Sarepta Therapeutics Reports Its SRP-9003 For Treatment Of Limb-Girdle Muscular Dystrophy Type-2E Shows Sustained Expression, Functional Improvements 2 Years After Administration
Sarepta Therapeutics Reports Its SRP-9003 For Treatment Of Limb-Girdle Muscular Dystrophy Type-2E Shows Sustained Expression, Functional Improvements 2 Years After Administration
Sarepta Therapeutics, Inc. (NASDAQ:SRPT), the leader in precision genetic medicine for rare diseases, today shared new results from the ongoing study of SRP-9003 (rAAVrh74.MHCK7.hSGCB), the Company’s investigational gene therapy for limb-girdle muscular dystrophy Type 2E (LGMD2E). In the first look at expression data from biopsies taken two years after a single administration of SRP-9003, results found sustained protein expression in muscle tissue. In functional outcomes assessments taken two years following treatment in Cohort 1 (low-dose cohort) and one year after treatment in Cohort 2 (high-dose cohort), patients continued to demonstrate stability in their NSAD (North Star Assessment for Dysferlinopathies) total score and improvements on timed function tests. Results are being presented today at the 2021 Muscular Dystrophy Association (MDA) Annual Clinical and Scientific Conference.
Sarepta治療公司(納斯達克:SRPT)今天分享了正在進行的SRP-9003(rAAVrh74.MHCK7.hSGCB)研究的新成果,SRP-9003是該公司針對2E型肢體帶狀肌營養不良症(LGMD2E)的探索性基因療法。在對單次注射SRP-9003兩年後活檢的表達數據的第一次觀察中,結果發現肌肉組織中持續的蛋白質表達。在隊列1(低劑量隊列)治療後兩年和隊列2(高劑量隊列)治療一年後進行的功能結果評估中,患者繼續表現出他們的NSAD(北極星功能障礙評估)總分的穩定性和定時功能測試的改善。研究結果將於今天在2021年肌營養不良症協會(MDA)年度臨牀和科學會議上公佈。
SRP-9003 is in development for the treatment of LGMD2E (also known as beta-sarcoglycanopathy and LGMDR4), a devastating monogenic neuromuscular disease caused by a lack of beta-sarcoglycan (beta-SG) proteins. SRP-9003 is a gene therapy construct that transduces skeletal and cardiac muscle, delivering a gene that codes for the full-length beta-SG protein, the absence of which is the sole cause of the progressive degeneration and a shortened lifespan characterized by the disease.
SRP-9003正在開發中,用於治療LGMD2E(也稱為β-肌糖病和LGMDR4),這是一種由缺乏β-肌聚糖(β-SG)蛋白引起的破壞性單基因神經肌肉疾病。SRP-9003是一種轉導骨骼肌和心肌的基因治療構建物,它提供了一種編碼全長β-SG蛋白的基因,該蛋白的缺失是以疾病為特徵的進行性退化和壽命縮短的唯一原因。
“This data is the first look at longer-term expression data with any gene therapy for muscular dystrophy. The meaningful and sustained levels of beta-sarcoglycan protein expression at two years and continued strength of the functional outcomes measured are tremendously positive and support continued advancement of this investigational treatment for patients,” said Louise Rodino-Klapac, Ph.D., executive vice president and chief scientific officer, Sarepta Therapeutics. “In Cohort 2, we also saw strong expression of delta-sarcoglycan and gamma-sarcoglycan proteins in addition to beta-sarcoglycan, which suggests that SRP-9003 is working to restore the dystrophin associated protein complex, or DAPC, which provides biological support for the sustained functional benefits observed in both cohorts. LGMD2E is one of the most severe forms of LGMD and causes significant disability in children while frequently leading to early mortality and the data continue to suggest this treatment could bring much needed hope to these patients.”
他説:“這些數據是首次使用基因療法治療肌營養不良症的長期表現數據。Sarepta治療公司執行副總裁兼首席科學官路易絲·羅迪諾-克拉帕克博士説:“兩年來有意義的、持續的β-肌聚糖蛋白表達水平和測量到的功能結果的持續強度是非常積極的,並支持繼續推進這種針對患者的研究治療。”在第2組中,除了β-肌聚糖外,我們還發現了δ-肌聚糖和γ-肌聚糖蛋白的強烈表達,這表明SRP-9003正在努力恢復肌營養不良蛋白相關蛋白複合體(DAPC),這為在兩個隊列中觀察到的持續功能益處提供了生物支持。LGMD2E是最嚴重的LGMD之一,會導致兒童嚴重殘疾,同時經常導致早期死亡,數據繼續表明,這種治療方法可能給這些患者帶來亟需的希望。“
Efficient transduction in skeletal muscle and robust beta-sarcoglycan protein expression were seen in both dose cohorts following infusion with SRP-9003, and significant creatine kinase (CK) reductions were observed.
