| Werner syndrome (adult progeria) | |
|---|---|
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| Werner syndrome has an autosomal recessive pattern of inheritance. | |
| Specialty | Endocrinology  |
Werner syndrome (WS), also known as "adult progeria", is a rare, autosomal recessive disorder which is characterized by the appearance of premature aging.
Werner syndrome is named after the German scientist Otto Werner. He identified the syndrome in four siblings observed with premature aging, which he explored as the subject of his dissertation of 1904.
It has a global incidence rate of less than 1 in 100,000 live births (although incidence in Japan and Sardinia is higher, affecting 1 in 20,000–40,000 and 1 in 50,000, respectively). 1,300 cases had been reported as of 2006. Affected individuals typically grow and develop normally until puberty; the mean age of diagnosis is twenty-four, often realized when the adolescent growth spurt is not observed. The youngest person diagnosed was six years old. The median and mean ages of death are 47–48 and 54 years, respectively. The main cause of death is cardiovascular disease or cancer.
Characteristics
Werner syndrome patients exhibit growth retardation, short stature, premature graying of hair, alopecia (hair loss), wrinkling, prematurely aged faces with beaked noses, skin atrophy (wasting away) with scleroderma-like lesions, lipodystrophy (loss of fat tissues), abnormal fat deposition leading to thin legs and arms, and severe ulcerations around the Achilles tendon and malleoli (around ankles). Other symptoms include change in voice (weak, hoarse, high-pitched), atrophy of gonads leading to reduced fertility, bilateral cataracts (clouding of lens), premature arteriosclerosis (thickening and loss of elasticity of arteries), calcinosis (calcium deposits in blood vessels), atherosclerosis (blockage of blood vessels), type 2 diabetes, osteoporosis (loss of bone mass), telangiectasia, and malignancies. The prevalence of rare cancers, such as meningiomas, are increased in individuals with Werner syndrome.
Gene expression
Gene transcription changes found in WS cells are strikingly similar to those observed in normal aging. At the level of gene expression, WRN protein deficiency causes changes in the pattern of gene expression that markedly resemble those of normal old age.
DNA methylation
The blood of WS patients exhibits accelerated DNA methylation changes that are similar to those observed in normal aging according to a molecular biomarker of aging known as epigenetic clock.
Diagnosis and clinical symptoms
The
mutation in the WRN gene that causes Werner syndrome is autosomal and
recessive, meaning that sufferers must inherit a copy of the gene from
each parent. Patients display rapid premature aging beginning in young
adulthood, usually in their early twenties.
Diagnosis is based on six cardinal symptoms: premature graying of the
hair or hair loss, presence of bilateral cataracts, atrophied or tight
skin, soft tissue calcification, sharp facial features, and an abnormal,
high-pitched voice.
Patients are also generally short-statured due to absence of the
adolescent growth spurt. Patients also display decreased fertility.
The most common symptom of the six is premature graying and loss of
hair. This is also generally the earliest observed symptom, with hair
loss occurring first on the scalp and the eyebrows.
Werner syndrome patients often have skin that appears shiny and tight, and may also be thin or hardened. This is due to atrophy of the subcutaneous tissue and dermal fibrosis.
Over time, the characteristic facial features may be more apparent due
to these skin conditions. Other associated skin conditions include
ulcers,
which are very difficult to treat in Werner syndrome patients, and are
caused in part by decreased potential of skin cells for replication.
WS cataracts are distinctly different from those of normal aging. They are associated with problems in the lens posterior cortex and subcapsular regions. These cataracts are generally treatable with cataract surgery, which should restore normal vision.
Symptoms become apparent in the late teens and early twenties and
continue to progress. Most patients live to about fifty years of age.
The most common causes of death for people are associated diseases and
complications, especially atherosclerosis and cancer.
