Your search keyword '"Surcel Heljä-Marja"' showing total 6 results

1. Missed hepatitis b/c or syphilis diagnosis among Kurdish, Russian, and Somali origin migrants in Finland: linking a population-based survey to the national infectious disease register

Author

Tiittala, Paula, Ristola, Matti, Liitsola, Kirsi, Ollgren, Jukka, Koponen, Päivikki, Surcel, Heljä-Marja, Hiltunen-Back, Eija, Davidkin, Irja, and Kivelä, Pia

Published

2018

2. The MATEX cohort - a Finnish population register birth cohort to study health effects of prenatal exposures.

Author

Rumrich, Isabell K., Vähäkangas, Kirsi, Viluksela, Matti, Gissler, Mika, Surcel, Heljä-Marja, de Ruyter, Hanna, Jokinen, Jukka, and Hänninen, Otto

Subjects

PRENATAL exposure delayed effects, PREGNANT women, WOMEN'S tobacco use, AIR pollution, HEALTH, COHORT analysis, CHILDHOOD cancer, SUDDEN infant death syndrome risk factors, EPIDEMIOLOGY, PUBLIC health, CANCER risk factors, LONGITUDINAL method, SMOKING, ACQUISITION of data

Abstract

Background: The prevalence of chronic diseases, such as immune, neurobehavioral, and metabolic disorders has increased in recent decades. According to the concept of Developmental Origin of Health and Disease (DOHaD), developmental factors associated with environmental exposures and maternal lifestyle choices may partly explain the observed increase. Register-based epidemiology is a prime tool to investigate the effects of prenatal exposures over the whole life course. Our aim is to establish a Finnish register-based birth cohort, which can be used to investigate various (prenatal) exposures and their effects during the whole life course with first analyses focusing on maternal smoking and air pollution. In this paper we (i) review previous studies to identify knowledge gaps and overlaps available for cross-validation, (ii) lay out the MATEX study plan for register linkages, and (iii) analyse the study power of the baseline MATEX cohort for selected endpoints identified from the international literature.Methods/design: The MATEX cohort is a fully register-based cohort identified from the Finnish Medical Birth Register (MBR) (1987-2015). Information from the MBR will be linked with other Finnish health registers and the population register to link the cohort with air quality data. Epidemiological analyses will be conducted for maternal smoking and air pollution and a range of health endpoints.Discussion: The MATEX cohort consists of 1.75 million mother-child pairs with a maximum follow up time of 29 years. This makes the cohort big enough to reach sufficient statistical power to investigate rare outcomes, such as birth anomalies, childhood cancers, and sudden infant death syndrome (SIDS). The linkage between different registers allows for an extension of the scope of the cohort and a follow up from the prenatal period to decades later in life. [ABSTRACT FROM AUTHOR]

Published

2017

3. Hormone concentrations throughout uncomplicated pregnancies: a longitudinal study.

Author

Schock, Helena, Zeleniuch-Jacquotte, Anne, Lundin, Eva, Grankvist, Kjell, Lakso, Hans-Åke, Idahl, Annika, Lehtinen, Matti, Surcel, Heljä-Marja, and Fortner, Renée T.

Subjects

STEROID hormones, PREGNANCY, CHRONIC disease risk factors, CANCER risk factors, HORMONE research, PSYCHOLOGY, CELL receptors, ESTRADIOL, GESTATIONAL age, HORMONES, LONGITUDINAL method, MEMBRANE proteins, DURATION of pregnancy, FIRST trimester of pregnancy, SECOND trimester of pregnancy, THIRD trimester of pregnancy, PROGESTERONE, PROLACTIN, RESEARCH funding, SEX distribution, SMOKING, STEROIDS, TESTOSTERONE, PARITY (Obstetrics), BLOOD

Abstract

Background: Evidence suggests that the hormonal milieu of pregnancy is an important determinant of subsequent cancer and other chronic diseases in both the mother and the offspring. Many of the existing maternity and birth cohorts include specimens drawn only once during pregnancy. How well a single blood specimen collected during a pregnancy characterizes exposure to these hormones throughout gestation, and also in subsequent pregnancies, is not well understood.Methods: We used serial serum samples from 71 pregnant women (25 primiparous, 25 multiparous, and 21 with two consecutive pregnancies) with natural, complication-free pregnancies and a healthy offspring at term who participated in a population-based screening trial for congenital infections in Finland between January 1st, 1988 and June 30, 1989 and provided a blood sample in each trimester.Results: Hormone levels were more strongly correlated between consecutive trimesters of a pregnancy than between the 1st and 3rd trimester (e.g., estradiol, rT1 vs. T2 = 0.51 and rT2 vs. T3 = 0.60, p < 0.01; rT1 vs. T3 = 0.32, p < 0.05). Concentrations of sRANKL remained stable throughout gestation, whereas estradiol, estrone, progesterone, testosterone, prolactin, and osteoprotegerin increased throughout pregnancy. First trimester hormone concentrations explained less of the variation in the third trimester on their own than second trimester hormone levels (e.g. estradiol R(2) T1  = 16 % and R(2) T2 = 42 %). Addition of maternal (e.g., smoking) and/or child characteristics (e.g., sex) improved the accuracy of the 3rd trimester estimates for some of the hormones.Conclusions: One hormone measurement in early pregnancy, in conjunction with maternal and fetal characteristics, permits estimation of 3rd trimester hormone concentrations. Therefore, single hormone measurements available from maternity cohorts are suitable to quantify hormone exposure during pregnancy. To our knowledge, we provide the first data on correlations between hormone concentrations both across trimesters of a single pregnancy, as well as between two subsequent pregnancies. [ABSTRACT FROM AUTHOR]

Published

2016

4. Low avidity of human papillomavirus (HPV) type 16 antibodies is associated with increased risk of low-risk but not high-risk HPV type prevalence.

