Li–Fraumeni syndrome

Li–Fraumeni syndrome
Li–Fraumeni syndrome
Other names	Sarcoma family syndrome of Li and Fraumeni
	Li–Fraumeni syndrome is inherited via an autosomal dominant manner
Specialty	Oncology, medical genetics, neurology

Li–Fraumeni syndrome is a rare,

predisposes carriers to cancer development. It was named after two American physicians, Frederick Pei Li and Joseph F. Fraumeni Jr., who first recognized the syndrome after reviewing the medical records and death certificates of 648 childhood rhabdomyosarcoma patients.^[2]

This syndrome is also known as the sarcoma, breast, leukaemia and adrenal gland (SBLA) syndrome.

The syndrome is linked to

embryogenesis, or in one of the parent's germ cells

.

Presentation

Li–Fraumeni syndrome is characterized by early onset of cancer, a wide variety of types of cancers, and development of multiple cancers throughout one's life.[4]

Pathology

LFS1: Mutations in TP53

Normal conditions:^{[citation needed]} TP53 is a tumor suppressor gene on chromosome 17 that normally assists in the control of cell division and growth through action on the normal cell cycle. TP53 typically become expressed due to cellular stressors, such as DNA damage, and can halt the cell cycle to assist with either the repair of repairable DNA damage, or can induce apoptosis of a cell with irreparable damage. The repair of "bad" DNA, or the apoptosis of a cell, prevents the proliferation of damaged cells.^{[citation needed]}
Mutant conditions:
missense mutations in the DNA-binding domain.^[5]
These missense mutations cause a decrease in the ability of p53 to bind to DNA, thus inhibiting the normal TP53 mechanism.

LFS fibroblast cells that are homozygous for TP53 mutations are deficient in global nucleotide excision repair of DNA and have increased genetic instability.^[6] Also these cells have reduced ability to undergo apoptosis (programmed cell death) in response to DNA damage and thus are resistant to the ordinary lethal effect of DNA damage.^[6]
Unique Brazilian mutation: Although other mutations leading to Li–Fraumeni syndrome have been found outside the DNA-binding domain, a mutation at codon 337 of the tetramerization domain of TP53 has shown a particularly high frequency. The tetramerization domain plays a major role in the oligomerization of the p53 protein, which exists as a
incomplete penetrance.^{[citation needed}
]

Dominant negative mutations: Most individuals with Li–Fraumeni syndrome are heterozygous for a mutant TP53 gene, and some p53 mutants can inhibit the function of the wild-type p53 in a
dominant negative manner. Mutated p53 proteins are typically more stable than wild-type, and can inhibit the activity of the wild-type protein in suppressing cell proliferation and in inducing cell cycle arrest.^[8]^{[non-primary source needed}
] Due to the mutant p53 being able to inhibit some wild-type p53, damaged cells are at an even greater susceptibility to proliferate and become transformed, resulting in cancer.

LFS2: mutations in CHEK2

Another variant of Li–Fraumeni that remains somewhat controversial, is a mutation of the CHEK2 (or CHK2) gene.^[5] CHK2 is also a tumor suppressor gene; it regulates the action of p53 and is activated by ATM, which detects DNA damage, and in this way, DNA damage information can be conveyed to p53 to indirectly arrest the cell cycle at that point for DNA repair to be able to take place or to cause apoptosis (programmed cell death).

LFS-L:

Families who do not conform to the criteria of classical Li–Fraumeni syndrome have been termed "LFS-like".^[5] LFS-like individuals generally do not have any detectable p53 mutations, and tend to be diagnosed on either the Birch or Eeles criteria.

A third locus has been mapped to the long arm of chromosome 1 (1q23), but no gene has yet been identified.^{[citation needed]}

Another locus that has been linked to this syndrome is CDKN2A-CDKN2B.^[9]

Clinical

The classical LFS malignancies—sarcoma, cancers of the breast, brain, and adrenal glands—comprise about 80% of all cancers that occur in this syndrome.

The risk of developing any invasive cancer (excluding skin cancer) is about 50% by age 30 (1% in the general population) and is 90% by age 70. Early-onset breast cancer accounts for 25% of all the cancers in this syndrome. This is followed by soft-tissue sarcomas (20%), bone sarcoma (15%), and brain tumors—especially glioblastomas—(13%). Other tumours seen in this syndrome include leukemia, lymphoma, and adrenocortical carcinoma.

About 90% of females with LFS develop breast cancer by age 60 years; the majority of these occur before age 45 years. Females with this syndrome have almost a 100% lifetime risk of developing cancer. This compares with 73% for affected males. The difference may be due to much smaller breast tissue in males and increased estrogen levels in females.

