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2 research outputs found

Increased risk of malignancies in a population-based study of 818 soft-tissue sarcoma patients

Author: A Bladström
A Rydholm
A Rydholm
A Virtanen
AC Moll
AL Hartley
BR Korf
CB Pratt
CE Yu
CR Antonescu
DG Sheppard
G Bacci
G Bisogno
H Olsson
HT Lynch
HT Lynch
J Engellau
J Engellau
J Fernebro
JN Cormier
JP Neglia
K Hirata
KM Thijssens
LJ Helman
M Bassal
M Nilbert
M Paulussen
MS Brady
NE Breslow
NM Lindor
O Beaty III
O Fletcher
O Merimsky
P Gustafson
P Gustafson
R Heyn
R Listernick
R Sijmons
RA Kleinerman
RJ Cohen
SJ Kony
SR Grobmyer
U Tateishi
V Medina Arana
YM Kirova
Publication venue
Publication date: 01/01/2006
Field of study

Soft-tissue sarcomas (STS) have been associated with various rare cancer syndromes and occur at increased frequencies in survivors of childhood cancer. Also adult patients with STS have been suggested to be at an increased risk of additional malignancies. After exclusion of syndrome-associated and radiation-induced sarcomas, we studied multiple primary malignancies in a population-based cohort of 818 patients with primary STS of the extremities and the trunk wall. In total, 203 other malignancies developed in 164 (20%) patients median 10 (0–32) years before and median 4 (0–35) years after the sarcoma diagnosis. Standardised morbidity ratios (SMRs) were determined for primary malignancies following a STS. Hereby individuals who had developed a STS were identified to be at increased risk of second primary malignancies (SMR for all malignant tumours=1.3; 95% CI=1.0–1.5; P=0.02) with STS being the only specific tumour type that occurred at an increased risk (SMR=17.6; 95% CI=8.1–33.5; P<0.001). Hence, this population-based series demonstrates a high frequency of second primary tumours among STS patients and indicates a particularly increased risk of developing a new STS

Lund University Publications

Crossref

PubMed Central

Complex Segregation Analysis Provides Compelling Evidence for a Major Gene Underlying Obsessive-Compulsive Disorder and for Heterogeneity by Sex

Author: Beaty T. H.
Bienvenu III O. J.
Cullen B.
Grados M.
Hoehn-Saric R.
Lan T.
Liang K. Y.
Nestadt G.
Riddle M.
Samuels J.
Shugart Y. Y.
Publication venue: The American Society of Human Genetics
Publication date: 31/10/2000
Field of study

Evidence from twin and family studies supports a genetic etiology for obsessive-compulsive disorder (OCD). The purpose of this study was to test whether a major gene is implicated in a proportion of families with OCD. Complex segregation analyses of 153 families (80 case and 73 control), ascertained in the Johns Hopkins OCD Family Study, provided strong evidence for a major gene. A Mendelian-dominant model, with significant sex effects and with residual familial effects, best explained the observed data. Stratification of the sample by the sex of probands provided further evidence of heterogeneity with respect to familial aggregation. Segregation analyses of 86 families with a female proband and of the 67 families with a male proband suggested that a Mendelian-dominant model with familial residual effects was the most parsimonious model explaining the inheritance of OCD in both subgroups

Elsevier - Publisher Connector

PubMed Central