All study objectives were met, demonstrating safety across dose groups and confirming efficacy and durability at the selected doses against placebo (lidocaine) and active control (steroid).
All RTX doses (7.5 to 20 μg) were well-tolerated, with few severe or serious adverse events (AEs). The majority of reported AEs related to pain post-administration and resolved within hours following treatment. Very few severe AEs were reported across groups (including placebo) with no dose correlation. RTX post-injection administration pain was easily controlled.
RTX 20mcg dose outperformed all other dose groups (including the approved drug for this indication (intra-articular corticosteroids)) for efficacy and durability at and beyond 26 weeks post-treatment. RTX 20mcg and 12.5mcg have been selected as the clinically optimal and minimally effective doses for further phase 2 pivotal or phase 3 trials.
SAN DIEGO, Sept. 07, 2023 (GLOBE NEWSWIRE) -- Sorrento Therapeutics, Inc. (OTC: SRNEQ, "Sorrento") announced today positive Phase 2a top-line clinical trial results for the RTX program.
The Phase 2a study follows the positive observations from the Phase 1b/2 trial results (NCT03542838) of RTX Day 84 patient data, for which Sorrento has completed the one-year follow up for the last patient dosed in February 2021.
The phase 2 trial, a multi-center, double blind, placebo- and active-controlled study, assessed the efficacy and safety of several dose groups of RTX to manage pain in patients with moderate-to-severe OAK (clinicaltrials.gov: NCT04885972). Given the durability of OAK pain relief response to RTX demonstrated in earlier phase 1b/2 trials, Sorrento decided to include an active approved comparator (Zilretta intra-articular corticosteroids) in the current trial protocol.
Top-Line Safety Outcomes (Summary)
Generally, treatment was well-tolerated, with the most common noted AE being pain following topical capsaicin 0.1% given to all patients for blinding purposes and study drug administration in the knee (across all dose groups).
Very few serious AEs were noted across all dose groups, with one in particular (see below for additional detail) in the 15mcg RTX group being severe/life threatening (hypertension following drug administration), which resolved within hours with treatment of pain and no additional intervention.
In the cases requiring pain control (any group) the dose of opioid was comparable. A few subjects in RTX groups required use of low dose oral opioids for up to 6 hours in some cases of prolonged moderate discomfort/pain. No patient required additional pain control or intervention after 6 hours or in the days following the day of administration and no patient left the clinic with opioids or an opioid prescription.
A table accompanying this announcement is available at
Subject 008-005, a 55-year-old female with a prior history of hypertension (HTN) and morbid obesity (BMI 46.9) developed elevated blood pressure about fourteen minutes post-RTX dose (208/147), which coincided with severe pain. The subject received hydromorphone 0.8 and 0.4 mg IV and then oxycodone 5 mg twice, and the HTN resolved without any other intervention. The HTN did not recur, and the subject's ECG was normal. Discharge blood pressure was 140/74. Sponsor's medical monitor disagreed with the characterization as life-threatening or an SAE as the clinic stay was not prolonged and the HTN required no treatment other than treating the subject's pain. Sponsor also felt that the AE should have been considered a related event (marked unrelated by investigator).
Top Line Efficacy and Durability Outcomes (Summary)
The RTX 20mcg dose group performed best among all dose groups, including placebo (lidocaine only) and approved intra-articular corticosteroid (Zilretta) on short-term and prolonged pain relief measures (SPID, KOOS, WOMAC).
Summary of Pain Intensity Difference (SPID)
Although at many time points, RTX 20mcg was statistically significant as compared to the approved drug (Zilretta) in this indication active control, we note that the study was not powered to demonstrate statistical significance for all end points listed (primary, secondary), with only 120 patients enrolled across 5 RTX dose groups and early terminations due to the Company's previously announced bankruptcy proceedings.
Despite the limitations of the study (small number of patients per group, high variability of placebo responders due to intra-articular use of 10ml lidocaine and capsaicin cream for blinding per FDA request), the results = demonstrate that RTX 20mcg is an effective pain treatment for longer durations (up to one year), with better score improvements at week 26 and 52 than the current standard of care (active steroid injection. Zilretta) up to and past week 26.
A higher proportion of patients responded to treatment with RTX 20mcg than any other treatment group, including Zilretta. Reduction in pain was also more pronounced with RTX 20mcg than with any other treatment group, including placebo and active control.
A table accompanying this announcement is available at
Durability of treatment was nearly twice as long for RTX 20mcg than active steroid control (mean time to return to 10% of baseline of 19 weeks for RTX versus 10 weeks for Zilretta).
