EOM Pharmaceutical Holdings Announces Topline Results of Its COVID-19 Clinical Trial of EOM613 in Brazil
EOM Pharmaceutical Holdings Announces Topline Results of Its COVID-19 Clinical Trial of EOM613 in Brazil
Results indicate that EOM613 treatment mitigates cytokine release in patients with COVID-19 pulmonary vascular inflammation
結果表明,EOM613治療可減輕新冠肺炎肺血管炎症患者細胞因數的釋放
MONTVALE, N.J., Sept. 6, 2023 /PRNewswire/ -- EOM Pharmaceutical Holdings, Inc (OTC: IMUC) ("EOM") today announced the results of its completed clinical trial in hospitalized COVID-19 patients with severe symptoms treated with its investigational immune-regulating drug product EOM613. The trial was conducted in Brazil.
新澤西州蒙特維爾,9月2023年6月美通社/--Eom製藥控股公司美國場外交易市場代碼:IMUC)(以下簡稱“EOM”)今天宣佈了其研究用免疫調節藥物產品EOM613治療新冠肺炎嚴重症狀住院患者的已完成臨床試驗結果。這項試驗是在巴西。
This exploratory Phase 1/2a clinical trial (NCT05212532), designated RESCUE, was a proof-of-concept, open-label study evaluating the safety, tolerability, and preliminary efficacy measures, such as the effects on serum cytokines, when EOM613 was added to the standard-of-care therapy. The trial included two cohorts of patients hospitalized for COVID-19: one cohort was in the intensive care unit (ICU) and the other cohort was not (non-ICU). The study was conducted at four different medical centers in the Brazilian states of Sao Paolo and Goaia.
這項名為RESAVE的探索性1/2a期臨床試驗(NCT05212532)是一項概念驗證、開放標籤研究,評估了將EOM613添加到標準治療中時的安全性、耐受性和初步療效措施,如對血清細胞因數的影響。試驗包括兩組因新冠肺炎住院的患者:一組在重症監護病房(ICU),另一組不在(非ICU)。這項研究是在巴西聖保羅州和戈亞州的四個不同的醫療中心進行的。
The trial was originally designed to enroll a total of 40 patients – 20 in each cohort. The trial was redesigned, however, due to challenges in patient enrollment during the COVID-19 pandemic as a result of Brazil's successful vaccination program which led to a reduction in eligible hospitalized patients. The redesigned trial enrolled a total of 23 patients eligible for evaluation. The study's Principal Investigator was Florentino Cardoso Filho, MD, at the Casa de Saude Hospital in Campinas, Sao Paolo, and former President of the Brazilian Medical Association.
這項試驗最初的設計是招募總共40名患者-每個隊列20名。然而,由於新冠肺炎大流行期間患者招募方面的挑戰,該試驗被重新設計巴西的成功的疫苗接種計劃,導致符合條件的住院患者減少。重新設計的試驗共招募了23名符合評估條件的患者。這項研究的主要調查者是弗洛倫蒂諾·卡多佐·菲略醫學博士,聖保羅坎皮納斯的卡薩德·索德醫院的醫學博士,前巴西醫學會的總裁。
Topline Results
背線結果
The study's topline results indicate that:
該研究的主要結果表明:
- EOM613, administered by subcutaneous (SC) injection was well-tolerated by hospitalized COVID-19 patients.
- EOM613 treatment produced a reduction in certain pro-inflammatory serum cytokine levels in line with its postulated mechanism of action of immune modulation.
- The non-ICU cohort was comprised of patients hospitalized for COVID-19 receiving supplemental oxygen therapy by mask or nasal prongs, corresponding to degrees 4-5 of the WHO Ordinal Clinical Scale for Disease Severity (WHO-OSDS). The ICU cohort was comprised of patients hospitalized for COVID-19 under mechanical ventilation in an ICU, corresponding to degrees 6 or 7 of WHO-OSDS.
- Both cohorts received the standard-of-care therapy for COVID-19 as defined by the participating hospitals, with the addition of any medications necessary for the study participant's special needs, such as diabetes, hypertension, etc., but excluding other experimental drugs and any drugs used off-label.
