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更新于：2025-05-07

SIRPβ1

更新于：2025-05-07

基本信息

别名

CD172 antigen-like family member B、CD172b、signal regulatory protein beta 1

+ [5]

简介-

关联

项与 SIRPβ1 相关的药物

ELA-026

靶点

SIRPα x SIRPβ1 x SIRPγ x Tubulin

作用机制

SIRPα调节剂 [+3]

在研机构

Electra Therapeutics, Inc.

原研机构

Electra Therapeutics, Inc.

在研适应症

噬血细胞性淋巴组织细胞增多症 [+1]

非在研适应症-

最高研发阶段临床2/3期

首次获批国家/地区-

首次获批日期1800-01-20

项与 SIRPβ1 相关的临床试验

NCT05416307

/ Active, not recruiting临床2/3期

A Multipart, Open-label, Single-arm, Multicenter Study to Evaluate the Safety, Efficacy and Pharmacokinetics of ELA026 in Participants with Secondary Hemophagocytic Lymphohistiocytosis (sHLH)

Hemophagocytic lymphohistiocytosis is a rare, aggressive and life-threatening syndrome of excessive immune activation. Secondary hemophagocytic lymphohistiocytosis (sHLH) is the most common form of this disease and is typically associated with several other clinical conditions (eg, malignancy associated HLH (mHLH), infection, or autoimmune disease). ELA026 is a fully human immunoglobulin G1 (IgG1) signal regulatory protein (SIRP)-directed monoclonal antibody designed to deplete the myeloid and T cells driving the inflammation. The purpose of this study is to assess the safety, efficacy pharmacokinetics and pharmacodynamics of ELA026 in participants with sHLH.

开始日期2022-05-19

申办/合作机构

Electra Therapeutics, Inc.

NCT05556863

/ Completed临床1期

A Randomized, Double-blind, Placebo-controlled Study of the Safety, Tolerability, Pharmacokinetics, and Pharmacodynamics of ELA026 Following Intravenous and/or Subcutaneous Administration of Single and Multiple Doses in Healthy Adults

ELA026 is a fully human IgG1 SIRP-directed monoclonal antibody designed to reduce the myeloid and T cells driving the inflammation. The purpose of this study is to assess the safety, tolerability, pharmacokinetics and pharmacodynamics of ELA026 in Single and Multiple Doses in Healthy Adults.

开始日期2021-10-18

申办/合作机构

Electra Therapeutics, Inc.

EUCTR2021-001387-20-ES

/ Unknown status临床1期

A Phase 1b, Open-label, Single-arm, Multicenter Study to Evaluate the Safety, Efficacy and Pharmacokinetics of Multiple Doses of ELA026 in Adults and Adolescents with Secondary Hemophagocytic Lymphohistiocytosis (sHLH).

开始日期2021-10-11

申办/合作机构

Electra Therapeutics, Inc.

100 项与 SIRPβ1 相关的临床结果

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100 项与 SIRPβ1 相关的转化医学

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0 项与 SIRPβ1 相关的专利（医药）

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项与 SIRPβ1 相关的文献（医药）

2025-03-14·Science Advances

Genetically supported targets and drug repurposing for brain aging: A systematic study in the UK Biobank

Article

作者: Wu, Fei ; Jia, Zhilong ; Huang, Zhengxing ; Yuan, Jing ; Zhu, Yi-Cheng ; Yi, Fan ; Somekh, Judith ; Peleg, Mor

Brain age gap (BAG), the deviation between estimated brain age and chronological age, is a promising marker of brain health. However, the genetic architecture and reliable targets for brain aging remains poorly understood. In this study, we estimate magnetic resonance imaging (MRI)–based brain age using deep learning models trained on the UK Biobank and validated with three external datasets. A genome-wide association study for BAG identified two unreported loci and seven previously reported loci. By integrating Mendelian Randomization (MR) and colocalization analysis on eQTL and pQTL data, we prioritized seven genetically supported druggable genes, including MAPT , TNFSF12 , GZMB , SIRPB1 , GNLY , NMB , and C1RL , as promising targets for brain aging. We rediscovered 13 potential drugs with evidence from clinical trials of aging and prioritized several drugs with strong genetic support. Our study provides insights into the genetic basis of brain aging, potentially facilitating drug development for brain aging to extend the health span.