In conclusion, we report that the phase 2a OAK study for RTX has met all the primary and secondary objectives for the study. The Phase 2a results were consistent with the prior safety profile of the drug from the previously completed Phase 1 study and has allowed for the potential determination of a therapeutically effective dose for further phase 2 pivotal or phase 3 studies, which is expected to be powered with a sufficient number of patients to provide significantly different results from the controls.
"We are extremely pleased with the outcome of this study. The clinical trial confirmed the potential of resiniferatoxin (RTX) in helping patients with moderate to severe osteoarthritis pain for at least 6 months, if not longer. No other drug on the market can provide this much pain relief, for this long a period, from a single administration," stated Dr. Henry Ji, Chairman and Chief Executive Officer.
About RTX
A thousand times "hotter" than pure capsaicin (16 billion Scoville units versus 16 million), and with a high affinity for afferent sensory pain nerves, RTX binds to TRPV1 receptors present and selectively ablates the nerve endings responsible for pain signals experienced by patients1. Delivered peripherally (into the joint space) the transient nerve ending ablation effect can have profound clinical benefits lasting for months to years (as shown in canine studies2).
The first arthritis pain clinical trial in humans was completed in 2021. That study was a multicenter, placebo-controlled Phase 1b/2 study to assess the safety and define the maximally tolerated dose of RTX administered in the knee joint in patients with moderate to severe pain associated with osteoarthritis of the knee. The study was a dose-escalation trial in which cohorts of patients receive increasing doses of RTX until the maximum tolerated dose (MTD) was achieved. The primary objective of the study was to evaluate the safety of RTX and identify the recommended Phase 3 dose. The secondary objective was to assess the preliminary efficacy of RTX measured by assessing changes in the intensity of pain using the A1 score from the WOMAC, a widely used proprietary validated pain questionnaire.
The second arthritis pain phase 2a clinical trial in humans completed enrollment in September 2022. The results of study are expected to confirm the phase 3 doses and demonstrate long-term effectiveness of RTX in controlling osteoarthritis pain when compared to placebo or active steroid intra-articular injections.
Sorrento continues to progress as planned on all clinical fronts of the RTX program, including exploring additional orphan indications with breakthrough potential.
RTX is an extremely potent compound used therapeutically in very small concentrations. It is very challenging to formulate and keep stable long-term when made in large quantities. Sorrento has been working on process optimization of RTX manufacturing for several years and continues to advance the validation and scale up, with the expectation to have final validated batches completed by the end of 2023. Ensuring the company can meet market demands from API to finished product once phase 3 trials have been completed has been identified as a critical priority, which Sorrento is currently addressing.
The osteoarthritis treatment market and in particular the Knee Osteoarthritis and injectable markets have historically seen healthy growth and are expected to continue the trend as populations age and present excessive weight.
About Sorrento Therapeutics, Inc.
Sorrento is a clinical and commercial stage biopharmaceutical company developing new therapies to treat cancer, pain (non-opioid treatments), autoimmune disease and COVID-19. Sorrento's multimodal, multipronged approach to fighting cancer is made possible by its extensive immuno-oncology platforms, including key assets such as next-generation tyrosine kinase inhibitors ("TKIs"), fully human antibodies ("G-MAB library"), immuno-cellular therapies ("DAR-T"), antibody-drug conjugates ("ADCs"), and oncolytic virus ("Seprehvec"). Sorrento is also developing potential antiviral therapies and vaccines against coronaviruses, including STI-1558, COVISHIELD and COVI-MSC; and diagnostic test solutions, including COVIMARK.
Sorrento's commitment to life-enhancing therapies for patients is also demonstrated by our effort to advance a TRPV1 agonist non-opioid pain management small molecule, resiniferatoxin ("RTX"), and SP-102 (10 mg, dexamethasone sodium phosphate viscous gel) (SEMDEXA), a novel, viscous gel formulation of a widely used corticosteroid for epidural injections to treat lumbosacral radicular pain, or sciatica, and to commercialize ZTlido (lidocaine topical system) 1.8% for the treatment of postherpetic neuralgia (PHN). RTX has been cleared for a Phase II trial for intractable pain associated with cancer and a Phase II trial in osteoarthritis patients. Positive final results from the Phase III Pivotal Trial C.L.E.A.R. Program for SEMDEXA, its novel, non-opioid product for the treatment of lumbosacral radicular pain (sciatica), were announced in March 2022. ZTlido was approved by the FDA on February 28, 2018.