- Of the total of 23 patients enrolled in the study, 5 patients were in the non-ICU cohort and 18 patients with severe respiratory inflammation symptoms requiring mechanical ventilation support were in the ICU cohort. For the non-ICU patients, EOM613 was administered SC at a dose of 2 mL once daily (QD) for 10 days, for a total of 20 mL. The ICU cohort received EOM613 SC at a dose of 2 mL twice daily (BID) for 5 days followed by 2 mL once daily (QD) for 5 days, for a total of 30 mL. All patients were followed for 28 days. A clinical data evaluation was made of the evolution of WHO-OSDS, and laboratory exams and adverse events were compared with historic controls treated for COVID-19 at the same hospitals.
- The results of the trial indicate that, EOM613 administered SC at a dose level of 2 mL QD for 10 days was well tolerated in COVID-19 non-ICU patients. Study drug was discontinued for only one enrolled patient in the ICU cohort after the first day of treatment due to hemodynamic worsening (Grade 4). In ICU patients receiving a dose level of 2 mL BID for 5 days followed by 2 mL QD for 5 days, a somewhat higher frequency of adverse events (AEs) of the cardiovascular system was observed than in the non-ICU cohort as would be expected with mechanically ventilated patients, but these AEs were not deemed related to EOM613 treatment by the clinical investigators. Both treatment group regimens had no negative effect on clinical laboratory parameters (complete blood count, SMA-18 metabolic panel, biochemistry) of patients with COVID-19 infection.
- Post-baseline clinically significant beneficial changes were seen with EOM613 treatment for two of the blood serum cytokines involved in the cytokine storm in hospitalized COVID-19 patients, namely, soluble interleukin-2 receptor (sIL-2R) and interleukin-10 (IL-10). In the seriously affected ICU cohort, changes were also observed in other cytokines, such as TNF-α, IL-1β, IL-6 and IL-13, in line with EOM613's mechanism of action as a broad-spectrum immune regulator.
- For example, at screening levels of sIL-2R cytokine were meaningfully higher in the ICU cohort patients with mean values of 1721.69 (± 720.31) pg/mL (median1602.30 pg/mL). sIL-2R levels decreased during the study in both study cohorts. A statistically significant change from baseline was observed on Day 8 in the ICU cohort, i.e., a drop of -512.15 (± 698.10), median -412.80 (p = 0.0214). Similarly, in the non-ICU cohort the mean baseline value at screening on Day 28 showed mean IL-2R levels were 588.55 (± 537.76) pg/mL (median 484.60) in the non-ICU cohort and 726.96 (± 331.70) pg/mL (median 861.50) in the ICU cohort. Median changes from baseline in sIL2-R were -485.35 pg/mL and -444.90 pg/mL, respectively.
- 住院新冠肺炎患者對皮下注射EOM613耐受性良好。
- EOM613治療可降低某些促炎血清細胞因數水準,這與其免疫調節作用機制相一致。
- 非重症監護病房隊列包括因新冠肺炎而住院的患者,他們通過面罩或鼻尖接受補充氧療,對應於世衛組織疾病嚴重程度臨床序貫量表(WHO-OSDs)的4-5級。重症監護病房隊列包括在重症監護病房機械通氣下因新冠肺炎住院的患者,相當於世衛組織OSDS6級或7級。
- 兩個隊列都接受了參與醫院定義的新冠肺炎標準治療,添加了研究參與者特殊需要所需的任何藥物,如糖尿病、高血壓等,但不包括其他實驗藥物和任何標籤外使用的藥物。