2024-11-01·Obesity

In silico and functional analysis identifies key gene networks and novel gene candidates in obesity‐linked human visceral fat

Article

作者: Ghosh, Sujoy ; Chua, Ruiming ; Zhou, Hongwen ; Seshachalam, Pratap Veerabrahma ; Lei, Sun ; Wang, Lijin

AbstractObjectiveVisceral adiposity is associated with increased proinflammatory activity, insulin resistance, diabetes risk, and mortality rate. Numerous individual genes have been associated with obesity, but studies investigating gene regulatory networks in human visceral obesity have been lacking.MethodsWe analyzed gene regulatory networks in human visceral adipose tissue (VAT) from 48 and 11 Chinese patients with and without obesity, respectively, using gene coexpression and gene regulatory network construction from RNA‐sequencing data. We also conducted RNA interference‐based functional tests on selected genes for effects on adipocyte differentiation.ResultsA scale‐free gene coexpression network was constructed from 360 differentially expressed genes between VAT samples from patients with and without obesity (absolute log fold change > 1, false discovery rate [FDR] < 0.05), with edge probability > 0.8. Gene regulatory network analysis identified candidate transcription factors associated with differentially expressed genes. A total of 15 subnetworks (communities) displayed altered connectivity patterns between obesity and nonobesity networks. Genes in proinflammatory pathways showed increased network connectivity in VAT samples with obesity, whereas the oxidative phosphorylation pathway displayed reduced connectivity (enrichment FDR < 0.05). Functional screening via RNA interference identified genes such as SOX30, SIRPB1, and OSBPL3 as potential network‐derived candidates influencing adipocyte differentiation.ConclusionsThis approach highlights the network architecture in human obesity, identifies novel candidate genes, and generates new hypotheses regarding network‐assisted gene regulation in VAT.

2024-03-19·Journal of Alzheimer’s Disease

An Insertion Within SIRPβ1 Shows a Dual Effect Over Alzheimer’s Disease Cognitive Decline Altering the Microglial Response

Article

作者: Sánchez-Juan, Pascual ; Rodriguez-Rodriguez, Eloy ; García-Madrona, Sebastián ; Nieto, María Dolores ; González-Pérez, Antonio ; Alarcón-Martín, Emilio ; De la Guía, Paz ; Alegret, Montserrat ; Lage, Carmen ; López de la Rica, María ; del Ser, Teodoro ; Huerto Vilas, Raquel ; Roberto, Natalia ; Jiménez-Sánchez, Rocío ; Orellana, Adelina ; Bernal Sánchez-Arjona, María ; Hernández, Isabel ; Sanchez-Mejias, Elisabeth ; Sánchez-Fernández, Ana ; Sanabria, Ángela ; Gonzalez-Palma, Laura ; Fibla Palazon, Joan ; Torrecilla, Javier ; Garrido-Martín, Diego ; Piñol-Ripoll, Gerard ; Menéndez-González, Manuel ; Carracedo, Ángel ; Pineda, Juan A. ; Ruiz, Agustín ; Muñoz-Castro, Clara ; Rueda, Lourdes ; Macías, Juan ; Pérez-Cordón, Alba ; García-González, Pablo ; Calero, Miguel ; Espinosa, Ana ; García-Alberca, José María ; Rosende-Roca, Maitée ; Govantes, Fernando ; Mendoza, Silvia ; Martín Montes, Ángel ; Furniet, María del Carmen ; Urbano, Concepción ; García-Peralta, María ; Mejias-Ortega, Marina ; Vitorica, Javier ; Buiza-Rueda, Dolores ; Pino-Angeles, Almudena ; Peña, Isabel ; Laplana, Marina ; Moreno-Grau, Sonia ; Tena, Juan Jesus ; Martínez Rodríguez, Carmen ; Royo, Jose Luis ; Lopez, Aroa ; Quintela, Inés ; Royo-Aguado, Jose Luis ; Cruz-Gamero, Jose Manuel ; Carrillejo, Rosario ; Rosas Allende, Irene ; Navarro, Victoria ; de Rojas, Itziar ; Mancilla, Tomás ; Fernández-Fuertes, Marta ; Lopez-Gutierrez, Lidia ; Frank-García, Ana ; Marquié, Marta ; Tárraga, Lluís ; Gris, Esther ; Gutierrez, Antonia ; Diez-Fairen, Mónica ; Tomas-Gallardo, Laura ; Alvarez, Ignacio ; Franco-Macías, Emilio ; Medina, Miguel ; Gonzalez, Irene ; Rábano, Alberto ; Pastor, Ana Belén ; Álvarez, Victoria ; Corma-Gómez, Anaïs ; Pareja, Nuria ; Zafra, Carmen ; Mir, Pablo ; Boada, Mercè ; Garcia-Ribas, Guillermo ; Polvillo, Rocio ; Pastor, Pau ; Ocejo, Olga ; Ortega, Gemma ; Sotolongo-Grau, Oscar ; Valero, Sergi ; Montrreal, Laura ; Reyes-Engel, Armando ; Sáez, María Eugenia ; Arias Pastor, Alfonso ; Bullido, María José ; Real, Luis Miguel ; Guigo, Roderic ; Jimenez, Sebastian ; Luque, Macarena ; García-Casares, Natalia ; Ruiz, Maximiliano ; Bravo, Maria Jose