The risks of sarcoma, female breast cancer, and haematopoietic malignancies in mutation carriers are more than 100 times greater than those seen in the general population.

Other tumours reported in this syndrome, but not yet proved to be linked with it, include melanoma, Wilms' and other kidney tumors, hepatocellular carcinoma, gonadal germ cell, pancreatic, gastric, choroid plexus, colorectal, and prostate cancers.

Around 80% of children with adrenocortical carcinoma and 2–10% of childhood brain tumors have p53 mutations. About 2–3% of osteosarcomas, 9% of rhabdomyosarcomas, and 7–20% of patients with multiple primary tumours have p53 mutations.^{[citation needed]}

Although most cases of this syndrome have early onset of cancer, cases have also been reported later in life.^[10]^{[non-primary source needed]}

Diagnosis

Li–Fraumeni syndrome is diagnosed if these three criteria are met:

The patient has been diagnosed with a sarcoma at a young age (below 45).
A first-degree relative has been diagnosed with any cancer at a young age (below 45).
Another first- or a second-degree relative has been diagnosed with any cancer at a young age (below 45) or with a sarcoma at any age.^{[citation needed]}

Other criteria have also been proposed:^[11]^{[non-primary source needed]}

A proband with any childhood cancer or sarcoma, brain tumor or adrenal cortical carcinoma diagnosed before age 45
A first- or second-degree relative with a typical LFS malignancy (sarcoma, leukaemia, or cancers of the breast, brain or adrenal cortex) regardless of age at diagnosis
A first- or second-degree relative with any cancer diagnosed before age 60

A third criterion has been proposed:^[12]

Two first- or second-degree relatives with LFS-related malignancies at any age.^{[verification needed]}

Management

Genetic counseling and genetic testing are used to confirm that somebody has this gene mutation.^{[citation needed]} Once such a person is identified, early and regular screenings for cancer are recommended for them as people with Li–Fraumeni are likely to develop another primary malignancy at a future time (57% within 30 years of diagnosis).^{[citation needed]}

Chompret criteria

A 2015 revision of the traditional Chompret criteria for screening has been proposed—a proband who has:^[13]

A tumor belonging to LFS tumor spectrum (e.g., premenopausal breast cancer, soft tissue sarcoma, osteosarcoma, CNS tumor, adrenocortical carcinoma) before age 46 years, and at least one first- or second-degree relative with LFS tumor (except breast cancer if the proband has breast cancer) before age 56 years or with multiple tumors at any age
Multiple tumors (except multiple breast tumors), two of which belong to LFS spectrum with the initial cancer occurring before the age of 46 years
An adrenocortical carcinoma, choroid plexus tumor, or rhabdomyosarcoma of embryonal anaplastic subtype, at any age of onset, irrespective of family history
Breast cancer before age 31

Recommendations

Recommendations for individuals from families affected by the syndrome include:^{[citation needed]}

Avoidance of radiation therapy to reduce risk of secondary radiation-induced malignancies
Children and adults undergo comprehensive annual physical examination
Women undergo age-specific breast cancer monitoring beginning at age 25 years
All patients consult a physician promptly for evaluation of lingering symptoms and illnesses

Suggestions

Adults should undergo routine screening for colorectal cancer beginning no later than age 25 years.
Individuals should undergo organ-targeted surveillance based on the pattern of cancer observed in their families.
Prophylactic mastectomy to reduce the risk of breast cancer is an option.

Epidemiology

Li–Fraumeni syndrome (LFS) is rare;^{[clarification needed]} as of 2011, cases had been reported in more than 500 families.^[5] The syndrome was discovered using an epidemiological approach. Li and Fraumeni identified four families in which siblings or cousins of rhabdomyosarcoma patients had a childhood sarcoma, which suggested a familial cancer syndrome.^[14]^{[non-primary source needed]}^[15] Identification of TP53s the gene affected by mutation was suggested by the same approach. Over half of the cancers in LFS families had been previously associated with inactivating mutations of the p53 gene and in one primary research study, DNA sequencing in samples taken from five Li–Fraumeni syndrome families showed autosomal dominant inheritance of a mutated TP53 gene.^[14]^[15]^{[non-primary source needed]}

References

PMID 23733769
.

S2CID 7540982
.

PMID 12619118
.

PMID 9554443
.

^
PMID 21779515
.

^ ^a ^b Ford JM, Hanawalt PC. Li-Fraumeni syndrome fibroblasts homozygous for p53 mutations are deficient in global DNA repair but exhibit normal transcription-coupled repair and enhanced UV resistance. Proc Natl Acad Sci U S A. 1995 Sep 12;92(19):8876-80. doi: 10.1073/pnas.92.19.8876. PMID 7568035; PMCID: PMC41070

PMID 11420672
.

