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Platelet factor 4 is a biomarker for lymphatic-promoted disorders
Indexado
WoS WOS:000568791800003
DOI 10.1172/JCI.INSIGHT.135109
Año 2020
Tipo artículo de investigación

Citas Totales

Autores Afiliación Chile

Instituciones Chile

% Participación
Internacional

Autores
Afiliación Extranjera

Instituciones
Extranjeras


Abstract



Genetic or acquired defects of the lymphatic vasculature often result in disfiguring, disabling, and, occasionally, life-threatening clinical consequences. Advanced forms of lymphedema are readily diagnosed clinically, but more subtle presentations often require invasive imaging or other technologies for a conclusive diagnosis. On the other hand, lipedema, a chronic lymphatic microvascular disease with pathological accumulation of subcutaneous adipose tissue, is often misdiagnosed as obesity or lymphedema; currently there are no biomarkers or imaging criteria available for a conclusive diagnosis. Recent evidence suggests that otherwise-asymptomatic defective lymphatic vasculature likely contributes to an array of other pathologies, including obesity, inflammatory bowel disease, and neurological disorders. Accordingly, identification of biomarkers of lymphatic malfunction will provide a valuable resource for the diagnosis and clinical differentiation of lymphedema, lipedema, obesity, and other potential lymphatic pathologies. In this paper, we profiled and compared blood plasma exosomes isolated from mouse models and from human subjects with and without symptomatic lymphatic pathologies. We identified platelet factor 4 (PF4/CXCL4) as a biomarker that could be used to diagnose lymphatic vasculature dysfunction. Furthermore, we determined that PF4 levels in circulating blood plasma exosomes were also elevated in patients with lipedema, supporting current claims arguing that at least some of the underlying attributes of this disease are also the consequence of lymphatic defects.

Revista



Revista ISSN
Jci Insight 2379-3708

Métricas Externas



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Disciplinas de Investigación



WOS
Medicine, Research & Experimental
Scopus
Medicine (All)
SciELO
Sin Disciplinas

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Publicaciones WoS (Ediciones: ISSHP, ISTP, AHCI, SSCI, SCI), Scopus, SciELO Chile.

Colaboración Institucional



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Autores - Afiliación



Ord. Autor Género Institución - País
1 Ma, Wanshu - NORTHWESTERN UNIV - Estados Unidos
2 Gil, Hyea Jin - NORTHWESTERN UNIV - Estados Unidos
St Jude Childrens Res Hosp - Estados Unidos
3 ESCOBEDO-MARAMBIO, NOELIA ANDREA Mujer NORTHWESTERN UNIV - Estados Unidos
Universidad Autónoma de Chile - Chile
4 Benito-Martin, Alberto Hombre Weill Cornell Med - Estados Unidos
5 Ximenez-Embun, Pilar Mujer Spanish Natl Canc Res Ctr - España
6 Munoz, Javier Hombre Spanish Natl Canc Res Ctr - España
7 Peinado, Hector Hombre Spanish Natl Canc Res Ctr - España
8 Rockson, Stanley G. Hombre Universidad de Stanford - Estados Unidos
Stanford Univ - Estados Unidos
9 Oliver, Guillermo Hombre NORTHWESTERN UNIV - Estados Unidos

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Financiamiento



Fuente
CONICYT/FONDECYT
NIH
European Union

Muestra la fuente de financiamiento declarada en la publicación.

Agradecimientos



Agradecimiento
This work was partially supported by the NIH (grant R01HL073402 to GO). WM was partially supported by NIH T32 HL134633 and NE by CONICYT/FONDECYT No 1204562. Additional support came from the European Union Horizon 2020 program INFRAIA project Epic-XS (project 823839) to HP.

Muestra la fuente de financiamiento declarada en la publicación.