Latest DB-OTO Results Show Dramatically Improved Hearing to Normal Levels in a Child With Profound Genetic Deafness Within 24 Weeks and Initial Hearing Improvements in a Second Child at 6 Weeks
Latest DB-OTO Results Show Dramatically Improved Hearing to Normal Levels in a Child With Profound Genetic Deafness Within 24 Weeks and Initial Hearing Improvements in a Second Child at 6 Weeks
Preliminary data detailed in an ASGCT oral presentation include results for one of the youngest children in the world to receive a gene therapy for genetic deafness
ASGCT口頭陳述中詳述的初步數據包括世界上最小的兒童之一接受遺傳性耳聾基因療法的結果
Ongoing Phase 1/2 CHORD trial is currently enrolling infants and children in the U.S., UK and Spain
正在進行的 1/2 期 CHORD 試驗目前正在美國、英國和西班牙招收嬰兒和兒童
TARRYTOWN, N.Y., May 08, 2024 (GLOBE NEWSWIRE) -- Regeneron Pharmaceuticals, Inc. (NASDAQ: REGN) today announced that the investigational gene therapy DB-OTO improved hearing to normal levels in one child (dosed at 11 months of age) within 24 weeks, and initial hearing improvements were observed in a second child (dosed at 4 years of age) at a 6-week assessment. Both children were born with profound genetic deafness due to variants of the otoferlin gene, and the child dosed at 11 months of age is one of the youngest in the world to receive a gene therapy for genetic deafness. The results are from the ongoing Phase 1/2 CHORD trial, which is currently enrolling infants and children and were detailed during an oral presentation at the American Society of Gene and Cell Therapy (ASGCT) annual conference.
紐約州塔裏敦,2024年5月8日(環球新聞專線)——Regeneron Pharmicals, Inc.(納斯達克股票代碼:REGN)今天宣佈,研究性基因療法DB-OTO在24周內將一名兒童(11個月大給藥)的聽力提高到正常水平,在爲期6周的評估中,觀察到第二個孩子(4歲時給藥)的聽力初步改善。由於otoferlin基因的變異,這兩個孩子出生時都患有嚴重的遺傳性耳聾,而在11個月大時給藥的孩子是世界上接受遺傳性耳聾基因治療的最年輕的孩子之一。結果來自正在進行的1/2期CHORD試驗,該試驗目前正在招收嬰兒和兒童,並在美國基因與細胞療法學會(ASGCT)年會的口頭髮言中進行了詳細介紹。
"The opportunity of providing the full complexity and spectrum of sound in children born with profound genetic deafness is a phenomenon I did not expect to see in my lifetime," said Lawrence R. Lustig, M.D., Chair of Columbia University's Department of Otolaryngology - Head & Neck Surgery and a clinical trial investigator. "These impressive results showcase the revolutionary promise of DB-OTO as a potential treatment for otoferlin-related deafness, and we are excited to see how this translates into an individual's development, especially since early intervention is associated with better outcomes for speech development. With the DB-OTO CHORD trial now enrolling participants in sites across the U.S. and Europe, we're part of the beginning of a new era of gene therapy research that looks to create treatment options that address the root cause of profound genetic deafness."
哥倫比亞大學耳鼻喉頭頸外科系主任、臨床試驗研究員勞倫斯·盧斯蒂格醫學博士說:“有機會爲出生時患有嚴重遺傳性耳聾的兒童提供完整的複雜性和聲音頻譜,這是我一生中沒想到會見到的現象。”“這些令人印象深刻的結果展示了DB-OTO作爲Otoferlin相關耳聾的潛在治療方法所具有的革命性前景,我們很高興看到這如何轉化爲個人的發展,尤其是因爲早期干預與更好的言語發育結果有關。隨着DB-OTO CHORD試驗現已在美國和歐洲各地招募參與者,我們是基因療法研究新時代開始的一部分,該研究旨在創造治療方案,解決嚴重遺傳性耳聾的根本原因。”
In the trial, both children received a single intracochlear injection of DB-OTO in one ear. The surgical procedure leverages the same approach used for cochlear implants, which is amenable for use in young infants. Hearing improvements were assessed by pure tone audiometry (PTA) and auditory brainstem response (ABR). PTA is considered by auditory experts to be the gold standard measurement of hearing and is measured through behavioral confirmation of sound (e.g., turning head towards sound) emitted at different intensity levels (measured in decibels or dB). ABR corroborates these behavioral responses, serving as an objective confirmation of hearing function, by measuring electrical brainstem responses to sound emitted at different dBs.