PMID 14743206
.

S2CID 1667633
.

PMID 23667851
.

PMID 8118819
.

PMID 8718514
.

PMID 26014290
.

^
PMID 1978757.{{cite journal}}: CS1 maint: multiple names: authors list (link
)

^
S2CID 27235459
.

Further reading

Li–Fraumeni Syndrome by Katherine Schneider, MPH, Kristin Zelley, MS, Kim E Nichols, MD and Judy Garber, MD, MPH, in GeneReviews, a section of GeneTests, published online by the University of Washington with funds from the National Institutes of Health

Li–Fraumeni syndrome, in the
National Library of Medicine

Li–Fraumeni syndrome; LFS1, entry in Online Mendelian Inheritance in Man (OMIM), published by Johns Hopkins University and the National Institutes of Health

v
t
e
Metabolic disease: DNA replication and DNA repair-deficiency disorder
DNA replication

Separation/initiation: RNASEH2A
Aicardi–Goutières syndrome 4

Termination/telomerase: DKC1
Dyskeratosis congenita

DNA repair
Nucleotide excision repair

Cockayne syndrome/DeSanctis–Cacchione syndrome

Thymine dimer

Xeroderma pigmentosum

IBIDS syndrome

MSI/DNA mismatch repair

Hereditary nonpolyposis colorectal cancer

Muir–Torre syndrome

Mismatch repair cancer syndrome

MRN complex

Ataxia–telangiectasia

Nijmegen breakage syndrome

Other

RecQ helicase
Bloom syndrome

Werner syndrome

Rothmund–Thomson syndrome/RAPADILINO syndrome

Fanconi anemia

Li–Fraumeni syndrome

Severe combined immunodeficiency

v
t
e
Genetic disorders relating to deficiencies of transcription factor or coregulators
(1) Basic domains
1.2

Feingold syndrome

Saethre–Chotzen syndrome

1.3

Tietz syndrome

(2) Zinc finger
DNA-binding domains
2.1

(Intracellular receptor): Thyroid hormone resistance

Androgen insensitivity syndrome
PAIS

MAIS

CAIS

Kennedy's disease

PHA1AD pseudohypoaldosteronism

Estrogen insensitivity syndrome

X-linked adrenal hypoplasia congenita

MODY 1

Familial partial lipodystrophy 3

SF1 XY gonadal dysgenesis

2.2

Barakat syndrome

Tricho–rhino–phalangeal syndrome

2.3

Greig cephalopolysyndactyly syndrome/Pallister–Hall syndrome

Denys–Drash syndrome

Duane-radial ray syndrome

MODY 7

MRX 89

Townes–Brocks syndrome

Acrocallosal syndrome

Myotonic dystrophy 2

2.5

Autoimmune polyendocrine syndrome type 1

(3) Helix-turn-helix domains
3.1

ARX
Ohtahara syndrome

Lissencephaly X2

MNX1
Currarino syndrome

HOXD13
SPD1 synpolydactyly

PDX1
MODY 4

LMX1B
Nail–patella syndrome

MSX1

Tooth and nail syndrome

OFC5

PITX2
Axenfeld syndrome 1

POU4F3
DFNA15

POU3F4
DFNX2

ZEB1
Posterior polymorphous corneal dystrophy

Fuchs' dystrophy 3

ZEB2
Mowat–Wilson syndrome

3.2

PAX2
Papillorenal syndrome

PAX3
Waardenburg syndrome 1&3

PAX4
MODY 9

PAX6
Gillespie syndrome

Coloboma of optic nerve

PAX8
Congenital hypothyroidism 2

PAX9
STHAG3

3.3

FOXC1
Axenfeld syndrome 3

Iridogoniodysgenesis, dominant type

FOXC2
Lymphedema–distichiasis syndrome

FOXE1
Bamforth–Lazarus syndrome

FOXE3
Anterior segment mesenchymal dysgenesis

FOXF1
ACD/MPV

FOXI1
Enlarged vestibular aqueduct

FOXL2

Premature ovarian failure 3

FOXP3
IPEX

3.5

IRF6
Van der Woude syndrome

Popliteal pterygium syndrome

(4) β-Scaffold factors
with minor groove contacts
4.2

Hyperimmunoglobulin E syndrome

4.3

Holt–Oram syndrome

Li–Fraumeni syndrome

Ulnar–mammary syndrome

4.7

Campomelic dysplasia

MODY 3

MODY 5

SF1
SRY XY gonadal dysgenesis

Premature ovarian failure 7

SOX10
Waardenburg syndrome 4c

Yemenite deaf-blind hypopigmentation syndrome

4.11

Cleidocranial dysostosis

(0) Other transcription factors
0.6

Kabuki syndrome

Ungrouped

TCF4
Pitt–Hopkins syndrome

ZFP57
TNDM1

TP63
OFC8

Transcription coregulators
Coactivator:

CREBBP
Rubinstein–Taybi syndrome

Corepressor:

HR (Atrichia with papular lesions)

v
t
e
Deficiencies of intracellular signaling peptides and proteins
GTP-binding protein regulators
GTPase-activating protein

Neurofibromatosis type I

Watson syndrome

Tuberous sclerosis

Guanine nucleotide
exchange factor

Marinesco–Sjögren syndrome

Aarskog–Scott syndrome

Juvenile primary lateral sclerosis

X-linked intellectual disability 1

G protein
Heterotrimeic

cAMP/GNAS1: Pseudopseudohypoparathyroidism

Progressive osseous heteroplasia

Pseudohypoparathyroidism

Albright's hereditary osteodystrophy

McCune–Albright syndrome

CGL 2

Monomeric

RAS: HRAS
Costello syndrome

KRAS
Noonan syndrome 3

KRAS Cardiofaciocutaneous syndrome

RAB: RAB7
Charcot–Marie–Tooth disease

RAB23
Carpenter syndrome

RAB27
Griscelli syndrome type 2

RHO: RAC2
Neutrophil immunodeficiency syndrome

SAR1B

Chylomicron retention disease

ARL13B
Joubert syndrome 8

ARL6
Bardet–Biedl syndrome 3

MAP kinase

Cardiofaciocutaneous syndrome

Other kinase/phosphatase
Tyrosine kinase

BTK
X-linked agammaglobulinemia

ZAP70
ZAP70 deficiency

Serine/threonine
kinase

RPS6KA3
Coffin-Lowry syndrome

CHEK2
Li–Fraumeni syndrome 2

IKBKG
Incontinentia pigmenti

STK11
Peutz–Jeghers syndrome

DMPK
Myotonic dystrophy 1

ATR
Seckel syndrome 1

GRK1
Oguchi disease 2

WNK4/WNK1
Pseudohypoaldosteronism 2

Tyrosine
phosphatase

PTEN
Bannayan–Riley–Ruvalcaba syndrome

Lhermitte–Duclos disease

Cowden syndrome

Proteus-like syndrome

MTM1
X-linked myotubular myopathy

PTPN11
Noonan syndrome 1

LEOPARD syndrome

Metachondromatosis

Signal transducing adaptor proteins

EDARADD
EDARADD Hypohidrotic ectodermal dysplasia

SH3BP2
Cherubism

LDB3
Zaspopathy

Other

NF2
Neurofibromatosis type II

Notch 3

CADASIL

PRKAR1A
Carney complex

PRKAG2
Wolff–Parkinson–White syndrome

PRKCSH
PRKCSH Polycystic liver disease

XIAP
XIAP2

See also intracellular signaling peptides and proteins

Classification
ICD-9-CM: 758.3
OMIM: 151623
MeSH: D016864
DiseasesDB: 7450
External resources
eMedicine: ped/1305
Orphanet: 524

Authority control databases: National

Latvia

Retrieved from "https://en.wikipedia.org/w/index.php?title=Li–Fraumeni_syndrome&oldid=1185181982"

[pmid_23733769-1] PMID 23733769
.

[pmid5360287-2] S2CID 7540982
.

[pmid12619118-3] PMID 12619118
.

[HisadaGarber1998-4] PMID 9554443
.

[malkin-5] 
PMID 21779515
.

[Ford1995-6] Ford JM, Hanawalt PC. Li-Fraumeni syndrome fibroblasts homozygous for p53 mutations are deficient in global DNA repair but exhibit normal transcription-coupled repair and enhanced UV resistance. Proc Natl Acad Sci U S A. 1995 Sep 12;92(19):8876-80. doi: 10.1073/pnas.92.19.8876. PMID 7568035; PMCID: PMC41070

[7] PMID 11420672
.

[8] PMID 14743206
.

[Chan2016-9] S2CID 1667633
.

[Cho2013-10] PMID 23667851
.

[Birch1994-11] PMID 8118819
.

[12] PMID 8718514
.

[13] PMID 26014290
.

[malkinD-14] 
PMID 1978757.{{cite journal}}: CS1 maint: multiple names: authors list (link
)

[malkinD_CORRECTION-15] 
S2CID 27235459
.

[2]

[5]

[6]

[9]

[10]

[11]

[12]

[13]

[14]

[15]