneration causes loss of body fat and muscle, stiff joints, hip dislocations, and other symptoms generally absent in the non-elderly population. Individuals usually retain normal mental and motor development.
infancy, additional conditions become apparent usually around 18–24 months. Limited growth, full-body alopecia, and a distinctive appearance (a small face with a shallow recessed jaw, and a pinched nose) are all characteristics of progeria. Signs and symptoms of this progressive disease tend to become more marked as the child ages. Later, the condition causes wrinkled skin, atherosclerosis, kidney failure, loss of eyesight, and cardiovascular problems. Scleroderma, a hardening and tightening of the skin on trunk and extremities of the body, is prevalent. People diagnosed with this disorder usually have small, fragile bodies, like those of elderly people. The face is usually wrinkled, with a larger head in relation to the body, a narrow face and a beak nose. Prominent scalp veins are noticeable (made more obvious by alopecia), as well as prominent eyes. Musculoskeletal degeneration causes loss of body fat and muscle, stiff joints, hip dislocations, and other symptoms generally absent in the non-elderly population. Individuals usually retain normal mental and motor development.
Cause
Steps in normal cell
|
Steps in cell with progeria
|
The
gene LMNA encodes a protein called prelamin A.
|
The
gene LMNA encodes a protein called prelamin A.
|
Prelamin A has a farnesyl group attached to its end.
|
Prelamin A has a farnesyl group attached to its end.
|
Farnesyl
group is removed from prelamin A.
|
Farnesyl
group remains attached to prelamin A.
|
Normal
form is called lamin A.
|
Abnormal
form of prelamin A is called progerin.
|
Lamin
A is not anchored to the nuclear rim.
|
Progerin
is anchored to the nuclear rim.
|
Normal
state of the nucleus.
|
Abnormally
shaped nucleus.
|
In normal conditions, the LMNA
gene codes for a structural protein called prelamin A. There is a farnesyl
functional group attached to the carboxyl-terminus of its structure. The
farnesyl group allows prelamin A to attach temporarily to the nuclear rim. Once
the protein is attached, the farnesyl group is removed. Failure to remove this
farnesyl group permanently affixes the protein to the nuclear rim. Without its
farnesyl group, prelamin A is referred to as lamin A. Lamin A, along with lamin B and lamin C,
makes up the nuclear lamina,
which provides structural support to the nucleus.
Before the late 20th century,
research on progeria yielded very little information about the syndrome. In
2003, the cause of progeria was discovered to be a point mutation in position 1824 of the LMNA
gene, in which cytosine is replaced with thymine. This mutation causes transcription
of the LMNA gene to stop too early, which results in the creation of an
abnormally short mRNA transcript. This mRNA strand, when translated,
yields an abnormal variant of the prelamin A protein whose farnesyl group
cannot be removed. Because its farnesyl group cannot be removed, this abnormal
protein, referred to as progerin, is permanently
affixed to the nuclear rim, and therefore does not become part of the nuclear
lamina. Without lamin A, the nuclear lamina is unable to provide the nuclear envelope with adequate structural
support, causing it to take on an abnormal shape. Since the support that the
nuclear lamina normally provides is necessary for the organizing of chromatin during mitosis, weakening of the nuclear lamina limits
the ability of the cell to divide. Progerin may also play a role in normal
human aging, since its production is activated in senescent wildtype cells. Unlike
"accelerated
aging diseases" (such as Werner syndrome, Cockayne syndrome or xeroderma pigmentosum),
progeria is not caused by defective DNA repair. Because these diseases cause changes
in different aspects of aging, but never in every aspect, they are often called
"segmental progerias.
Diagnosis
Diagnosis is suspected according to
signs and symptoms, such as skin changes, abnormal growth, and loss of hair. A
genetic test for LMNA mutations can confirm the diagnosis of progeria.
Treatment
No treatment has proven effective.
Most treatment focuses on reducing complications (such as cardiovascular
disease) with coronary artery
bypass surgery or low-dose aspirin. Children may also benefit from a
high-energy diet.
Growth hormone
treatment has been attempted. The use of Morpholinos has also been attempted in order to
reduce progerin production. Antisense Morpholino oligonucleotides specifically
directed against the mutated exon 11–exon 12 junction in the mutated pre-mRNAs
were used.[20]
Potential therapeutic targets for
the inhibition of progerin farnesylation
A type of anticancer drug, the farnesyltransferase
inhibitors (FTIs), has been proposed, but their use has been mostly
limited to animal models. A Phase
II clinical trial using the FTI lonafarnib began in May 2007. In studies on the cells another anti-cancer
drug, rapamycin, caused removal of progerin from the nuclear membrane through autophagy. It has been proved that pravastatin and zoledronate are effective drugs when it comes to
the blocking of farnesyl group production. However, it is important to remember
that no treatment is able to cure progeria.
