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Maria Terradas-Terradas

Explore the profile of Maria Terradas-Terradas including associated specialties, affiliations and a list of published articles. Areas
Snapshot
Articles 4
Citations 73
Followers 0
Related Specialties
General Medicine
Biology
Cell Biology
Top 10 Co-Authors
Kristina Kirschner
Tamir Chandra
Neil A Robertson
Riccardo E Marioni
Ian J Deary
Robert F Hillary
Joseph A Marsh
Lucy M Gee
Fiona Oakley
David P Baird
Published In
Curr Biol
Nat Cell Biol
Mech Ageing Dev
Nat Med
Affiliations
Soon will be listed here.
Recent Articles
1.
Hepatocellular senescence induces multi-organ senescence and dysfunction via TGFβ
Kiourtis C, Terradas-Terradas M, Gee L, May S, Georgakopoulou A, Collins A, et al.
Nat Cell Biol . 2024 Nov; 26(12):2075-2083. PMID: 39537753
Cellular senescence is not only associated with ageing but also impacts physiological and pathological processes, such as embryonic development and wound healing. Factors secreted by senescent cells affect their microenvironment...
2.
Longitudinal dynamics of clonal hematopoiesis identifies gene-specific fitness effects
Robertson N, Latorre-Crespo E, Terradas-Terradas M, Lemos-Portela J, Purcell A, Livesey B, et al.
Nat Med . 2022 Jul; 28(7):1439-1446. PMID: 35788175
Clonal hematopoiesis of indeterminate potential (CHIP) increases rapidly in prevalence beyond age 60 and has been associated with increased risk for malignancy, heart disease and ischemic stroke. CHIP is driven...
3.
Clonality in haematopoietic stem cell ageing
Terradas-Terradas M, Robertson N, Chandra T, Kirschner K
Mech Ageing Dev . 2020 Jun; 189:111279. PMID: 32526214
Clonal haematopoiesis of indeterminate potential (CHIP) is widespread in the elderly. CHIP is driven by somatic mutations in leukaemia driver genes, such as Janus Kinase 2 (JAK2), Tet methylcytosine dioxygenase...
4.
Age-related clonal haemopoiesis is associated with increased epigenetic age
Robertson N, Hillary R, McCartney D, Terradas-Terradas M, Higham J, Sproul D, et al.
Curr Biol . 2019 Aug; 29(16):R786-R787. PMID: 31430471
Age-related clonal haemopoiesis (ARCH) in healthy individuals was initially observed through an increased skewing in X-chromosome inactivation [1]. More recently, several groups reported that ARCH is driven by somatic mutations...