Ab0282 safety, Tolerability and Selective Expansion of Regulatory T Cells by a Single Dose of the Novel Il-2 Mutein Pt101 in a Phase 1 Study in Healthy Volunteers

Sundy, John S.; Otipoby, Kevin L.; Higginson-Scott, Nathan; Visweswaraiah, J.; Sampson, Emma; Kis-Toth, K.; Monsef, Alireza; Petaipimol, P.; Essayan, David M.; Cosenza, Mary Ellen; Kakkar, Reva; Viney, Joanne L.

doi:10.1136/annrheumdis-2021-eular.1200

Cited by 3 publications

(3 citation statements)

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“… SLE MAD: five dosing cohorts; every 2 weeks; treatment for 12 weeks; subcutaneously; 2nd line Phase 1; NCT03451422, completed (Oct 2021) Peak T reg expansion at day 8 post dose sustained for up to 42 days after the last dose; Mean peak increases in T reg 1.1-17.4-fold above the baseline depending on the dose; Increased Helios, PD-1, ICOS, CD39, GITR in expanded T reg ; No significant changes in CD4 and CD8 T cells nor NK cells; No changes in pro-inflammatory cytokines. AE: mild-to-moderate injection site reactions, No dose-limiting toxicities; PK: linear and dose-dependent, half-life 18 −30 h. RA MAD: multiple dosing schedules, follow-up for 12 weeks; 2nd line Phase 1/2; NCT03410056, terminated (May 2020) N/A N/A GvHD (chronic) MAD: weekly or every 2 weeks; 2nd line Phase 1/2; NCT03422627, terminated (Feb 2022) N/A N/A SLE Dose-ranging; 2nd line Phase 2b; NCT04680637, terminated (Jun 2023) N/A N/A Ulcerative colitis Dose-finding; 2nd line Phase 2; NCT04987307, recruiting (Jun 2024) N/A N/A RG7835 (RO7049665) [ 115 ] IL-2Rα-biased IL-2m (T3A, N88D, C125A) IgG1-fusion protein Healthy volunteers SAD; subcutaneous Phase 1; NCT03221179, completed (Jul 2019) N/A N/A Ulcerative colitis MAS; subcutaneous; 1st line Phase 1; NCT03943550, terminated based on the lack of robust clinical improvement in the underlying condition after 8 weeks of treatment (Jul 2021) N/A N/A Autoimmune hepatitis Every 2 weeks; subcutaneous administration; 2nd line Phase 2; NCT04790916, terminated based on a lack of efficacy seen with RO7049665 in a study of ulcerative colitis (Nov 2021) N/A N/A PT101/ MK-6194 [ 144 ] IL-2Rα-biased IL-2m (L118I, N88D, V69A, Q74P, C125S) Fc-fusion protein Healthy volunteers SAD: five dose levels from 1 mg to 10 mg, subcut...…”

Section: Il-2-based Immunotherapiesmentioning

confidence: 99%

“…These expanded T reg had increased expression of FOXP3 and CD25, suggesting enhanced function and stability. In a phase 1a single ascending dose clinical trial in healthy volunteers, PT101 was safe and well-tolerated, and a dose-dependent expansion of CD25 bright T reg cells was observed with a mean maximum increase of 72.5-fold for CD25 bright T reg by day 8-10 (and an overall 3.6-fold increase in total T reg ) [ 144 ]. T conv and NK cells were not increased while increases in eosinophil counts were transient.…”

Section: Il-2-based Immunotherapiesmentioning

confidence: 99%

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IL-2 immunotherapy for targeting regulatory T cells in autoimmunity