Farnesyltransferase inhibitors
(FTIs) are drugs that inhibit the activity of an enzyme needed in order to make
a link between progerin proteins and farnesyl groups. This link generates the
permanent attachment of the progerin to the nuclear rim. In progeria, cellular
damage can be appreciated because that attachment takes place and the nucleus
is not in a normal state. Lonafarnib is an FTI, which means it can avoid this
link, so progerin can not remain attached to the nucleus rim and it now has a
more normal state.
The delivery of lonafarnib is not
approved by the US Food and Drug
Administration (FDA). Therefore, it can only be used in certain
clinical trials. Until the treatment of FTIs is implemented in progeria
children we will not know its effects—which are positive in mice. Pravastatin, traded as Pravachol or Selektine, is
included in the family of statins. As well as zoledronate (also known as Zometa and Reclast,
which is a bisphosphonate), its utility in HGPS is the prevention of farnesyl
groups formation, which progerin needs to provoke the disease. Some animal
trials have been realized using FTIs or a combination of pravastatin and zoledronate so as to observe whether they are
capable of reversing abnormal nuclei.
The results, obtained by blinded
electron microscopic analysis and immunofluorescence microscopy, showed that
nucleus abnormalities could be reversed in transgenic mice expressing progerin.
The reversion was also observed in vivo—cultured cells from human subjects with
progeria—due to the action of the pharmacs, which block protein prenylation
(transfer of a farnesyl polypeptide to C-terminal cysteine). The authors of
that trial add, when it comes to the results, that: “They further suggest that
skin biopsy may be useful to determine if protein farnesylation inhibitors are
exerting effects in subjects with HGPS in clinical trials”. Unlike FTIs, pravastatin and zoledronate were approved by the U.S. FDA (in
2006 and 2001 respectively), although they are not sold as a treatment for
progeria. Pravastatin is used to decrease cholesterol
levels and zoledronate to prevent hypercalcaemia.
Rapamycin, also known as Sirolimus, is a macrolide. There are recent studies concerning
rapamycin which conclude that it can minimize the phenotypic effects of
progeria fibroblasts. Other observed consequences of its use are: abolishment
of nuclear blebbing, degradation of progerin in affected cells and reduction of
insoluble progerin aggregates formation. All these results do not come from any
clinical trial, although it is believed that the treatment might benefit HGPS
kids. A 2012 clinical trial found that the cancer drug Lonafarnib can improve weight gain and other
symptoms of progeria.
Prognosis
As there is no known cure, few
people with progeria exceed 13 years of age. At least 90% of patients die from
complications of atherosclerosis, such
as heart attack or stroke. Mental development is not adversely affected; in
fact, intelligence tends to be normal to above average. With respect to the
features of aging that progeria appears to manifest, the development of
symptoms is comparable to aging at a rate eight to ten times faster than
normal. With respect to features of aging that progeria does not exhibit,
patients show no neurodegeneration
or cancer predisposition. They also do not develop
the so-called "wear and tear" conditions commonly associated with
aging, such as cataracts (caused by UV
exposure) and osteoarthritis (caused
by mechanical wear). Although there may not be any successful treatments for
progeria itself, there are treatments for the problems it causes, such as
arthritic, respiratory, and cardiovascular problems.
Epidemiology
A study from the Netherlands has
shown an incidence of 1 in 4 million births. Currently, there are 100
known cases in the world. Approximately 140 cases have been reported in medical
history. However, the Progeria Research
Foundation believes there may be as many as 150 undiagnosed cases
worldwide.
Classical Hutchinson–Gilford
progeria syndrome is usually caused by a sporadic mutation taking place during
the early stages of embryo development. It is almost never passed on from
affected parent to child, as affected children rarely live long enough to have
children themselves.
There have been only two cases in
which a healthy person was known to carry the LMNA mutation that causes
progeria. These carriers were identified because they passed it on to their
children. One family from India has five children with progeria, though not the
classical HGPS type. This family was the subject of a 2005 Bodyshock documentary entitled The
80 Year Old Children. The Vandeweert family of Belgium has two
children, Michiel and Amber, with classic HGPS.
The first reported case of a black
child with progeria was identified in September 2011. The South African child,
named Ontlametse
Phalatse, was born in 1999. The Progeria Research
Foundation at Children's Hospital
Boston, affiliated with the Harvard
University Medical School, is treating her and monitoring her case.It is also discovered that kids with progeria dont live past the age 12.Although if discovered early and the body responds to treatment the kids life span will increase.
Research
Several discoveries have been made
that have led to greater understandings and perhaps eventual treatment for this
disease. A 2003 report in Nature said that progeria may be a de novo dominant trait. It develops during cell division in a newly conceived zygote or in
the gametes of one of the parents. It is caused by mutations in the LMNA (lamin A protein) gene
on chromosome 1; the mutated form of lamin A is
commonly known as progerin. One of the
authors, Leslie Gordon, was a physician who did not know anything about
progeria until her own son, Sam, was diagnosed at 21 months. Gordon and her
husband, pediatrician Scott Berns, founded the Progeria Research
Foundation.
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