December 2024:

SABC funds and co-leads a research study that began recruiting scleroderma patients with and without interstitial lung disease (ILD) in July 2017.  Blood samples have also been taken from patients with idiopathic pulmonary fibrosis (IPF) and undifferentiated connective tissue disease (UCTD) and both blood and skin samples have been taken from control participants. This research program is creating a firm foundation for intensive research to control lung and skin damage in patients with scleroderma and lung damage in patients with IPF, with the expectation of receiving future support from donations and, hopefully, research funding agencies.  While the number of voluntary participants with UCTD are few at this time, it is expected that these patients will be helped too.

Hello from the Research Team: Ms. Raveen Badyal continues her MSc thesis research in scleroderma and Mr. Brandon Kohlen started his MSc thesis research in scleroderma in September 2024.  Both are being supervised at UBC by Drs. Tillie-Louise Hackett and James Dunne. Under the joint supervision of Dr. Amrit Singh of the Computational Biology Lab (CBL) and Dr. James Dunne, postgraduate fellow Dr. Young Woong Kim is continuing to telecommute out of Edmonton and working on a half-time basis on the metabolite analysis, for which the lab work was done in Edmonton by The Metabolomics Innovation Centre (TIMC) at the University of Alberta.  Ms. Gaea Buenaventura is continuing to work on a part-time basis to help out in the laboratory.

Follow @SABCResearch on X (formerly known as Twitter) and Facebook or Instagram for progress and development updates. These social media handles were created in October 2020 and have been providing communication on this SABC Research Program since.

Congratulations to the SABC Research Program team.

Their current research has been published in the journal Scientific Reports. The article “Circulating cytokine levels in systemic sclerosis related interstitial lung disease and idiopathic pulmonary fibrosis” is available at Publication #1. A simplified version is included below.

The journal Scientific Reports on 24 April 2023 published an article by The SABC Research Program on a study of the differences in certain proteins called cytokines in people with either systemic scleroderma or interstitial lung disease, or both. The levels of 87 cytokines in blood plasma were compared with those of healthy individuals.  No substantial association was found for any of the cytokines with changes in lung capacity over time, but four cytokines were found to be markedly different in patients compared to healthy individuals. One cytokine associated with ageing was increased two-fold in all patient groups. Another cytokine associated with tissue inflammation was increased eight-fold but only in patients with interstitial lung disease and was not increased in healthy individuals or patients with scleroderma but no lung involvement. A third cytokine associated with blood clotting was decreased in all patient groups compared to healthy individuals. Another cytokine was increased two-fold only in patients with the limited cutaneous form of scleroderma compared to healthy individuals. This fourth cytokine is associated with immune-cell migration into tissue and the promotion of fibrosis and may be a marker of milder forms of scleroderma. These results suggest there may be common and different reasons why people develop pulmonary fibrosis.  Further research is needed.  This study was funded by the Scleroderma Association of B.C. Scientific Reports is published by Springer Nature.

The aim of the SABC Genome Research Program is to identify biomarkers specific to people who have pulmonary fibrosis caused by systemic sclerosis (scleroderma).   Being able to distinguish between pulmonary fibrosis that is idiopathic (of various or unknown origin) or the result of scleroderma will allow medical professionals to provide patients with an accurate diagnosis. Identifying reliable biomarkers also provides an opportunity to develop a functional cure; an ongoing treatment that corrects and prevents the disease from continuing to damage the affected organs (in this case, lungs).

This proof-of-concept study is to discover miRNA sequences and their impact on biochemical processes at the cellular level with the goal of targeted therapeutic interventions to correct the disturbed cycle of regeneration in heart, lung, and skin tissues in scleroderma and lung tissue in IPF.  This study is important for the approximately 15,604 Canadians with scleroderma and the approximately 7,045 Canadians with IPF (as confirmed by CT, biopsy, or bronchoscopy). Discovering which miRNA sequences are too low or too high and correcting these imbalances could lead to effective treatment of skin damage in patients with scleroderma and treatment of lung damage in patients with IPF only and in patients with both scleroderma and ILD.

SABC has been behind this program since 2017. Your donations do make a difference in contributing to research that otherwise would not even be considered for funding for these two orphan diseases.

The research team brings together experts in respirology, rheumatology, bioinformatics, and genetical statistics to uniquely tackle this challenge.  The team is led by SABC President Rosanne Queen, Beth Miller, Drs. James Dunne and Kevin Keen.  Drs. Chris Ryerson and Pearce Wilcox round out the scientific research team.  Both Rosanne and Beth participate on the leadership team to keep us informed on the progress of this SABC-funded research program and to ensure the interests of patients and their families are at the forefront.