Author

Namujju, Proscovia B, Hedman, Lea, Hedman, Klaus, Banura, Cecily, Mbidde, Edward K., Kizito, Dennison, Byaruhanga, Romano N., Muwanga, Moses, Kirnbauer, Reinhard, Surcel, Heljä-Marja, and Lehtinen, Matti

Abstract

Background: Low avidity of antibodies against viral, bacterial and parasitic agents has been used for differential diagnosis of acute versus recent/past infections. The low-avidity antibodies may however, persist for a longer period in some individuals. Findings: We studied the association of human papillomavirus (HPV) type 16 antibody avidity with seroprevalence to HPV types 6/11/18/31/33/45. Antibody avidity was analysed for 365 HPV16 seropositive pregnant Finnish and Ugandan women using a modified ELISA. Low avidity of HPV16 antibodies was found in 15% of Finnish and 26% of Ugandan women. Ugandan women with low-avidity HPV16 antibodies had an increased risk estimate for HPV6/11 (odds ratio, OR 2.9; 95%CI 1.01-8.4) seropositivity but not to high-risk HPV types 18/31/33/45. Conclusion: Association of the low avidity HPV16 antibody "phenotype" with possible susceptibility to infections with other HPV types warrants investigation. [ABSTRACT FROM AUTHOR]

Published

2011

5. Newly discovered KI, WU, and Merkel cell polyomaviruses: No evidence of mother-to-fetus transmission.

Author

Sadeghi, Mohammadreza, Riipinen, Anita, Väisänen, Elina, Tingting Chen, Kantola, Kalle, Surcel, Heljä-Marja, Karikoski, Riitta, Taskinen, Helena, Söderlund-Venermo, Maria, and Hedman, Klaus

Subjects

POLYOMAVIRUSES, MERKEL cells, AUTOPSY, MISCARRIAGE, IMMUNOGLOBULINS

Abstract

Background: Three* human polyomaviruses have been discovered recently, KIPyV, WUPyV and MCPyV. These viruses appear to circulate ubiquitously; however, their clinical significance beyond Merkel cell carcinoma is almost completely unknown. In particular, nothing is known about their preponderance in vertical transmission. The aim of this study was to investigate the frequency of fetal infections by these viruses. We sought the three by PCR, and MCPyV also by real-time quantitative PCR (qPCR), from 535 fetal autopsy samples (heart, liver, placenta) from intrauterine fetal deaths (IUFDs) (N = 169), miscarriages (120) or induced abortions (246). We also measured the MCPyV IgG antibodies in the corresponding maternal sera (N = 462) mostly from the first trimester. Results: No sample showed KIPyV or WUPyV DNA. Interestingly, one placenta was reproducibly PCR positive for MCPyV. Among the 462 corresponding pregnant women, 212 (45.9%) were MCPyV IgG seropositive. Conclusions: Our data suggest that none of the three emerging polyomaviruses often cause miscarriages or IUFDs, nor are they transmitted to fetuses. Yet, more than half the expectant mothers were susceptible to infection by the MCPyV. [ABSTRACT FROM AUTHOR]

Published

2010

6. A discrepancy of Chlamydia trachomatis incidence and prevalence trends in Finland 1983-2003.

Author

Lyytikäinen E, Kaasila M, Hiltunen-Back E, Lehtinen M, Tasanen K, Surcel HM, Koskela P, and Paavonen J

Subjects

Adult, Antibodies, Bacterial blood, Chlamydia Infections immunology, Chlamydia trachomatis immunology, Cohort Studies, Female, Finland epidemiology, Humans, Immunoglobulin G blood, Incidence, Pregnancy, Pregnancy Complications, Infectious immunology, Prevalence, Seroepidemiologic Studies, Young Adult, Chlamydia Infections epidemiology, Pregnancy Complications, Infectious epidemiology

Abstract

Background: Reported rates of Chlamydia trachomatis are on the rise contradicting the declining rates of C. trachomatis associated reproductive sequelae in Western countries. Population based evaluation of the real trend of C. trachomatis infection is important to contemplate prevention efforts. We studied C. trachomatis occurrence during the past 20 years in Finland comparing incidence rate data based on serology and reported C. trachomatis laboratory notifications., Methods: A random sample of 7999 women with two consecutive pregnancies within five years was selected from the population of the Finnish Maternity Cohort (FMC) serum bank stratified by calendar year and age. C. trachomatis IgG antibodies were determined by a standard peptide-ELISA. The reported incidence rates of C. trachomatis infections based on case notifications were obtained from the National Registry of Infectious Diseases (NIDR)., Results: C. trachomatis seroprevalence rates decreased significantly from 1983 to 2003 both in women under 23 years of age (23.3% to 9.2%) and in women between 23-28-years of age (22.2% to 12.6%). However, seroconversion rates increased from 31 per 10000 person years in 1983-85 to 97 per 10000 person years in 2001-2003 (incidence rate ratio 3.2, 95% CI, 1.1-8.7) among the older age group. Seroconversion rate was highest (264) in 1983-1985 in the younger age-group, then declined and subsequently increased again (188) in 2001-2003. The incidence based on seroconversions was in agreement with the reported incidence rates in both age groups., Conclusion: C. trachomatis seroprevalence rate decreased during 1983-2003 among fertile-aged women in Finland. During the same time period incidence rates based both on seroconversions and reported laboratory notifications of diagnosed C. trachomatis infections increased. The discrepancy between the C. trachomatis incidence and seroprevalence trends warrants further studies.

Published

2008