Associated diseases
Werner syndrome patients are at increased risk for several other diseases, many associated with aging. Atherosclerosis, the thickening of artery walls due to cholesterol buildup, is one common complication. While normal atherosclerosis generally involves the major arteries, smaller arterioles are more likely to be affected. It is possible nervous system disorders are associated. Brain atrophy is present in 40% of patients. Osteoporosis,
the loss of bone mineral density common in post-menopausal women, is
another common symptom. In contrast with the normal population, the rate
of osteoporosis is especially high for male patients. Diabetes mellitus is another common accompaniment. Skin ulcers occur in about 75% of patients – and can be difficult to treat. If skin ulcers become badly infected or develop gangrene, they often require amputation. Unlike most other related diseases and complications, these ulcers are not associated with normal aging.
Patients are also at an increased risk of cancer, especially malignant melanoma. Soft-tissue sarcomas are the most common cancer types. Other types of skin cancer, other epithelial cancers such as thyroid and liver cancers, MDS (myelodysplastic syndrome), and MFH (malignant fibrous histiocytoma) are also prevalent among. Mutations in the WRN gene, especially single-nucleotide polymorphisms
(SNPs), are associated with many of the cancers and other associated
diseases. WRN SNPs correlate with cancers such as sarcomas and
non-Hodgkin lymphomas, as well as diabetes and cardiovascular problems
including atherosclerosis.
Causes
Approximately 90% of individuals presenting Werner syndrome have any of a range of mutations in the gene, WRN, the only gene currently attributed to cause Werner syndrome. WRN, which lies on chromosome 8 in humans, encodes the WRNp protein, a 1432 amino acid protein with a central domain resembling members of the RecQ
helicases. RecQ helicases are a special type of helicase that function
at unique times during DNA repair of doubled stranded breaks, which are a
form of DNA damage
that results in a break of both strands of DNA. Thus, RecQ helicases
are important for maintaining DNA stability, and loss of function of
these helicases has important implications in the development of Werner
syndrome. In addition to the central domain, there are three exonuclease domains at the N-terminus and a Helicase and Ribonuclease D C-terminal (HRDC) domain at the C-terminus.
When functioning normally, the WRN gene and associated protein are important for maintaining genome stability. WRNp is active in unwinding DNA, a step necessary in DNA repair and DNA replication. Specifically, the WRN protein has an important role in responding to replication malfunctions, particularly double-stranded breaks, and stalled replication machinery.
WRN may reactivate replication by preventing unwanted recombination
processes from occurring or by promoting recombination, depending on the
type of DNA damage. In addition, the WRN protein physically interacts
with or binds to several other proteins that are involved in processing
DNA. For example, the WRN protein binds to RPA, which stimulates WRNp's helicase activity. WRNp also physically interacts with p53, a tumor suppressor gene that stops the formation of tumors and the progression of cancers, which inhibits the exonuclease activity of the WRNp. Since WRNp's function depends on DNA, it is only functional when localized to the nucleus.
DNA repair processes
The finding that WRN protein interacts with DNA-PKcs and the Ku protein
complex, combined with evidence that WRN deficient cells produce
extensive deletions at sites of joining of non-homologous DNA ends,
suggests a role for WRN protein in the DNA repair process of non-homologous end joining (NHEJ). WRN protein also physically interacts with the major NHEJ factor X4L4 (XRCC4-DNA ligase 4 complex). X4L4 stimulates WRN exonuclease activity that likely facilitates DNA end processing prior to final ligation by X4L4.
WRN protein appears to play a role in resolving recombination intermediate structures during homologous recombinational repair (HRR) of DNA double-strand breaks.
WRN protein participates in a complex with RAD51, RAD54, RAD54B and ATR proteins in carrying out the recombination step during inter-strand DNA cross-link repair.
Evidence was presented that WRN protein plays a direct role in the repair of methylation induced DNA damage. This process likely involves the helicase and exonuclease activities of WRN protein that operate together with DNA polymerase beta in long patch base excision repair.
Effects on cell structure and function
Mutations
which cause Werner syndrome all occur at the regions of the gene which
encode for protein, and not at non-coding regions. There are 35 different known mutations of WRN, which correspond to stop codons, insertions, or deletions that result in a frameshift mutation.
These mutations can have a range of effects. They may decrease the stability of the transcribed messenger RNA (mRNA), which increases the rate at which they are degraded. With less mRNA, less is available to be translated into the WRNp protein. Mutations may also lead to the truncation (shortening) of the WRNp protein, leading to the loss of its nuclear localization signal sequence, thus it is no longer transported into the nucleus where it interacts with the DNA. This leads to a reduction in DNA repair. Furthermore, mutated proteins are more likely to be degraded than normal WRNp.
