Systemic Sclerosis Pathogenesis and Emerging Therapies, beyond the Fibroblast

Sierra-Sepúlveda, Andrea; Esquinca-González, Alexia; Suárez, Sergio Adán Benavides; Sordo-Lima, Diego E.; Caballero-Islas, Adrián E.; Cabral-Castañeda, Antonio; Rodríguez‐Reyna, Tatiana Sofía

doi:10.1155/2019/4569826

Cited by 66 publications

(72 citation statements)

References 104 publications

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“…Systemic sclerosis (SSc) is a rare autoimmune disease representing one of the most severe connective tissue pathologies, characterized by vascular obliteration, immunological abnormalities, and excessive extracellular matrix deposition, which causes fibrosis of the skin and of internal organs [1]. The etiopathogenesis of the disease is still unknown; possibly, multiple initial events may trigger the release of different cytokines by inflammatory cells, diffuse microangiopathy, fibroblast activation with abnormal collagen deposition, and subsequent ischemic and fibrotic manifestations [2].…”

Section: Introductionmentioning

confidence: 99%

HHV-6A Infection and Systemic Sclerosis: Clues of a Possible Association

et al. 2019

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Systemic sclerosis (SSc) is an autoimmune disease characterized by vasculopathy, excessive extracellular matrix deposition, and fibrosis of the skin and internal organs. Several infectious agents, including human herpesvirus-6 (HHV-6), have been suggested as possible triggering factors, but a direct association is still missing. We characterized 26 SSc patients for the presence of HHV-6 in tissues and blood, the anti-HHV-6 response, HLA-G plasma levels, and KIR typing. Given the prominent role of endothelial cells (EC) in SSc pathogenesis, along with HHV-6 tropism for EC, we also investigated the expression of pro-fibrosis factors in HHV-6 infected EC. Results showed the presence of HHV-6A in skin biopsies, and an increased virus load was associated with disease severity and poor natural killer (NK) response against the virus, particularly in subjects exhibiting a KIR2 phenotype. HLA-G plasma levels were significantly higher in HHV-6A/B-KIR2 positive SSc patients and in vitro HHV-6A infection-induced pro-fibrosis factors expression in EC, supporting its role in the development of the fibrosing process. Our data suggest an association between virus infection/reactivation and disease, opening the way to future studies to understand the mechanisms by which HHV-6A might contribute to the multifactorial pathogenesis of SSc.

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Section: Introductionmentioning

confidence: 99%

HHV-6A Infection and Systemic Sclerosis: Clues of a Possible Association

et al. 2019

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“…Furthermore, SSc patients had higher SCX levels than controls, particularly those in late stages of the disease, and with anti-topoisomerase I autoantibodies. As a systemic disease, in SSc, many factors have local and systemic effects on specific tissues that have been associated with severity and progression [44]. Circulating anti-topoisomerase I antibodies (Scl70) have been linked to diffuse disease and the presence and severity of interstitial lung diseases [45].…”

Section: Discussionmentioning

confidence: 99%

The Transcription Factor SCX is a Potential Serum Biomarker of Fibrotic Diseases

Ramírez-Aragón

Hernández-Sánchez

Rodríguez‐Reyna

et al. 2020

IJMS

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Fibrosing diseases are causes of morbidity and mortality around the world, and they are characterized by excessive extracellular matrix (ECM) accumulation. The bHLH transcription factor scleraxis (SCX) regulates the synthesis of ECM proteins in heart fibrosis. SCX expression was evaluated in lung fibroblasts and tissue derived from fibrotic disease patients and healthy controls. We also measured SCX in sera from 57 healthy controls, and 56 Idiopathic Pulmonary Fibrosis (IPF), 40 Hypersensitivity Pneumonitis (HP), and 100 Systemic Sclerosis (SSc) patients. We report high SCX expression in fibroblasts and tissue from IPF patients versus controls. High SCX-serum levels were observed in IPF (0.663 ± 0.559 ng/mL, p < 0.01) and SSc (0.611 ± 0.296 ng/mL, p < 0.001), versus controls (0.351 ± 0.207 ng/mL) and HP (0.323 ± 0.323 ng/mL). Serum levels of the SCX heterodimerization partner, TCF3, did not associate with fibrotic illness. IPF patients with severely affected respiratory capacities and late-stage SSc patients presenting anti-topoisomerase I antibodies and interstitial lung disease showed the highest SCX-serum levels. SCX gain-of-function induced the expression of alpha-smooth muscle actin (α-SMA/ACTA2) in fibroblasts when co-overexpressed with TCF3. As late and severe stages of the fibrotic processes correlated with high circulating SCX, we postulate it as a candidate biomarker of fibrosis and a potential therapeutic target.

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“…В последние годы достигнут определенный прогресс в понимании патогенеза ССД. Если ранее считалось, что в основе заболевания лежат преимущественно фиброзирующие процессы, то в настоящее время доказано, что в его развитии принимают участие несколько механизмов, базирующихся на кооперации иммуно-воспалительных процессов, васкулопатии и фиброза [9,16] Относительно недавно, рядом исследований была выявлена потенциальная роль «окислительного стресса» в патогенезе ССД [11,17]. Было обнаружено, что уровни циркулирующих биомаркеров (малоновый диальдегид, липопротеины низкой плотности, изопростаны, тиолы) активных форм кислорода (АФК), коррелируют с васкулопатией, фиброзом и продукцией аутоантител при ССД [5,8].…”

Section: введение/цельunclassified

Enzymatic Profile of Blood Plasma in Systemic Sclerosis: Activity of Xanthine Oxidase, Xanthine Dehydrogenase and Superoxide Dismutase

Bedina¹,

Mozgovaya²,

Trofimenko³

et al. 2019

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Systemic Sclerosis Pathogenesis and Emerging Therapies, beyond the Fibroblast

Cited by 66 publications

References 104 publications

HHV-6A Infection and Systemic Sclerosis: Clues of a Possible Association

HHV-6A Infection and Systemic Sclerosis: Clues of a Possible Association

The Transcription Factor SCX is a Potential Serum Biomarker of Fibrotic Diseases

Enzymatic Profile of Blood Plasma in Systemic Sclerosis: Activity of Xanthine Oxidase, Xanthine Dehydrogenase and Superoxide Dismutase

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