High prevalence and breast cancer predisposing role of the BLM c.1642 C&gt;T (Q548X) mutation in Russia

Sokolenko, Anna P.; Iyevleva, Aglaya G.; Preobrazhenskaya, Elena V.; Mitiushkina, Natalia V.; Abysheva, Svetlana N.; Suspitsin, Evgeny N.; Kuligina, Ekatherina Sh.; Gorodnova, Tatiana V.; Pfeifer, Werner; Togo, Alexandr V.; Turkevich, E A; Ivantsov, Alexandr O.; Voskresenskiy, Dmitry V; Dolmatov, Georgy D; Bit-Sava, E.M.; Matsko, Dmitry E.; Семиглазов, Владимир; Fichtner, Iduna; Larionov, Alexey; Kuznetsov, Sergey G.; Antoniou, Antonis C.; Imyanitov, Evgeny N.

doi:10.1002/ijc.26342

Cited by 62 publications

(58 citation statements)

References 39 publications

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“…The founder populations represent a genetically enriched subgroup ideal for gene discovery studies 8,[37][38][39] . The enrichment of the qpcs with participants of French-Canadian descent is particularly valuable because fpdac is prevalent in that population 40 .…”

Section: Discussionmentioning

confidence: 99%

Establishing a Clinic-Based Pancreatic Cancer and Periampullary Tumour Research Registry in Quebec

Bascuñana

Hall

et al. 2015

Current Oncology

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Participation rates were 88.4% for all referrals and 89.2% for pdac referrals. Family history, epidemiologic and clinical data, and biospecimens were ascertained from 91.9%, 54.6%, and 97.5% respectively of patients with pdac. Although demographics and trends in risk factors in our patients were consistent with published statistics for patients with pdac, the qpcs is enriched for families with French-Canadian ancestry (37.4%), a population with recurrent germline mutations in hereditary diseases. ConclusionsUsing rapid ascertainment, a pdac and pat research registry with high participation rates can be established. The qpcs is a valuable research resource and its enrichment with patients of French-Canadian ancestry provides a unique opportunity for studies of heredity in these diseases.

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Section: Discussionmentioning

confidence: 99%

Establishing a Clinic-Based Pancreatic Cancer and Periampullary Tumour Research Registry in Quebec

Bascuñana

Hall

et al. 2015

Current Oncology

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“…We recently analyzed the BLM gene as a candidate for hereditary breast cancer (BC), and revealed its association with BC risk [Sokolenko et al, 2012]. The BC-predisposing role of BLM was later confirmed by exome sequencing and case-control studies [Thompson et al, 2012;Prokofyeva et al, 2013], although a negative report has been published as well [Anisimenko et al, 2014].…”

Section: Novel Insightsmentioning

confidence: 99%

“…However, it is still appropriate to expect an increased occurrence of BS in this part of the world. After the initial publication on high frequency of the BLM c.1642C>T (p.Q548X) mutation [Sokolenko et al, 2012], we contacted all major genetic centers operating in Russia by telephone, but no patients with BS were identified upon this effort. …”

Section: Novel Insightsmentioning

confidence: 99%

First Two Cases of Bloom Syndrome in Russia: Lack of Skin Manifestations in a BLM c.1642C>T (p.Q548X) Homozygote as a Likely Cause of Underdiagnosis

Suspitsin

Sibgatullina

Lyazina³

et al. 2017

Mol Syndromol

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hypersensitivity to ultraviolet irradiation, and a strong predisposition to early-onset cancers. We have previously described a recurrent BLM c.1642C>T (p.Q548X) mutation, which is present in heterozygous state in 0.2-0.6% of individuals of Slavic origin. Despite the high occurrence of this founder allele, BS has not yet been described in patients of Slavic ethnicity. Here, we present 2 cases of BS, which were missed by standard genetic counseling and were eventually identified entirely due to chance. Our patients show Key WordsBloom syndrome · Immune deficiency · Short stature · Photosensitivity · Recurrent mutations Abstract Bloom syndrome (BS) is an exceptionally rare hereditary disease. Typical manifestations of BS usually include growth deficiency, a characteristic facial appearance, skin

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“…A large deletion of exons 20-22 was characteristic among persons with BS from Portugal or Brazil, Gln700 * was found among BS Italians or Americans with Italian ancestry, and Ser186 * as well as Asn515fs account for most Japanese BS chromosomes. The mutation Gln548 * is more frequent in Slavic populations with a carrier frequency of 0.1% [Sokolenko et al, 2012;Prokofyeva et al, 2013].…”

Section: Structure and Function Of The Blm Genementioning

confidence: 99%

“…Among 64 different mutations that were reported by German et al [2007], 19 were recurrent, including several from Portugese/Brazilian, Japanese, Anglo-German, and Italian American persons. A recurrent founder allele (c.1642C>T) of BLM has also been identified in Slavic populations of Eastern Europe [Sokolenko et al, 2012].…”

mentioning

confidence: 99%

Bloom's Syndrome: Clinical Spectrum, Molecular Pathogenesis, and Cancer Predisposition

2016

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Bloom's syndrome is an autosomal recessive disorder characterized by prenatal and postnatal growth deficiency, photosensitive skin changes, immune deficiency, insulin resistance, and a greatly increased risk of early onset of cancer and for the development of multiple cancers. Loss-of-function mutations of BLM, which codes for a RecQ helicase, cause Bloom's syndrome. The absence of a functional BLM protein causes chromosome instability, excessive homologous recombination, and a greatly increased number of sister chromatid exchanges that are pathognomonic of the syndrome. A common founder mutation designated blm^Ash is present in about 1 in 100 persons of Eastern European Jewish ancestry, and there are additional recurrent founder mutations among other populations. Missense, nonsense, and frameshift mutations as well as multiexonic deletions have all been observed. Bloom's syndrome is a prototypical chromosomal instability syndrome, and the somatic mutations that occur as a result of that instability are responsible for the increased cancer risk. Although there is currently no treatment aimed at the underlying genetic abnormality, persons with Bloom's syndrome benefit from sun protection, aggressive treatment of infections, surveillance for insulin resistance, and early identification of cancer.

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High prevalence and breast cancer predisposing role of the BLM c.1642 C>T (Q548X) mutation in Russia

Cited by 62 publications

References 39 publications

Establishing a Clinic-Based Pancreatic Cancer and Periampullary Tumour Research Registry in Quebec

Establishing a Clinic-Based Pancreatic Cancer and Periampullary Tumour Research Registry in Quebec

First Two Cases of Bloom Syndrome in Russia: Lack of Skin Manifestations in a BLM c.1642C>T (p.Q548X) Homozygote as a Likely Cause of Underdiagnosis

Bloom's Syndrome: Clinical Spectrum, Molecular Pathogenesis, and Cancer Predisposition

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