Background:Microglial dysfunction plays a causative role in Alzheimer’s disease (AD) pathogenesis. Here we focus on a germline insertion/deletion variant mapping SIRPβ1, a surface receptor that triggers amyloid-β(Aβ) phagocytosis via TYROBP.Objective:To analyze the impact of this copy-number variant in SIRPβ1 expression and how it affects AD molecular etiology.Methods:Copy-number variant proxy rs2209313 was evaluated in GERALD and GR@ACE longitudinal series. Hippocampal specimens of genotyped AD patients were also examined. SIRPβ1 isoform-specific phagocytosis assays were performed in HEK393T cells.Results: The insertion alters the SIRPβ1 protein isoform landscape compromising its ability to bind oligomeric Aβ and its affinity for TYROBP. SIRPβ1 Dup/Dup patients with mild cognitive impairment show an increased cerebrospinal fluid t-Tau/Aβ ratio ( p = 0.018) and a higher risk to develop AD (OR = 1.678, p = 0.018). MRIs showed that Dup/Dup patients exhibited a worse initial response to AD. At the moment of diagnosis, all patients showed equivalent Mini-Mental State Examination scores. However, AD patients with the duplication had less hippocampal degeneration ( p < 0.001) and fewer white matter hyperintensities. In contrast, longitudinal studies indicate that patients bearing the duplication allele show a slower cognitive decline ( p = 0.013). Transcriptional analysis also shows that the SIRPβ1 duplication allele correlates with higher TREM2 expression and an increased microglial activation. Conclusions: The SIRPβ1 internal duplication has opposite effects over MCI-to-Dementia conversion risk and AD progression, affecting microglial response to Aβ. Given the pharmacological approaches focused on the TREM2-TYROBP axis, we believe that SIRPβ1 structural variant might be considered as a potential modulator of this causative pathway.

项与 SIRPβ1 相关的新闻（医药）

2024-12-10

·PipelineReview

Electra Therapeutics Presents Positive Clinical Results From Completed Phase 1b Study of ELA026 in Secondary Hemophagocytic Lymphohistiocytosis (sHLH) in an Oral Session at ASH 2024