所有研究目標均已實現,證明了各劑量組的安全性,並證實了選定劑量對抗安慰劑(利多卡因)和主動對照(類固醇)的療效和耐久性。
所有RTX劑量(7.5至20 μg)耐受性良好,幾乎沒有嚴重或嚴重的不良事件(AE)。報告的大多數不良事件與給藥後的疼痛有關,並在治療後數小時內消失。各組(包括安慰劑)報告的嚴重不良事件很少,沒有劑量相關性。RTX 注射後的疼痛很容易得到控制。
在治療後26周及以後的療效和耐久性方面,RTX 20mcg劑量優於所有其他劑量組(包括該適應症的批准藥物(關節內皮質類固醇))。RTX 20mcg和12.5mcg已被選爲進一步的2期關鍵或3期試驗的臨床最佳和最低有效劑量。
聖地亞哥,2023年9月7日(GLOBE NEWSWIRE)——Sorrento Therapeutics, Inc.(場外交易代碼:SRNEQ,“Sorrento”)今天宣佈了RTX計劃的2a期頂線臨床試驗結果爲積極性。
2a期研究遵循了RTX第84天患者數據的1b/2期試驗結果(NCT03542838)的積極觀察,索倫託已經完成了對2021年2月最後一位給藥患者的爲期一年的隨訪。
這項2期試驗是一項多中心、雙盲、安慰劑和主動對照研究,評估了幾組RTX在控制中度至重度OAK患者疼痛方面的有效性和安全性(clinicaltrials.gov:NCT04885972)。鑑於OAK對RTX的緩解疼痛反應在早期的1b/2期試驗中表現出的持久性,索倫託決定在當前的試驗方案中納入經批准的活性比較劑(Zilretta關節內皮質類固醇)。
主要安全成果(摘要)
總體而言,治療耐受性良好,最常見的AE是所有患者外用辣椒素0.1%後疼痛,用於致盲目的,並研究膝蓋中的藥物給藥(所有劑量組)。
在所有劑量組中,很少發現嚴重的不良事件,特別是15mcg RTX組中有一個(更多細節見下文)嚴重/危及生命(給藥後的高血壓),通過治療疼痛且沒有額外的干預,這種不良事件在數小時內就消失了。
在需要控制疼痛的病例(任何一組)中,阿片類藥物的劑量相當。在某些長期出現中度不適/疼痛的情況下,RTX組中的一些受試者需要使用低劑量口服阿片類藥物長達6小時。6小時後或給藥後的幾天內,沒有患者需要額外的疼痛控制或干預,也沒有患者帶着阿片類藥物或阿片類藥物處方離開診所。
本公告附帶的表格可在以下網址查閱
受試者008-005是一名既往有高血壓(HTN)和病態肥胖(BMI 46.9)史的55歲女性,在服用RTX劑量(208/147)大約十四分鐘後出現血壓升高,這與劇烈疼痛相吻合。受試者接受了0.8和0.4 mg的氫嗎啡酮靜脈注射,然後兩次接受羥考酮5 mg,HTN在沒有任何其他干預的情況下消失了。HTN 沒有復發,受試者的心電圖正常。出院血壓爲140/74。贊助商的醫療監護人不同意將其描述爲危及生命或SAE,因爲臨床停留時間沒有延長,HTN除了治療受試者的疼痛之外不需要任何治療。贊助商還認爲,AE本應被視爲相關事件(調查人員將其標記爲無關)。
主要功效和耐久性結果(摘要)
RTX 20mcg劑量組在所有劑量組中表現最好,包括安慰劑(僅限利多卡因)和經批准的短期和長期止痛措施(SPID、KOOS、WOMAC)的關節內皮質類固醇(Zilretta)。
疼痛強度差異摘要 (SPID)
儘管在許多時間點,與該適應症活性對照中的批准藥物(Zilretta)相比,RTX 20mcg具有統計學意義,但我們注意到,該研究並不能證明列出的所有終點(原發性、繼發性)的統計學意義,由於該公司先前宣佈的破產程序,只有120名患者入組了5個RTX劑量組,並且提前終止了治療。
儘管該研究存在侷限性(每組患者人數少,由於根據美國食品藥品管理局的要求在關節內使用10ml利多卡因和辣椒素乳膏進行失明,安慰劑反應者的差異性很大),但結果=表明,RTX 20mcg是一種有效的疼痛治療方法,持續時間更長(長達一年),在第26周和第52周的分數提高比目前的護理標準(主動注射類固醇)要好。Zilretta) 在第 26 周之前和過去一週。
對RTX 20mcg治療有反應的患者比例高於包括Zilretta在內的任何其他治療組。與包括安慰劑和主動對照組在內的任何其他治療組相比,使用RTX 20mcg的疼痛減輕也更爲明顯。
