Susceptibility and modifier genes in Portuguese transthyretin V30M amyloid polyneuropathy: complexity in a single-gene disease

Soares, Miguel Luz; Coelho, Teresa; Sousa, Alda; Batalov, Serge; Conceição, Isabel; Sales-Luis, M.L.; Ritchie, Marylyn D.; Williams, Scott M.; Nievergelt, Caroline M.; Schork, Nicholas J.; Saraiva, Maria João; Buxbaum, Joel N.

doi:10.1093/hmg/ddi051

Cited by 100 publications

(87 citation statements)

References 36 publications

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“…We also included five SNPs previously studied in order to replicate the results found by Soares et al 9 The SNP frequencies in the European population were obtained by resorting to the HapMap Project and dbSNP. All variants were submitted to the Leiden Open Variation Database shared installation (URL: http://databases.lovd.nl/ shared/screenings?search_owned_by_=="Carolina%20Lemos"), with the following submission IDs: APCS: http://www.lovd.nl/APCS; AR: http://www.…”

Section: Selection Of Snps and Genotypingmentioning

confidence: 99%

“…7 Some modifier genes such as amyloid P component, serum (APCS), complement C1QA and C1QC and plasma retinol-binding protein 4 (RBP4) have been unraveled so far but they only explain a small part of the AO variability in FAP ATTRV30M. 8,9 In a previous study, Soares et al 9 compared Portuguese patients in a classic casecontrol approach; these authors found that the variants studied in the APCS gene had a combined modifier effect when analyzing early-onset group versus controls, whereas the combination of one variant from APCS (rs6689429) and two variants from RBP4 (rs7091052 and rs28383574) seemed to be involved with late-onset group. 9 No comparisons were made between early-and late-onset cases.…”

Section: Introductionmentioning

confidence: 99%

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Variants in RBP4 and AR genes modulate age at onset in familial amyloid polyneuropathy (FAP ATTRV30M)

et al. 2015

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Familial amyloid polyneuropathy (FAP) ATTRV30M is a neurodegenerative disorder due to point mutations in the transthyretin gene, with V30M being the commonest. FAP ATTRV30M shows a wide variation in age at onset (AO) between clusters, families and generations. Portuguese patients also show remarkable AO differences between genders. Genes found to be associated with FAP ATTRV30M pathways may act as AO modifiers. Our aim was to further explore the role of APCS and RBP4 genes and to study for the first time the involvement of sex-linked genetic modifiers -AR and HSD17B1 genes -in AO variation in Portuguese families. We collected DNA from a sample of 318 patients, currently under follow-up. A total of 18 tagging SNPs from APCS, RBP4, AR and HSD17B1 and 5 additional SNPs from APCS and RBP4 previously studied were genotyped. To account for nonindependency of AO between members of the same family, we used generalized estimating equations (GEEs). We found that APCS and RBP4 were associated with late AO. In addition, rs11187545 of the RBP4 was associated with an early AO. For the AR, in the male group three SNPs were associated with an early AO, whereas in the female group four were associated with both an early and later AO. These results strengthened the role of APCS and RBP4 genes and revealed for the first time the contribution of AR genes as an AO modifier in both males and females. These findings may have important implications in genetic counseling and for new therapeutic strategies.

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Section: Selection Of Snps and Genotypingmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Variants in RBP4 and AR genes modulate age at onset in familial amyloid polyneuropathy (FAP ATTRV30M)

et al. 2015

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“…Those studies did not show significant effects of any of the five genes analyzed, but demonstrated that many more interactions among alleles at these loci occurred in patients with late onset of the disease than among individuals with early onset. 109 These results suggested that early onset was the default state of the mutation and interactions with the products of some of these alleles delayed the appearance of symptoms, contributing perhaps 25% to the late onset phenotype. The sample size was not sufficiently large to establish whether single gene effects were also present.…”

Section: Other Genetic Lessons Learned From the Amyloidosesmentioning

confidence: 94%

The genetics of the amyloidoses: interactions with immunity and inflammation

Buxbaum

2006

Genes Immun

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Historically, the amyloidoses have been associated with inflammation and the immune response. From Virchow's original description in human pathologic inflammatory states through their identification in horses used to produce antitoxin to their frequent occurrence in the course of multiple myeloma and a somewhat abortive designation as 'gammaloid', the disorders were felt to have an inflammatory origin. These presumptive associations antedated the availability of a reliable method for tissue extraction that would allow chemical analysis of the major deposited molecules. With the identification of the multiple precursors and the realization that most were not intrinsic elements of immune/inflammatory pathways, the investigative emphasis shifted to the analysis of the biophysical events involved in aggregation and fibril formation. As more in vivo models and better tools for examination of tissues have become available, it appears as if inflammation may participate as both a response to, and an amplifier of, the effects of the fibrillar aggregates. Hence, while only a limited number of amyloid protein precursors are involved in immunity and inflammation per se, host defense, in its broadest sense, is likely to be involved in the clinically relevant amyloidoses. Further it now appears that harnessing the immune respone in an appropriate fashion may be able to play a role in treatment.

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“…We have demonstrated an interaction between TTR and RBP-4. Moreover, Soares et al (25) reported RBP-4 to play a role in Portuguese TTR v30M amyloid polyneuropathy.…”

Section: A B Cmentioning

confidence: 99%

Confirmation of the biological significance of transthyretin as a biomarker for cutaneous T-cell lymphoma by its protein interaction partners

Eggeling¹

2010

Mol Med Rep

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Abstract. We previously identified transthyretin (TTR) and its posttranslational modifications as a down-regulated marker in mycosis fungoides (MF), a benign subtype of cutaneous T-cell lymphoma (CTCL). In order to more precisely understand the biological role of TTR in the etiology of MF, it is essential to clarify the pathways of progression by identifying further interacting proteins. This study is the first to combine blue native polyacrylamide gel electrophoresis (BN-PAGE) with surface enhanced laser desorption/ionization time-of-flight mass spectrometry (SELDI-TOF-MS) to detect new TTR interaction partners and to determine whether these TTR interaction partners can themselves be used as biomarkers. By this procedure, apolipoprotein A1, which was additionally found to be down-regulated in the serum of MF patients, apolipoprotein A4, retinol binding protein 4 (RBP-4), and retinoid X receptor β (RXR-β) were identified as interaction partners of TTR. The RXR family plays a role in cell differentiation and proliferation and is known to be the target of bexarotene, which is used in the treatment of CTCL. In conclusion, the combination of BN-PAGE and SELDI-TOF-MS used in this study allowed for the detection of protein interaction partners, which, in the case of RBP-4 and RXR, indicated a connection between the common tumor marker TTR and tumor progression in CTCL.

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Susceptibility and modifier genes in Portuguese transthyretin V30M amyloid polyneuropathy: complexity in a single-gene disease

Cited by 100 publications

References 36 publications

Variants in RBP4 and AR genes modulate age at onset in familial amyloid polyneuropathy (FAP ATTRV30M)

Variants in RBP4 and AR genes modulate age at onset in familial amyloid polyneuropathy (FAP ATTRV30M)

The genetics of the amyloidoses: interactions with immunity and inflammation

Confirmation of the biological significance of transthyretin as a biomarker for cutaneous T-cell lymphoma by its protein interaction partners

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