在試驗中,兩名兒童在一隻耳朵內接受了單次 DB-OTO 注射。外科手術採用了與人工耳蝸植入相同的方法,適用於年幼的嬰兒。通過純音聽力測量(PTA)和聽覺腦幹反應(ABR)評估聽力改善。聽覺專家認爲 PTA 是衡量聽力的黃金標準,是通過對不同強度級別(以分貝或 dB 測量)發出的聲音(例如將頭轉向聲音)的行爲確認來衡量的。ABR 通過測量腦幹對不同數據庫發出的聲音的電反應,證實了這些行爲反應,客觀地確認了聽覺功能。
At baseline, both participants had no behavioral (PTA) or electrophysiological (ABR) responses at maximum sound levels (≥100 dB). Following treatment with DB-OTO, both children showed auditory responses at the first efficacy assessment of 4 weeks.
在基線時,兩名參與者在最大聲級(≥100 dB)下均沒有行爲(PTA)或電生理(ABR)反應。在使用DB-OTO治療後,兩名兒童在爲期4周的首次療效評估中均出現聽覺反應。
As presented at ASGCT, the first participant dosed in the trial was 16 months of age at the 24-week assessment and showed:
正如在ASGCT上所述,在爲期24周的評估中,該試驗中第一位給藥的參與者年齡爲16個月,並顯示:
Improvement of hearing to normal levels across key speech frequencies, with an average 84 dB improvement from baseline and one frequency measure reaching 10 dB in hearing level per PTA. Across all tested frequencies, an average 80 dB improvement from baseline was observed.
Positive ABR responses, with best frequency reaching 45 dB.
將關鍵語音頻率的聽力提高到正常水平,每個 PTA 的聽力水平平均比基線提高了 84 dB,一項頻率測量值的聽力水平達到了 10 dB。在所有測試頻率中,觀察到平均比基線提高了80 dB。
ABR 響應良好,最佳頻率達到 45 dB。
The second participant dosed in the trial was 4 years of age at the 6-week assessment and experienced consistent results to the first participant at the same timepoint, including:
在爲期6周的評估中,該試驗中的第二名受試者年齡爲4歲,並且在同一時間點與第一名參與者的結果一致,包括:
Initial improvement of hearing with responses to loud sounds, which was observed across key speech frequencies, with an average 19 dB improvement from baseline and one frequency measure reaching 80 dB in hearing level per PTA. Across all tested frequencies, an average 16 dB improvement from baseline was observed.
Positive ABR responses, with best frequency reaching 75 dB.
在關鍵語音頻率上觀察到對響亮聲音的反應,聽力得到初步改善,與基線相比平均改善了19 dB,每個 PTA 的聽力水平達到了 80 dB。在所有測試頻率中,觀察到比基線平均提高了16 dB。
ABR 響應良好,最佳頻率達到 75 dB。
Both the surgical procedure (delivery and post-operation) and DB-OTO were well tolerated, and there were no related adverse events or serious adverse events following treatment.
外科手術(分娩和術後)和DB-OTO均具有良好的耐受性,治療後沒有相關的不良事件或嚴重的不良事件。
DB-OTO received Orphan Drug, Rare Pediatric Disease and Fast Track Designations from the U.S. Food and Drug Administration and Orphan Drug Designation was granted by the European Medicines Agency. The potential use of DB-OTO for otoferlin-related hearing loss is currently under clinical investigation, and its safety and efficacy have not been evaluated by any regulatory authority.
DB-OTO 獲得了美國食品藥品監督管理局頒發的孤兒藥、罕見兒科疾病和快速通道認定,孤兒藥認證由歐洲藥品管理局授予。DB-OTO治療耳聾相關聽力損失的潛在用途目前正在臨床研究中,其安全性和有效性尚未經過任何監管機構的評估。
About Otoferlin-related Hearing Loss
Congenital deafness (hearing loss present at birth) is a significant unmet medical need that affects approximately 1.7 out of every 1,000 children born in the U.S. Although approximately half of these cases have genetic causes, otoferlin-related hearing loss is ultra-rare. This specific condition is caused by variants in the otoferlin gene, which impairs the production of the OTOF protein that is critical for the communication between the sensory cells of the inner ear and the auditory nerve. While hearing aids and cochlear implants can amplify sound to improve hearing for individuals with a range of hearing loss, these devices do not currently restore the full spectrum of sound.