- 在總共登記參加研究的23名患者中,5名患者在非ICU隊列中,18名患有嚴重呼吸道炎症癥狀需要機械通氣的患者在ICU隊列中。對於非ICU患者,EOM613口服SC,每日2毫升,每日1次,療程10天,共20毫升。ICU組給予EOM613SC 2mL2次/d,連服5d,後2mL1次/d,連服5d,共30mL。所有患者均隨訪28天。對WHO-OSD的演變進行臨床資料評估,並將實驗室檢查和不良事件與同一醫院接受新冠肺炎治療的歷史對照進行比較。
- 試驗結果表明,新冠肺炎非ICU患者對EOM613 SC的耐受性良好,劑量為2mLqd,連用10天。由於血流動力學惡化(4級),ICU隊列中只有一名入選患者在治療第一天後停用了研究藥物。在ICU患者中,接受2mLBid的劑量水準為5天,然後2mLqd為5天,觀察到心血管系統不良事件(AEs)的頻率略高於非ICU隊列中的機械通氣患者,但臨床研究人員認為這些AEs與EOM613的治療無關。兩組治療方案對新冠肺炎感染患者的臨床實驗室指標(全血細胞計數、SMA-18代謝板、生化)均無不良影響。
- 治療後,新冠肺炎患者血清中參與細胞因數風暴的兩種細胞因數,即可溶性白介素2受體(sIL-2R)和白介素10(IL-10)在基線後發生了顯著的臨床有益變化。在受影響嚴重的ICU隊列中,還觀察到了其他細胞因數的變化,如腫瘤壞死因數-α、IL-1β、IL-6和IL-13,符合EOM613的S作為廣譜免疫調節劑的作用機制。
- 例如,在篩查時,ICU隊列患者的sIL-2R細胞因數水準顯著較高,平均值為1721.69(±720.31)pg/mL(中位數1602.30 pg/ml)。在這兩個研究隊列中,sIL-2R水準在研究期間都有所下降。在重症監護病房隊列中,第8天觀察到與基線相比有統計學意義的變化,即-512.15(±698.10),中位數-412.80(p=0.0214)。同樣,在非ICU隊列中,第28天篩查時的平均基線值顯示,非ICU隊列的平均IL-2R水準為588.55(±537.76)pg/mL(中位數484.60),ICU隊列中的平均IL-2R水準為726.96(±331.70)pg/mL(中位數861.50)。SIL-2-R較基線變化的中位數分別為-485.35 pg/m L和-444.90 pg/m L。
Shalom Z. Hirschman, MD, Chief Medical Officer of EOM Pharmaceuticals, stated: "I am encouraged by the results of this trial indicating that EOM613 was well-tolerated even in this group of seriously affected hospitalized COVID-19 patients, as it had earlier been shown to be trials in patients with AIDS, cancer cachexia and rheumatoid arthritis. Furthermore, I am pleased that the serum cytokine measurements in COVID-19 patients validate the putative mechanism of action of EOM613 as a broad-spectrum immunomodulating agent affecting pro- and anti-inflammatory cytokine levels, as these results are consistent with previous results in cell culture in immune cells. Both sIL-2R and IL-10 cytokines have been implicated in the scientific literature as biomarkers for the progression of severe COVID-19 infection, with elevated levels of sIL-2R in particular being a predictor of hospital mortality. Thus, an agent that can be shown to diminish serum levels of this cytokine may prove beneficial. Cytokines such as sIL-2R are also associated in various other chronic inflammatory conditions such as rheumatoid arthritis in which enhanced T-cell activation is involved."
夏洛姆·Z·赫希曼EOM製藥公司首席醫療官,MD說:“這項試驗的結果表明,即使在這群嚴重感染住院的新冠肺炎患者中,EOM 613的耐受性也很好,這讓我感到鼓舞,因為它早些時候被證明是用於艾滋病、癌症惡病質和類風濕性關節炎患者的試驗。此外,我很高興新冠肺炎患者的血清細胞因數測量證實了EOM 613作為影響促炎和抗炎細胞因數水準的廣譜免疫調節劑的假定作用機制,因為這些結果與先前免疫細胞細胞培養的結果一致。在科學文獻中,sIL-2R和IL-10細胞因數都被認為是嚴重新冠肺炎感染進展的生物標誌物,特別是sIL-2R水準升高是醫院死亡率的預測因數。因此,一種可以降低血清中這種細胞因數水準的藥物可能會被證明是有益的。細胞因數,如sIL-2R,也與各種其他慢性炎症性疾病有關,如類風濕性關節炎,其中涉及T細胞的增強激活。
"The results of this trial further elucidate EOM613's mechanism of action in patients, thus corroborating the earlier preclinical lab research, and suggesting broader potential utility. This provides an additional support for EOM's future clinical drug development in various chronic inflammatory diseases," added Irach B. Taraporewala, PhD, CEO of EOM Pharmaceuticals. "A well-tolerated broad-spectrum immune regulating agent such as EOM613 which can modulate multiple cytokines involved in disease pathogenesis could have meaningful therapeutic value. We look forward to conducting additional investigation of EOM613's potential utility."