Apart from causing defects in DNA repair, its aberrant association with
p53 down-regulates the function of p53, leading to a reduction in
p53-dependent apoptosis and increasing the survival of these
dysfunctional cells. Cells of affected individuals also have reduced lifespan in culture, have more chromosome breaks and translocations and have extensive deletions.
Patients with Werner syndrome lose the RecQ helicase activity in
the WRN protein because of the loss of its C-terminus region, but the
mechanism by which this happens is unclear. The loss of the helicase
activity can have far-reaching consequences in terms of cell stability
and mutation. One instance of these consequences involves telomeres.
It is thought that the WRN helicase activity is important not only for
DNA repair and recombination, but also for maintaining telomere length
and stability. Thus, WRN helicase is important for preventing
catastrophic telomere loss during DNA replication. In a normal cell, the telomeres (the ends of chromosomes) undergo repeated shortening during the cell cycle, which can prevent the cell from dividing and multiplying. This event can be counteracted by telomerase,
an enzyme that extends the ends of the chromosomes by copying the
telomeres and synthesizing an identical, but new end that can be added
to the existing chromosome.
However, patients with Werner syndrome often exhibit accelerated
telomere shortening, indicating that there may be a connection between
the loss of the WRN helicase activity and telomere and cell instability.
While evidence shows that telomere dysfunction is consistent with the
premature aging in WS, it has yet to be determined if it is the actual
cause of the genomic instability observed in cells and the high rate of
cancer in WS patients.
Without the WRN protein, the interwoven pathways of DNA repair
and telomere maintenance fail to suppress cancer and the aging symptoms
seen in patients with WS. Events such as rapid telomere shortening cause
Werner syndrome cells to exhibit low responses to overall cellular
stress. In addition to telomere dysfunction, over-expression of oncogenes and oxidation
can induce this type of response. High stress causes a synergistic
effect, where WS cells become even more sensitive to agents that
increase cell stress and agents that damage DNA. As a result, WS cells
show a drastic reduction in replicative lifespan and enter into a stage
of aging prematurely. The accumulation of these damaged cells due to
telomere shortening over many years may be indicative of why Werner
syndrome symptoms only appear after an individual is about twenty years
old.
Protection of DNA against oxidative damage
WRN protein was found to have a specific role in preventing or repairing DNA damages resulting from chronic oxidative stress, particularly in slowly replicating cells. This finding suggested that WRN may be important in dealing with oxidative DNA damages that underlie normal aging.
Treatment
A
cure for Werner syndrome has not yet been discovered. It is often
treated by managing the associated diseases and relieving symptoms to
improve quality of life. The skin ulcers that accompany WS can be
treated in several ways, depending on the severity. Topical treatments
can be used for minor ulcers, but are not effective in preventing new
ulcers from occurring. In the most severe cases, surgery may be required
to implant a skin graft
or amputate a limb if necessary. Diseases commonly associated with
Werner syndrome such as diabetes and cancer are treated in generally the
same ways as they would be for a non-Werner syndrome individual. A
change in diet and exercise can help prevent and control
arteriosclerosis, and regular cancer screenings can allow for early
detection of cancer.
There is evidence that suggests that the cytokine-suppressive anti-inflammatory drug SB203580 may be a possible therapeutic option for patients with Werner's syndrome. This drug targets the p38
signaling pathway, which may become activated as a result of genomic
instability and stalled replication forks that are characteristic
mutations in WS. This activation of p38 may play a role in the onset of
premature cell aging, skin aging, cataracts, and graying of the hair.
The p38 pathway has also been implicated in the anti-inflammatory
response that causes atherosclerosis, diabetes, and osteoporosis, all of
which are associated with Werner's syndrome. This drug has shown to
revert the aged characteristics of young WS cells to those seen in
normal, young cells and improve the lifespan of WS cells in vitro. SB203580 is in the clinical trial stages, and the same results have not yet been seen in vivo.