關於與Otoferlin相關的聽力損失
先天性耳聾(出生時出現聽力損失)是一項尚未得到滿足的重大醫療需求,在美國出生的每1,000名兒童中,約有1.7人受到影響。儘管這些病例中約有一半是遺傳原因,但與耳聾素相關的聽力損失極爲罕見。這種特殊情況是由otoferlin基因的變異引起的,該變異會損害OTOF蛋白的產生,而OTOF蛋白對於內耳感覺細胞和聽覺神經之間的交流至關重要。雖然助聽器和人工耳蝸可以放大聲音以改善患有各種聽力損失的人的聽力,但這些設備目前無法恢復全譜的聲音。
About the CHORD Trial
The CHORD trial (NCT# 05788536) is a Phase 1/2 first-in-human, multicenter, open-label trial to evaluate the safety, tolerability, and preliminary efficacy of DB-OTO in infants, children and adolescents with otoferlin variants.
關於 CHORD 試用版
CHORD試驗(NCT# 05788536)是一項第1/2期人體、多中心、開放標籤的試驗,旨在評估DB-OTO對患有奧托費林變體的嬰兒、兒童和青少年的安全性、耐受性和初步療效。
Currently enrolling children across sites in the U.S., United Kingdom and Spain (<18 years of age; staggered by age in the U.S.), CHORD is being conducted in two parts. In the initial dose-escalation cohort (Part A), participants will receive a single intracochlear injection of DB-OTO in one ear, while in expansion cohort (Part B), participants will receive simultaneous single intracochlear injections of DB-OTO in both ears at the selected dose from Part A.
CHORD目前在美國、英國和西班牙的各個地點招收兒童(年齡小於18歲;在美國按年齡錯開),分兩部分進行。在最初的劑量遞增隊列(A部分)中,參與者將在一隻耳朵內接受單次DB-OTO注射,而在擴展隊列(B部分)中,參與者將按A部分的選定劑量在雙耳中同時注射單次DB-OTO。
Additional information about the trial, including enrollment, can be obtained by contacting clinicaltrials@regeneron.com.
有關該試用的更多信息,包括註冊信息,可通過聯繫 clinicaltrials@regeneron.com 獲取。
About DB-OTO and the Regeneron Auditory Program
DB-OTO is an investigational cell-selective, adeno-associated virus (AAV) gene therapy designed to provide durable, physiological hearing to individuals with profound, congenital hearing loss caused by variants of the otoferlin gene. The treatment aims to deliver a working copy to replace the faulty otoferlin gene using a modified, non-pathogenic virus that is delivered via an injection into the cochlea under general anesthesia (similar to the procedure used for cochlear implantation). In this gene therapy, the newly introduced otoferlin gene is under the control of a proprietary cell-specific Myo15 promoter, which is intended to restrict expression only to inner hair cells that normally express otoferlin.
關於 DB-OTO 和 Regeneron 聽覺計劃
DB-OTO 是一種正在研究的細胞選擇性、腺相關病毒 (AAV) 基因療法,旨在爲由 otoferlin 基因變異引起的嚴重先天性聽力損失的患者提供持久的生理聽力。該治療旨在提供一個工作拷貝,使用一種經過改良的非致病性病毒來替換有缺陷的otoferlin基因,該病毒在全身麻醉下通過注射到耳蝸(類似於人工耳蝸植入的程序)。在這種基因療法中,新引入的otoferlin基因受專有的細胞特異性Myo15啓動子的控制,該啓動子旨在僅限制通常表達奧托費林的內部毛細胞的表達。
The ongoing CHORD trial is Regeneron's first clinical-stage auditory program. In addition to DB-OTO, AAV.103 is also being investigated for people with GJB2-related hearing loss.
正在進行的CHORD試驗是Regeneron的第一個臨床階段聽覺項目。除了DB-OTO,AAV.103也在調查中,以尋找與GJB2相關的聽力損失患者。