ELA026 demonstrated 100% overall response rate, improved survival, and a favorable safety profile in malignancy-associated HLH (mHLH), the most common type of sHLH with the poorest prognosis. Company is advancing ELA026 as a frontline treatment for patients with sHLH and plans to initiate a global pivotal study in 2025. SOUTH SAN FRANCISCO, CA, USA I December 09, 2024 I Electra Therapeutics , Inc., a clinical stage biotechnology company developing antibody therapies against novel targets for immunological diseases and cancer, announced the presentation of positive results from the completed Phase 1b study of ELA026 for the treatment of secondary hemophagocytic lymphohistiocytosis (sHLH). ELA026 is a first-in-class monoclonal antibody that targets SIRP-α/β1/γ on the cell surface of myeloid cells and T lymphocytes, the principal pathological immune cells that induce the cytokine storm and hyperinflammation in sHLH. Targeting SIRP to selectively deplete pathogenic immune cells has potential for broad therapeutic applications in immunology, inflammation and cancer. The results of the ELA026 study in sHLH are being presented today at 2:45 PM PST in an oral session at the American Society of Hematology (ASH) Annual Meeting in San Diego, CA. The Phase 1b study was an open-label, single-arm, multicenter study designed to evaluate the safety and efficacy of ELA026, assess the pharmacodynamic (PD) and pharmacokinetic (PK) profile, and identify a dose regimen for further evaluation in a Phase 2/3 study ( NCT05416307 ). The Phase 1b study demonstrated that for sHLH patients with the poorest prognosis, those with malignancy-associated HLH (mHLH), treatment with ELA026 in frontline settings achieved 100% overall response rate by week 4 and 100% hospital discharge, as well as 92% survival at two months. Various PD and HLH-related biomarkers showed that ELA026 rapidly attenuated inflammation, which correlated with clinical responses. “ELA026 has shown potential to be a transformative treatment for sHLH, a life-threatening disease with no approved therapies. Compared with available treatment, which may include chemotherapy and single cytokine-directed therapies, ELA026 may offer a safer, more effective approach to address the overwhelming immune reaction in sHLH. The Phase 1b study results showing rapid PD and biomarker effects and improved survival at two months are particularly promising,” said Swaminathan P. Iyer, MD, Professor in the Department of Lymphoma/Myeloma at The University of Texas MD Anderson Cancer Center. “There is a growing appreciation that controlling the cytokine storm early in the sHLH disease course is necessary to prevent multiorgan failure and allow for proper treatment of the underlying cancer. It is clear that overcoming this critical early period of hyperinflammation in sHLH provide significant clinical benefits for patients.” “We are highly encouraged by these compelling results for sHLH patients, and Electra is working to advance ELA026 into a pivotal study as rapidly as possible. Through rigor and resolve, our team has pioneered a drug development program targeting SIRP, going from a novel idea to pivotal study readiness in five years,” said Kathy Dong, PharmD, MBA, President and CEO of Electra Therapeutics. “We have demonstrated the therapeutic value of selectively depleting pathological immune cells to modulate inflammation and look forward to applying this novel approach with ELA026 and our pipeline to expand to other diseases with high unmet need.” Phase 1b Study Results Presented in Oral Session at ASH The oral presentation at the ASH Annual Meeting, entitled “ELA026, a monoclonal antibody targeting signal regulatory protein-α/β1/γ rapidly controls inflammation and improves 2-month survival in treatment-naïve malignancy-associated hemophagocytic lymphohistiocytosis,” is being presented by the lead author, Abhishek Maiti, MD, Assistant Professor in the Department of Leukemia at The University of Texas MD Anderson Cancer Center. This presentation was featured in the section “Granulocytes, Monocytes, and Macrophages: From Inflammation to Hemophagocytic Lymphohistiocytosis.” The clinical results presented for ELA026 described the analysis of 12 mHLH patients treated in frontline settings in the completed Phase 1b clinical study. Highlights of the Phase 1b results are as follows: “Because sHLH is a complex, rapidly progressing disease with limited development precedents, advancing ELA026 required a focused approach that our Electra team boldly took on, in collaboration with leading researchers and clinicians. It is gratifying to see the positive Phase 1b results for ELA026 and the potential to improve outcomes for sHLH patients who face this life-threatening condition,” said Kim‑Hien Dao, DO, PhD, Chief Medical Officer at Electra. “We have a clear path forward based on recent alignment with the US FDA on the pivotal study design and are moving towards initiating a global Phase 2/3 study in 2025 to address the significant disease burden in sHLH.” About Secondary Hemophagocytic Lymphohistiocytosis (sHLH) Secondary hemophagocytic lymphohistiocytosis (sHLH) is a rare, life-threatening hyperinflammatory disease for which there is no approved treatment. It can be triggered by cancer, infection, autoimmune disease, or immunotherapy. sHLH is associated with a severe inflammatory response for which patients require immediate intervention. Without treatment, patients may experience multiorgan failure and death. sHLH is associated with high mortality early in the disease course, with malignancy-associated HLH (mHLH) patients having a mortality rate of approximately 50% at two months with available therapies. 3 About Electra Therapeutics Electra Therapeutics is a clinical stage biotechnology company developing therapies against novel targets for immune disorders and cancer. The company’s lead product candidate, ELA026, is a first-in-class monoclonal antibody that targets signal regulatory proteins (SIRP) on the cell surface of myeloid cells and T lymphocytes, and selectively depletes pathological immune cells. This novel approach has potential therapeutic benefit across numerous diseases. ELA026 is in clinical development for secondary hemophagocytic lymphohistiocytosis (sHLH), a rare, life-threatening hyperinflammatory condition for which there is no approved treatment. The company is pursuing other disease indications for ELA026, as well as additional development candidates, including an antibody with selectivity for activated T lymphocytes for broad application in immunology and inflammation. For more information, please visit www.electra-therapeutics.com and follow us on LinkedIn . 1 Lorenz F, et al. Leuk Lymphoma. 2018 Aug;59(8):1840-1850. 2 Abdelhay A, et al. Ann Hematol. 2023 Jul;102(7):1705-1711. 3 Löfstedt A, et al. Blood. 2024 Jan 18;143(3):233-242. SOURCE: Electra Therapeutics

