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Last update 01 Apr 2026
The American Thrombosis & Hemostasis Network
Last update 01 Apr 2026
Overview
Related
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Safety of SEVENFACT® for the Treatment of Bleeding Events in Patients With Hemophilia A or B With Inhibitors
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100 Clinical Results associated with The American Thrombosis & Hemostasis Network
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01 Aug 2025Research and Practice in Thrombosis and Haemostasis
Characterization of the clinical and laboratory phenotype of hemophilia carriers and trends of utilization of hemostatic therapies: analysis of the American Thrombosis and Hemostasis Network dataset
Article
Author: Currie, Alison ; Kulkarni, Roshni ; Pipe, Steven ; Swaminathan, Neeraja ; Kouides, Peter ; Hu, Jianzhong ; Sharathkumar, Anjali
Background:
Hemophilia carriers (HCs) experience varied bleeding tendencies affecting their quality of life, yet their bleeding phenotype and management remain poorly understood. Since majority of the studies in carriers have focused on women of reproductive age, an unmet need exists to characterize their clinical, laboratory phenotype and treatment patterns across the lifespan.
Objectives:
The objective of our study was to investigate the age-dependent clinical and laboratory phenotype of hemophilia carriers across the lifespan. We also aimed to study the longitudinal treatment trends in HCs through analysis of the American Thrombosis and Hemostasis Network dataset.
Methods:
We investigated the age-dependent variation of bleeding phenotype, coagulation factor levels, and trends of utilization of factor concentrates and nonfactor hemostatic therapies (antifibrinolytics, 1-desamino-8-D-arginine vasopressin) in HCs using the American Thrombosis and Hemostasis Network dataset from 2010 to 2020. The study included 3663 HCs (2728 hemophilia A, 935 hemophilia B) divided into 3 age groups: 0 to 12, 13 to 49, and >50 years.
Results:
Joint bleeding was prevalent across all ages of HCs. While bleeding events were more frequent among HCs within the reproductive-age group, hemophilia B carriers received factor therapy more frequently than hemophilia A carriers (P = .03). Factor (F)VIII activity levels in hemophilia A carriers increased significantly with age (P < .001). Analysis of treatment trends from 2010 to 2020 showed increased utilization of factor concentrates and nonfactor hemostatic therapies among HCs (P < .001 and P = .02, respectively).
Conclusion:
Our study confirms prior reports of increased bleeding in reproductive-age HCs and identifies lifelong joint bleeding risk. While the rising trend in hemostatic therapy use suggests growing awareness of bleeding tendencies, age-dependent increase in FVIII levels in hemophilia A carriers emphasizes the need for developing tailored management strategies across the lifespan for this population.
01 Jun 2025Journal of Parkinsons Disease
Intestinal biomarkers, microbiota composition, and genetic predisposition to inflammatory bowel disease as predictors of Parkinson's disease manifestation
Article
Author: Schwiertz, Andreas ; Lammert, Frank ; Fang, Gang ; Peter, Inga ; Debebe, Anketse ; Weber, Susanne N ; Fenton, Seth ; Augustin-Emmerichs, Kerstin ; Unger, Marcus M ; Picker, Mellissa ; Ouyang, Yuxia ; Hu, Jianzhong ; Lee, Won-Jun ; Becker-Dorison, Anouck ; Chai, Zhi
Background:
Parkinson's disease (PD) is often accompanied by gastrointestinal symptoms. While elevated inflammatory biomarkers have been reported in PD patients compared to controls, the role of intestinal dysmotility and inflammation in disease manifestation is not fully understood.
Objective:
This study sought to determine if fecal biomarkers and genetic predisposition to intestinal inflammation could help identify PD subtypes for future targeted therapies.
Methods:
The association of disease activity, assessed through United Parkinson's disease Rating Scale (UPDRS) and Non-Motor Symptoms Questionnaire (NMSQ), with constipation severity, fecal calprotectin and six short-chain fatty acid (SCFA) levels, polygenic risk scores (PRS) for inflammatory bowel disease (IBD) and PD, and microbiota diversity were investigated in 95 participants with established PD using regression analyses. Unsupervised k-means clustering was applied to stratify PD patients based on inflammatory biomarkers.
Results:
Having constipation was linked to worse mentation (UPDRSI, adj.
p
= 0.03) and more limited daily living activities (UPDRSII, adj.
p
= 0.03), with symptom severity linearly associated with higher disease activity (UPDRSI, adj.
p
= 0.002; NMSQ-total, adj.
p
= 0.02). Fecal calprotectin was elevated in those with constipation (
p
= 0.02) and associated with longer disease duration irrespective of the age (adj.
p
= 0.02). Cluster analysis demonstrated that PD patients with a higher non-motor symptom UPDRSII score were more likely to have more severe constipation, lower fecal SCFA levels, lower bacterial diversity, and higher PRS-CD and PRS-IBD.
Conclusions:
Gut dysmotility, along with pro-inflammatory intestinal profiles, and greater genetic predisposition to IBD were observed in PD patients with worse non-motor symptoms. Monitoring intestinal biomarkers may help identify PD patients for targeted interventions.
01 Mar 2025DIGESTIVE DISEASES AND SCIENCES
Elevated Fecal Lipocalin-2 Levels During Early Life Are Associated with Maternal Inflammatory Bowel Disease Diagnosis
Article
Author: Rendon, Alexa ; Stone, Joanne ; Peter, Inga ; Chen, Rosemary ; Agrawal, Manasi ; Mørk, Einar ; Barre, Amelie ; Hu, Jianzhong ; Thjømøe, Anne ; Picker, Mellissa ; Torres, Joana ; Weinstein, Kaitlyn ; Tarassishin, Leonid ; Colombel, Jean-Frederic ; Kim, Taegyu
BACKGROUND:
Fecal lipocalin-2 (LCN2) is a biomarker of neutrophil activation, which is elevated in patients with inflammatory bowel disease (IBD); however, its dynamic changes during pregnancy and early life are largely unknown. We characterized LCN2 levels by maternal IBD diagnosis, offspring feeding behavior, and gut microbiota composition.
METHODS:
In the prospective MECONIUM (Exploring Mechanisms of Disease Transmission In Utero through the Microbiome) study, we analyzed 559 fecal samples from 91 pregnant women with IBD, 78 healthy controls, and their 147 offspring for LCN2 levels at each trimester of pregnancy and multiple time points during early life using linear mixed-effects model and multiple logistic regression analyses. Gut microbiota community compositions were evaluated following 16S rRNA gene sequencing.
RESULTS:
IBD cases had higher LCN2 levels throughout pregnancy compared to controls. In offspring, significantly higher LCN2 was found in babies born to mothers with IBD, compared to those without IBD, at 3 months, 1 year, and 4 years (all p < 0.03), with offspring LCN2 levels being predictive of maternal IBD case status with > 85% accuracy at ages 1 and 4. We also detected correlations between LCN2 levels and certain IBD-associated bacterial taxa in both mothers and babies. Exclusively breastfed babies had lower LCN2 in the first weeks of life compared to formula or mixed-fed counterparts.
CONCLUSIONS:
Babies born to mother with IBD had significantly higher LCN2 during early life compared to controls with exclusive breastfeeding impacting LCN2 levels early on. LCN2 levels correlated with IBD-associated microbial taxa in both mothers and babies. Future studies should identify the biological drivers and health-related consequences of elevated LCN2 during early childhood.
100 Deals associated with The American Thrombosis & Hemostasis Network
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