本公告附帶的表格可在以下網址查閱
RTX 20mcg的治療持續時間幾乎是主動類固醇對照組的兩倍(RTX恢復到基線的10%的平均時間爲19周,而Zilretta的平均恢復時間爲10周)。
總之,我們報告說,針對RTX的2a期OAK研究已滿足該研究的所有主要和次要目標。2a期結果與先前完成的1期研究中該藥物的先前安全性特徵一致,因此有可能確定進一步的2期關鍵或3期研究的治療有效劑量,預計該研究將有足夠數量的患者來提供與對照組明顯不同的結果。
“我們對這項研究的結果非常滿意。臨床試驗證實,樹脂菲拉毒素(RTX)有可能幫助患有中度至重度骨關節炎疼痛的患者至少6個月甚至更長時間。在這麼長的一段時間內,市場上沒有其他藥物能夠通過單一的管理來緩解疼痛。” 董事長兼首席執行官Henry Ji博士說。
關於 RTX
RTX 比純辣椒素 “熱” 一千倍(160 億個 Scoville 單位對 1600 萬個),並且對傳入感官疼痛神經具有很高的親和力,它與存在的 TRPV1 受體結合,有選擇地消滅導致患者出現疼痛信號的神經末梢1。短暫的神經末端消融作用在外周(進入關節空間)可以產生深遠的臨床益處,持續數月至數年(如犬類研究2所示)。
首項人體關節炎疼痛臨床試驗於2021年完成。該研究是一項多中心、安慰劑對照的1b/2期研究,旨在評估與膝關節骨關節炎相關的中度至重度疼痛患者在膝關節中施用RTX的安全性並確定其最大耐受劑量。該研究是一項劑量遞增試驗,在該試驗中,一組患者接受增加劑量的RTX,直到達到最大耐受劑量(MTD)。該研究的主要目的是評估RTX的安全性並確定推薦的3期劑量。次要目標是評估RTX的初步療效,方法是使用廣泛使用的專有經過驗證的疼痛問卷WOMAC的A1評分評估疼痛強度的變化。
第二項針對人類的關節炎疼痛2a期臨床試驗於2022年9月完成了入組。研究結果有望證實第三階段的劑量,並證明與安慰劑或活性類固醇關節內注射相比,RTX在控制骨關節炎疼痛方面的長期有效性。
索倫託繼續按計劃在RTX項目的所有臨床方面取得進展,包括探索其他具有突破潛力的孤兒適應症。
RTX 是一種極其有效的化合物,用於治療的濃度非常小。大量生產時,配方和長期保持穩定性非常困難。索倫託多年來一直致力於RTX製造的流程優化,並繼續推進驗證和擴大規模,預計將在2023年底之前完成最終的驗證批次。第三階段試驗完成後,確保公司能夠滿足從原料藥到成品的市場需求已被確定爲關鍵優先事項,索倫託目前正在解決這個問題。
骨關節炎治療市場,尤其是膝蓋骨關節炎和注射劑市場,歷來都出現了健康的增長,隨着人口老齡化和體重過重,預計這種趨勢將繼續下去。
關於索倫託 Therapeutics, Inc.
索倫託是一家臨床和商業階段的生物製藥公司,正在開發治療癌症、疼痛(非阿片類藥物治療)、自身免疫性疾病和 COVID-19 的新療法。索倫託的多模式、多管齊下的抗癌方法得益於其廣泛的免疫腫瘤學平台,包括下一代酪氨酸激酶抑制劑(“TKI”)、全人源抗體(“G-MAB庫”)、免疫細胞療法(“DAR-T”)、抗體藥物偶聯物(“ADC”)和溶瘤病毒(“Seprehly”)等關鍵資產 vec”)。索倫託還在開發針對冠狀病毒的潛在抗病毒療法和疫苗,包括 STI-1558、COVISHIELD 和 COVI-MSC;以及包括 COVIMARK 在內的診斷測試解決方案。
我們努力推進 TRPV1 激動劑非阿片類藥物疼痛管理小分子、樹脂菲拉毒素(“RTX”)和 SP-102(10 mg,地塞米松磷酸鈉粘稠凝膠)(SEMDEXA),這是一種廣泛用於硬膜外注射的皮質類固醇的新型粘性凝膠配方,用於治療硬膜外注射骶骨神經根性疼痛或坐骨神經痛,並將ztLido(利多卡因局部治療系統)1.8%用於治療帶狀皰疹後遺神經痛(PHN)。RTX已獲准進行一項針對癌症相關難治性疼痛的II期試驗和一項針對骨關節炎患者的II期試驗。用於治療腰骶神經根性疼痛(坐骨神經痛)的新型非阿片類藥物SEMDEXA的III期Pivotal試驗C.L.E.A.R. 項目於2022年3月宣佈了積極的最終結果。ztLido 於 2018 年 2 月 28 日獲得美國食品藥品管理局的批准。