临床结果临床1期免疫疗法AACR会议ASCO会议

2024-11-04

·Business Wire

Electra Therapeutics Receives FDA Fast Track Designation for ELA026 in Secondary Hemophagocytic Lymphohistiocytosis (sHLH)

SOUTH SAN FRANCISCO, Calif.--( BUSINESS WIRE )-- Electra Therapeutics, Inc., a clinical stage biotechnology company developing antibody therapies against novel targets for immunological diseases and cancer, today announced that the U.S. Food and Drug Administration (FDA) has granted Fast Track designation for ELA026 for the treatment of secondary hemophagocytic lymphohistiocytosis (sHLH). ELA026, a first-in-class antibody therapy targeting signal regulatory proteins (SIRP), is a novel approach to treat secondary HLH (sHLH), a rare, life-threatening disease for which there is no approved treatment. “Receiving Fast Track designation for ELA026 reinforces the urgent need for effective treatment options for patients suffering from sHLH,” said Kathy Dong, PharmD, CEO of Electra Therapeutics. “This designation gives us the opportunity to accelerate the development of ELA026, a therapy that we believe has the potential to transform the treatment landscape for sHLH patients. We are committed to advancing this drug candidate with urgency and to work closely with the FDA to bring this innovative therapy to patients as soon as possible.” The FDA grants investigational medicines Fast Track designation to facilitate the development and expedite the review of medicines that demonstrate the potential to treat serious conditions and fill an unmet medical need. Programs with Fast Track designation can benefit from early and more frequent interactions with the FDA to discuss the product candidate's development plan in addition to a rolling submission of the marketing application. Product candidates with Fast Track designation may also be eligible for priority review and accelerated approval. About Secondary Hemophagocytic Lymphohistiocytosis Secondary hemophagocytic lymphohistiocytosis (sHLH) is a rare, life-threatening hyperinflammatory disease for which there is no approved treatment. It can be triggered by cancer, infection, autoimmune disease, or immunotherapy. sHLH is associated with a severe inflammatory response for which patients require immediate intervention. Without effective treatment, patients may experience multiple organ failure and death. sHLH has a high mortality rate during the first months of diagnosis, with malignancy-associated HLH (mHLH) patients having the poorest outcomes. About Electra Therapeutics Electra Therapeutics is a clinical stage biotechnology company developing therapies against novel targets for immunological diseases and cancer. The company’s lead product candidate, ELA026, is a first-in-class monoclonal antibody that targets SIRP on the cell surface of myeloid cells and T lymphocytes, and selectively depletes pathological immune cells. ELA026 is in clinical development for secondary hemophagocytic lymphohistiocytosis (sHLH), a rare, life-threatening hyperinflammatory condition for which there is no approved treatment, as well as additional disease indications. For more information, please visit www.electra-therapeutics.com and follow us on LinkedIn .

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