AUTHOR=Gül Fethi , Gonen Zeynep Burcin , Jones Olcay Y. , Taşlı Neslihan Pakize , Zararsız Gökmen , Ünal Ekrem , Özdarendeli Aykut , Şahin Fikrettin , Eken Ahmet , Yılmaz Semih , Karakukçu Musa , Kırbaş Oğuz Kaan , Gökdemir Nur Seda , Bozkurt Batuhan Turhan , Özkul Yusuf , Oktay Burçin Doruk , Uygut Muhammet Ali , Cinel Ismail , Çetin Mustafa 

TITLE=A pilot study for treatment of severe COVID-19 pneumonia by aerosolized formulation of convalescent human immune plasma exosomes (ChipEXO™)

JOURNAL=Frontiers in Immunology

VOLUME=13

YEAR=2022

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2022.963309

DOI=10.3389/fimmu.2022.963309

ISSN=1664-3224

ABSTRACT=<p>This is a single-center prospective, open-label, single arm interventional study to test the safety and efficacy of recently described ChipEXO™ for severe COVID-19 pneumonia. The ChipEXO™ is a natural product derived from convalescent human immune plasma of patients recovered from moderate COVID-19 infection. In September 2021, 13 patients with pending respiratory failure were treated with ChipEXO™ adapted for aerosolized formulation delivered <italic>via</italic> jet nebulizer. Patients received 1-5x10<sup>10</sup> nano vesicle/5 mL in distilled water twice daily for five days as an add-on to ongoing conventional COVID-19 treatment. The primary endpoint was patient safety and survival over a 28-day follow-up. The secondary endpoint was longitudinal assessment of clinical parameters following ChipEXO™ to evaluate treatment response and gain insights into the pharmacodynamics. ChipEXO™ was tolerated well without any allergic reaction or acute toxicity. The survival rate was 84.6% and 11 out of 13 recovered without any sequel to lungs or other organs. ChipEXO™ treatment was effective immediately as shown in arterial blood gas analyses before and two hours after exosome inhalation. During the 5 days of treatment, there was a sustainable and gradual improvement on oxygenation parameters: i.e. respiratory rate (RR) [20.8% (P &lt; 0.05)], oxygen saturation (SpO<sub>2</sub>) [6,7% (P &lt; 0.05)] and partial pressure of oxygen to the fraction of inspired oxygen (PaO<sub>2</sub>/FiO<sub>2</sub>) [127.9% (P &lt; 0.05)] that correlated with steep decrease in the disease activity scores and inflammatory markers, i.e. the sequential organ failure assessment (SOFA) score (75%, p &lt; 0.05), C-reactive protein (46% p &lt; 0.05), ferritin (58% p = 0.53), D-dimer (28% p=0.46). In conclusion, aerosolized ChipEXO™ showed promising safety and efficacy for life-threatening COVID-19 pneumonia. Further studies on larger patient populations are required to confirm our findings and understand the pathophysiology of improvement toward a new therapeutic agent for the treatment of severe COVID-19 pneumonia.</p>