Subcutaneous Administration of a Zwitterionic Chitosan-Based Hydrogel for Controlled Spatiotemporal Release of Monoclonal Antibodies

被引：20

作者：

Grea, Thomas ^{[1
,2
]}

Jacquot, Guillaume ^{[3
,4
,5
]}

Durand, Arthur ^{[1
,6
]}

Mathieu, Clelia ^{[3
,5
]}

Gasser, Adeline ^{[3
,5
]}

Zhu, Chen ^{[3
,5
,7
]}

Banerjee, Mainak ^{[3
,5
,7
]}

Hucteau, Elyse ^{[3
,8
]}

Mallard, Joris ^{[3
,8
]}

Lopez Navarro, Pedro ^{[3
,5
]}

Popescu, Bogdan V. ^{[3
,5
]}

Thomas, Eloise ^{[9
]}

Kryza, David ^{[9
,10
]}

Sidi-Boumedine, Jacqueline ^{[9
,10
]}

Ferrauto, Giuseppe ^{[11
]}

Gianolio, Eliana ^{[11
]}

Fleith, Guillaume ^{[12
]}

Combet, Jerome ^{[12
]}

Brun, Susana ^{[13
]}

Erb, Stephane ^{[5
,14
,15
]}

Cianferani, Sarah ^{[5
,14
,15
]}

Charbonniere, Loic J. ^{[7
]}

Fellmann, Lyne ^{[16
]}

Mirjolet, Celine ^{[17
,18
]}

David, Laurent ^{[2
]}

Tillement, Olivier ^{[1
]}

Lux, Francois ^{[1
,19
]}

Harlepp, Sebastien ^{[3
,5
]}

Pivot, Xavier ^{[3
,5
]}

Detappe, Alexandre ^{[3
,5
,7
]}

机构：

[1] Univ Lyon, Univ Claude Bernard Lyon 1, Inst Lumiere Matiere, UMR 5306,CNRS, F-69622 Villeurbanne, France

[2] Univ Lyon, Jean Monnet Univ, Univ Claude Bernard Lyon 1, CNRS,UMR 5223,INSA Lyon,Ingn Mat Polymeres, F-69621 Villeurbanne, France

[3] Inst Cancerol Strasbourg Europe, Radiophys, F-67200 Strasbourg, France

[4] Nanoh, F-38070 St Quentin Fallavier, France

[5] Strasbourg Drug Discovery & Dev Inst IMS, F-67000 Strasbourg, France

[6] MexBrain, 13 Ave Albert Einstein, F-69100 Villeurbanne, France

[7] Univ Strasbourg, Inst Pluridisciplinaire Hubert Curien, Equipe Synth Pour IAnal, UMR CNRS 7178, F-67087 Strasbourg 02, France

[8] Biomed Res Ctr Strasbourg, oxidat stress & muscular protect Lab, Mitochondria, UR 3072, F-67000 Strasbourg, France

[9] Univ Claude Bernard Lyon 1, LAGEPP, CNRS, UMR 5007, F-69622 Villeurbanne, France

[10] Hosp Civils Lyon, Imthernat Plateform, F-69002 Lyon, France

[11] Univ Turin, Mol Imaging Ctr, Dept Mol Biotechnol & Hlth Sci, I-10124 Turin, Italy

[12] Univ Strasbourg, Inst Charles Sadron UPR 22, CNRS, 23 rue Loess,BP 84047, F-67034 Strasbourg 2, France

[13] Univ Strasbourg, IPST, F-67100 Strasbourg, France

[14] Univ Strasbourg, Lab Spectrometrie Masse BioOrgan, IPHC UMR 7178, CNRS, F-67087 Strasbourg, France

[15] Infrastructure Natl Prote ProFI, FR2048, F-67087 Strasbourg, France

[16] Univ Strasbourg, SILABE, F-67207 Niederhausbergen, France

[17] Ctr Georges Francois Leclerc, Radiat Oncol Dept, Preclin Radiat Therapy & Radiobiol Unit, F-21000 Dijon, France

[18] TIReCS team, INSERM UMR 1231, F-21000 Dijon, France

[19] Inst Univ France, F-75231 Paris, France

来源：

ADVANCED MATERIALS | 2024年 / 36卷 / 13期

基金：

欧洲研究理事会;

关键词：

antibody; hydrogel; subcutaneous administration; OPEN-LABEL; TRASTUZUMAB; PHARMACOKINETICS; MULTICENTER; MECHANISMS; PREFERENCE; RITUXIMAB; PHASE-3; ENZYME;

D O I：

10.1002/adma.202308738

中图分类号：

O6 [化学];

学科分类号：

0703 ;

摘要：

Subcutaneous (SC) administration of monoclonal antibodies (mAbs) is a proven strategy for improving therapeutic outcomes and patient compliance. The current FDA-/EMA-approved enzymatic approach, utilizing recombinant human hyaluronidase (rHuPH20) to enhance mAbs SC delivery, involves degrading the extracellular matrix's hyaluronate to increase tissue permeability. However, this method lacks tunable release properties, requiring individual optimization for each mAb. Seeking alternatives, physical polysaccharide hydrogels emerge as promising candidates due to their tunable physicochemical and biodegradability features. Unfortunately, none have demonstrated simultaneous biocompatibility, biodegradability, and controlled release properties for large proteins (>= 150 kDa) after SC delivery in clinical settings. Here, a novel two-component hydrogel comprising chitosan and chitosan@DOTAGA is introduced that can be seamlessly mixed with sterile mAbs formulations initially designed for intravenous (IV) administration, repurposing them as novel tunable SC formulations. Validated in mice and nonhuman primates (NHPs) with various mAbs, including trastuzumab and rituximab, the hydrogel exhibited biodegradability and biocompatibility features. Pharmacokinetic studies in both species demonstrated tunable controlled release, surpassing the capabilities of rHuPH20, with comparable parameters to the rHuPH20+mAbs formulation. These findings signify the potential for rapid translation to human applications, opening avenues for the clinical development of this novel SC biosimilar formulation. A novel hydrogel is developed using chitosan and chitosan@DOTAGA, enabling the repurposing of sterile monoclonal antibodies formulations designed for intravenous administration as tunable subcutaneous (SC) formulations. This hydrogel has demonstrated biodegradability, biocompatibility, and controlled release properties in mice and nonhuman primates, offering rapid translation to human use and potential for clinical development of SC biosimilars.image

引用

页数：10

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