注射SRP-9003後,兩個劑量組的骨骼肌信號轉導有效,β-肌聚糖蛋白表達旺盛,肌酸激酶(CK)顯著降低。
Cohort 1 (Dosed at 1.85×1013 vg/kg), 24 months following treatment:
隊列1(劑量為1.85×1013Vg/kg),治療後24個月:
- As measured by western blot, mean beta-SG of 54% at 24 months of normal control, compared to 36% measured at Day 60.
- Percent immunofluorescent (IF) positive fibers was 48% compared to normal control, compared to 51% at Day 60.
- Participants showed a mean intensity of 35% of transduced beta-SG, properly localized to the muscle sarcolemma, as measured by IF, compared to 47% at Day 60.
- The mean NSAD improvement from baseline of 5.7 points at 18 months was sustained through 24 months.
- All three participants demonstrated continued improvements from baseline across all functional measures, including time-to-rise, four-stair climb, 100-meter walk test and 10-meter walk test.
- 通過Western blot檢測,正常對照組24個月時的平均β-SG為54%,而在60天時的平均β-SG為36%。
- 免疫熒光(IF)陽性纖維的百分比與正常對照組相比為48%,而在第60天時為51%。
- 參與者表現出35%的轉導β-SG的平均強度,根據IF的測量,適當地定位於肌肉肌膜,而在第60天,這一比例為47%。
- 在18個月時,非甾體抗炎藥的平均改善從基線的5.7分持續到24個月。
- 所有三名參與者都顯示出在所有功能指標上都比基線有了持續的改善,包括上升時間、四級爬樓梯、100米步行測試和10米步行測試。
Cohort 2 (Dosed at 7.41×1013 vg/kg), 12 months following treatment:
隊列2(劑量為7.41×1013Vg/kg),治療後12個月:
- At Day 60, the expression of beta-SG (72% mean positive fibers and 73% mean intensity) resulted in increased expression of delta-sarcoglycan, with 65% mean positive fibers and 103% intensity, and gamma-sarcoglycan, 60% mean positive fibers and 97% intensity. These results suggest treatment with SRP-9003 demonstrates reconstitution of the DAPC, which could lead to improved membrane integrity and thus improved clinical motor outcomes measures.
- All three participants demonstrated improvements from baseline across all functional measures, including the NSAD, time-to-rise, four-stair climb, 100-meter walk test and 10-meter walk test.
- The mean NSAD improvement from baseline was 4.0 points at one year, compared to 3.7 at 6 months.
- 60d時,β-SG的表達(72%平均陽性纖維,73%平均強度)導致δ-肌聚糖表達增加,平均陽性纖維數為65%,平均強度為103%;γ-肌聚糖表達增加,平均陽性纖維數為60%,平均強度為97%。這些結果表明,SRP-9003治療顯示了DAPC的重建,這可能導致膜完整性的改善,從而改善臨牀運動結果措施。
- 所有三名參與者在所有功能測試中都顯示出比基線有所改善,包括NSAD、起牀時間、四級爬樓梯、100米步行測試和10米步行測試。
- 與基線相比,NSAD在一年內的平均改善為4.0分,而在6個月時為3.7分。
In an exploratory evaluation of all SRP-9003 treated patients compared to a natural history cohort; patients treated with SRP-9003 demonstrated significant improvements in functional outcomes after 24 months. The mean decline in total NSAD score for patients in the natural history cohort was 4.6 points while SRP-9003 treated patients demonstrated a mean improvement of 4.6 points for a clinically meaningful difference of 9.2 points.
在一項對所有接受SRP-9003治療的患者與自然病史隊列進行比較的探索性評估中,接受SRP-9003治療的患者在24個月後顯示出功能結果的顯著改善。自然病史隊列患者的NSAD總分平均下降4.6分,而接受SRP-9003治療的患者平均改善4.6分,具有臨牀意義的差異為9.2分。
Since the last update from this study in October 2020, there have been no new drug-related safety signals observed, and no decreases in platelet counts outside of the normal range and no evidence of clinical complement activation observed in either dose cohort.
自2020年10月這項研究的最後一次更新以來,沒有觀察到新的與藥物相關的安全信號,也沒有觀察到超出正常範圍的血小板計數下降,也沒有觀察到兩個劑量隊列中都有臨牀補體激活的證據。
譯文內容由第三人軟體翻譯。