EOM製藥公司首席執行官伊拉赫·B·塔拉波雷瓦拉補充說:“這項試驗的結果進一步闡明瞭EOM 613在患者中的作用機制,從而證實了早期的臨床前實驗室研究,並提出了更廣泛的潛在用途。這為EOM未來治療各種慢性炎症性疾病的臨床藥物開發提供了額外的支持。”“一種耐受性良好的廣譜免疫調節劑,如EOM613,可以調節參與疾病發病機制的多種細胞因數,可能具有有意義的治療價值。我們期待著對EOM613的S潛在用途進行進一步的研究。”
About EOM613
關於EOM613
EOM's lead asset, EOM613, is an investigational, novel peptide-nucleic acid solution immunomodulator believed to have both anti- and pro-inflammatory broad-spectrum cytokine effects. In human cell culture studies, EOM613 demonstrated a unique "dynamic dual action" by suppressing or stimulating monocytes and macrophages depending on the activation state and environment of those key immune cells. It is hypothesized that this dynamic dual-action may overcome a limitation of many approved immunomodulators that only reduce the inflammatory state without achieving immune system balance
EOM的主要資產EOM613是一種研究中的新型多肽-核酸溶液免疫調節劑,據信具有抗炎和促炎廣譜細胞因數作用。在人類細胞培養研究中,EOM613根據關鍵免疫細胞的激活狀態和環境,通過抑制或刺激單核細胞和巨噬細胞,展示了一種獨特的“動態雙重作用”。據推測,這種動態的雙重作用可以克服許多已批准的免疫調節劑的侷限性,這些免疫調節劑只減少炎症狀態,而不實現免疫系統平衡
About EOM Pharmaceutical Holdings, Inc.
EOM製藥公司簡介 控股公司。
EOM Pharmaceutical Holdings, Inc. is a clinical-stage company focused on developing novel drugs with the potential to transform therapeutic paradigms and improve quality of life in patients suffering from debilitating and sometimes deadly diseases. The Company was founded with a specific vision to pursue innovative approaches to rescue, repair, and restore health of patients with urgent and unmet medical needs. For more information about EOM Pharmaceuticals, please visit .
Eom製藥控股公司是一家臨床階段的公司,專注於開發有潛力改變治療模式並改善患有衰弱甚至有時致命疾病的患者的生活品質的新藥。該公司的成立具有明確的願景,以追求創新的方法來拯救、修復和恢復有緊急和未得到滿足的醫療需求的患者的健康。欲瞭解更多有關EOM製藥公司的資訊,請訪問網站。
Forward Looking Statements
前瞻性陳述
This press release contains forward-looking statements within the meaning of Section 27A of the Securities Act of 1933, as amended, and Section 21E of the Securities Exchange Act of 1934, as amended. In some cases, you can identify these statements by forward-looking words such as "may," "will," "continue," "anticipate," "intend," "could," "project," "expect" or the negative or plural of these words or similar expressions, and other similar terms. Forward-looking statements are not guarantees of future performance and are subject to risks and uncertainties that could cause actual results and events to differ materially from those anticipated, including, but not limited to, EOM's ability to develop and commercialize its product candidates; EOM's ability to obtain and maintain regulatory approval of product candidates; EOM's ability to operate in a competitive industry and compete successfully against competitors that have greater resources; EOM's reliance on third parties; EOM's ability to obtain and adequately protect intellectual property rights for product candidates; and the effects of COVID-19 on clinical programs and EOM's business operations. Any forward-looking statements in this press release speak only as of the date of this press release. EOM assumes no obligation to update forward-looking statements whether as a result of new information, future events or otherwise, after the date of this press release.
本新聞稿包含符合修訂後的1933年證券法第27A節和修訂後的1934年證券交易法第21E節的前瞻性陳述。在某些情況下,您可以通過“可能”、“將會”、“繼續”、“預期”、“打算”、“可能”、“專案”、“預期”或這些詞的否定或複數或類似表達以及其他類似術語來識別這些陳述。前瞻性聲明受風險和不確定性因素的影響,可能會導致實際結果和事件與預期的結果和事件大不相同。這些風險和不確定性包括但不限於:EOM對候選產品進行開發和商業化的能力;EOM獲得並保持對候選產品的監管批准的能力;EOM在競爭激烈的行業中運營並與擁有更多資源的競爭對手成功競爭的能力;EOM對第三方的依賴;EOM獲取並充分保護候選產品知識產權的能力;以及新冠肺炎對EOM臨床專案和EOM業務運營的影響。本新聞稿中的任何前瞻性陳述僅限於本新聞稿發佈之日。EOM沒有義務在本新聞稿發佈之日之後更新前瞻性陳述,無論是由於新資訊、未來事件還是其他原因。
SOURCE EOM Pharmaceutical Holdings
來源:EOM製藥控股
譯文內容由第三人軟體翻譯。