Lykhopiy,

Malviya,

Humblet-Baron

et al. 2023

Genes Immun

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FOXP3+ regulatory T cells (Treg) are indispensable for immune homoeostasis and for the prevention of autoimmune diseases. Interleukin-2 (IL-2) signalling is critical in all aspects of Treg biology. Consequences of defective IL-2 signalling are insufficient numbers or dysfunction of Treg and hence autoimmune disorders in human and mouse. The restoration and maintenance of immune homoeostasis remain central therapeutic aims in the field of autoimmunity. Historically, broadly immunosuppressive drugs with serious side-effects have been used for the treatment of autoimmune diseases or prevention of organ-transplant rejection. More recently, ex vivo expanded or in vivo stimulated Treg have been shown to induce effective tolerance in clinical trials supporting the clinical benefit of targeting natural immunosuppressive mechanisms. Given the central role of exogenous IL-2 in Treg homoeostasis, a new and promising focus in drug development are IL-2-based approaches for in vivo targeted expansion of Treg or for enhancement of their suppressive activity. In this review, we summarise the role of IL-2 in Treg biology and consequences of dysfunctional IL-2 signalling pathways. We then examine evidence of efficacy of IL-2-based biological drugs targeting Treg with specific focus on therapeutic candidates in clinical trials and discuss their limitations.

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Section: Il-2-based Immunotherapiesmentioning

confidence: 99%

Section: Il-2-based Immunotherapiesmentioning

confidence: 99%

IL-2 immunotherapy for targeting regulatory T cells in autoimmunity

Lykhopiy,

Malviya,

Humblet-Baron

et al. 2023

Genes Immun

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“…The engineered IL-2 mutein-IgG complex supported selective Treg expansion over a wide dose range and resolved non-obese diabetes (NOD) in mice [ 66 ]. The promise of IL-2 mutein in human disease is now being realised after safety and dose finding studies supported the progression to a pioneering clinical trial of PT101 IL-2 mutein complex in patients with active ulcerative colitis [ 67 , 68 ] (ClinicalTrials.gov NCT04924114).…”

Section: Key Challenges and Opportunitiesmentioning

confidence: 99%

Challenges and opportunities in achieving effective regulatory T cell therapy in autoimmune liver disease

et al. 2022

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Autoimmune liver diseases (AILD) include autoimmune hepatitis (AIH), primary biliary cholangitis (PBC) and primary sclerosing cholangitis (PSC). These immune-mediated liver diseases involve a break down in peripheral self-tolerance with largely unknown aetiology. Regulatory T cells (Treg) are crucial in maintaining immunological tolerance. Hence, Treg immunotherapy is an attractive therapeutic option in AILD. Currently, AILD do not have a curative treatment option and patients take life-long immunosuppression or bile acids to control hepatic or biliary inflammation. Clinical investigations using good manufacturing practice (GMP) Treg in autoimmune liver disease have thus far demonstrated that Treg therapy is safe and that Treg migrate to inflamed liver tissue. For Treg immunotherapy to achieve efficacy in AILD, Treg must be retained within the liver and maintain their suppressive phenotype to dampen ongoing immune responses to hepatocytes and biliary epithelium. Therefore, therapeutic Treg subsets should be selected for tissue residency markers and maximal functionality. Optimisation of dosing regime and understanding longevity of Treg in vivo are critical to successful Treg therapy. It is also essential to consider combination therapy options to complement infused Treg, for instance low-dose interleukin-2 (IL-2) to support pre-existing and infused Treg survival and suppressive function. Understanding the hepatic microenvironment in both early- and late-stage AILD presents significant opportunity to better tailor Treg therapy in different patient groups. Modification of a hostile microenvironment to a more favourable one either prior to or during Treg therapy could enhance the efficacy and longevity of infused GMP-Treg. Applying recent technology to discovery of autoantigen responses in AILD, T cell receptor (TCR) sequencing and use of chimeric antigen receptor (CAR) technology represents the next frontier for disease-specific CAR-Treg therapies. Consideration of all these aspects in future trials and discovery research would position GMP Treg immunotherapy as a viable personalised-medicine treatment option for effective control of autoimmune liver diseases.

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