Severe Pneumonia Clinical Trial
Official title:
A Singlecenter, Randomized, Open Lable, Intervention Controlled Clinical Study on the Efficacy and Safety of Umbilical Cord Mesenchymal Stem Cells for the Treatment of Severe Viral Pneumonia
The purpose of this clinical study is to answer the questions:
1. Is the proposed intervention safe?
2. Is the proposed intervention effective in improving the health of subjects with severe
viral pneumonia?
Viral pneumonia is an acute respiratory infectious disease caused by respiratory viruses. It
is mainly caused by the invasion of respiratory viruses such as influenza virus and
adenovirus into the lower respiratory tract. Every winter and spring is the epidemic season.
Influenza virus and adenovirus have high infectivity and pathogenicity. The rapid progress of
some patients may be caused by acute respiratory distress syndrome (ARDS) or multiple organ
dysfunction And died of complications. The fatality rate of severe patients is 9.8% - 60%.
Most of the dead cases were the elderly and the patients with basic diseases. In addition to
the complications, the main cause of death is ARDS caused by virus infection, on the other
hand, the basic immune function of the elderly is poor, so it is difficult to form an
effective antiviral response in response to virus infection. The direct destruction of the
alveolar epithelial barrier and the systemic inflammatory response induced by the infection,
namely, the destruction of the alveolar capillary barrier by the inflammatory waterfall, are
the important pathogenesis of ARDS. How to effectively regulate the inflammatory response,
prevent the inflammatory exudation and edema of the lungs, improve oxygenation, and reduce
organ damage; at the same time, how to effectively improve the basic immune function and
enhance the anti-virus immune response of such patients, has become the key to the success of
the treatment of patients with severe viral pneumonia.
Umbilical cord mesenchymal stem cells (UC-MSCs) can differentiate into the different germ
layers and play an important role in immune regulation and damage repair regulation. Clinical
trials have shown that MSC is safe and effective in the treatment of acute lung injury and
pulmonary fibrosis, and it can improve the immune function of patients with viral infectious
diseases. Hence, intravenous infusion of HUC-MSCs is attractive therapy against severe viral
pneumonia.
This is a randomized, singlecenter, open lable, intervention controlled clinical trial. The
participants (n = 40) will be randomly distributed into two groups. The routine treatment
group (n = 20) will receive the treatment according to "Influenza diagnosis and treatment
plan (2019 version)", the HUC-MSCs adjuvant Group (n = 20) will receive intravenous infusion
of definitive HUC-MSCs (1×10^6 cells/Kg × body weight(kg), which was selected by
immunomodulatory assay through coculture with BV2 cell) on the basis of the routine treatment
once at day 1 after joining. Follow-up duration is 90 days. The difference of 90 day
mortality and average length of stay between the two groups will be observed and recorded.
The changes of inflammatory index, viral load, oxygenation index and pulmonary imaging will
be monitored at different time points after treatment in the two groups. The serious adverse
events (SAEs) and adverse events (AEs) will be observed during the period.
The intent of this study is to explore the efficacy of HUC-MSCs in the treatment of severe
viral pneumonia through improving the antiviral immune response of patients, reduce the lung
inflammatory damage caused by the virus and the pulmonary interstitial fibrosis after the
injury, and finally achieve the goal of reducing the mortality and improving the prognosis of
severe patients, and to evaluate the safety.
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