In 2010, vitamin C
supplementation was found to reverse the premature aging and several
tissue dysfunctions in a genetically modified mouse model of the
disease. Vitamin C supplementation also appeared to normalize several
age-related molecular markers such as the increased levels of the
transcription factor NF-κB.
In addition, it decreases activity of genes activated in human Werner
syndrome and increases gene activity involved in tissue repair.
Supplementation of vitamin C is suspected to be beneficial in the
treatment of human Werner syndrome, although there was no evidence of
anti-aging activity in nonmutant mice. In general, treatments are available for only the symptoms or complications and not for the disease itself.
Background and history
Otto Werner was the first to observe Werner syndrome in 1904 as a part of his dissertation research. As a German ophthalmologist, Werner described several progeria-like features and juvenile cataracts
in many of his patients. He noticed these symptoms particularly in a
family with four sequential children who all showed the characteristics
of the syndrome at around the same age. He assumed the cause to be
genetic, though most of his evidence was clinical. Between 1934 and
1941, two internists from New York, Oppenheimer and Kugel, coined the
term "Werner Syndrome," igniting a wave of interest and research on the
disease.
During that time, Agatson and Gartner suggested a possible link between
Werner's syndrome and cancer. However, It was not until 1966 that there
was a general consensus on the autosomal recessive mode of inheritance
for the syndrome. By 1981, geneticists
had located the WRN gene on chromosome 8, leading to its cloning in
1996. This cloning of the WRN was significant because it revealed the
predicted WRN protein was made from a family of DNA helicases.
Prior to 1996, Werner syndrome was thought to be a model for
accelerated aging. Since the discovery of the gene, it has become clear
that the premature aging displayed in Werner syndrome is not the same,
on a cellular level, as normal aging. The role of WRN in DNA repair and
its exonuclease and helicase activities have been the subject of many
studies in recent years.
Since the initial discovery in 1904, several other cases of
Werner syndrome have been recorded. Many of these cases have occurred in
Japan, where a founder effect
has caused a higher incidence rate than in other populations. The
incidence rate of Werner syndrome in Japan is approximately 1 case per
100 thousand people (1:100,000), a large contrast with the rate of
incidence for the rest of the world, which is between 1:1,000,000 and
1:10,000,000. A founder effect is also apparent in Sardinia, where there
have been 18 recorded cases of Werner syndrome.
Popular culture
On the episode "Stargazer in a Puddle" from the television series Bones,
the victim has Werner syndrome, the team discovering in the course of
the investigation that her mother killed her daughter because she was
dying of another disease and worried that her daughter would have nobody
to look after her afterwards, with the tragic twist that the mother
began to recover from her disease after her daughter's death.
Werner syndrome is featured in the 1996 film Jack, starring Robin Williams, in which his character ages four times faster than normal.
In an early cutscene from the game Metal Gear Solid 4, Otacon cites "classic Werner syndrome" as the most likely cause of Solid Snake's
premature aging, though he goes on to say that testing had been
inconclusive. It is however later said that Solid Snake's body, created
as a genetically engineered clone, had been designed to break down
quickly.
In season 3 episode 9, "The Ballad of Kevin and Tess", of the TV series The 4400, Kevin is said to have Werner syndrome to hide his real condition from the public.
In The Invisible Man
season 1 episode 6, "Impetus", the new character Gloria has an
experimentally altered type of Werner syndrome that causes it to become
contagious.
The central character in Gail Tsukiyama's novel DREAMING WATER (2002) has Werner's syndrome.
In season 1 episode 8 Cold Comfort from TV series Dark Angel,
a character has a "form of progeria, similar to Werner syndrome", due
to genetic manipulation. With an appropriate treatment, her condition
seems to be stabilized.
In *Resident Evil: The Final Chapter* (2016), the deadly "T-Virus," which causes the viral pandemic in the Resident Evil (film series),
is revealed to be the cure for "adult progeria." James Marcus
originally develops the virus to cure his young daughter Alicia Marcus.
Ratsasan
(2018) Tamil movie, features a young man born with Werner's and is a
victim of childhood bullying due to his appearance and has bad
experience proposing to a girl, who turns into serial killer and hunts
down and kills school girls.
