NCT06722105

Brief Summary

Systemic sclerosis (SSc) is a rare, severe and chronic systemic autoimmune disease (AD) characterized by vasculopathy, immune dysregulation and fibrosis leading to multi-organ dysfunction (primarily skin, lungs, heart gastrointestinal tract and kidneys), with high morbidity and mortality, altered health-related quality of life, all at high cost for patients and society. Treatment are mostly symptomatic and only autologous hematopoietic stem cell transplantation (AHSCT) has shown long term improvement in overall and event-free survival with disease-modifying properties. However, AHSCT is contra-indicated in case of advanced visceral involvement and in eligible patients, it is still associated with risk of toxicity. There is an urgent need to identify safe and effective treatments for severe SSc. Mesenchymal stromal cells (MSC) are multipotent cells which carry immunomodulatory, pro-angiogenic and anti-fibrotic properties, that can target SSc pathogenesis and its clinical manifestations. The increasing use of MSC, harvested from bone marrow (MSC(M)), adipose tissue (MSC(AT)), or umbilical cord (MSC(UC)) in a variety of indications, provides consistent evidence supporting their safety in humans. The efficacy of MSC(M) intravenous (IV) injection for treating acute graft versus host disease led to their marketing approval in 2012 and MSC(AT) (Alofisel) were approved for severe Crohn's fistula in 2018. MSC represent a promising therapeutic approach for SSc. We have previously a) shown disease-specific abnormalities in MSC(M) from SSc patients, providing strong rationale to use allogeneic MSC to treat SSc patients, b) published the first phase I/II dose escalation trial using allogenic MSC(M) infusion in 20 severe SSc patients (ClinicalTrials.gov: NCT02213705, PHRC AOM 11-250) with no safety issues, significant improvement in skin fibrosis at 3 to 6 months after infusion which appeared lower thereafter, thereby supporting the need for repeated infusions. In vitro, experimental and clinical studies suggest that MSC properties vary according to their tissue of origin/source. We demonstrated that compared to MSC(M), MSC(AT) are easier to harvest and display higher proliferative capability before entering senescence, higher genetic stability, and superior immunosuppressive properties. Considering the above rationale, we hypothesize that use of healthy donors allogeneic MSC(AT) produced by Etablissement Français du Sang (EFS) will demonstrate a) no safety issues, b) an efficacy profile that will increase with repeated infusion of allogeneic MSC(AT) to treat SSc.

Trial Health

65
Monitor

Trial Health Score

Automated assessment based on enrollment pace, timeline, and geographic reach

Enrollment
18

participants targeted

Target at P25-P50 for phase_1

Timeline
12mo left

Started Dec 2024

Typical duration for phase_1

Status
not yet recruiting

Health score is calculated from publicly available data and should be used for screening purposes only.

Trial Relationships

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Study Timeline

Key milestones and dates

Study Progress59%
Dec 2024May 2027

Study Start

First participant enrolled

December 1, 2024

Completed
2 days until next milestone

First Submitted

Initial submission to the registry

December 3, 2024

Completed
6 days until next milestone

First Posted

Study publicly available on registry

December 9, 2024

Completed
1.3 years until next milestone

Primary Completion

Last participant's last visit for primary outcome

April 1, 2026

Completed
1.1 years until next milestone

Study Completion

Last participant's last visit for all outcomes

May 1, 2027

Expected
Last Updated

December 9, 2024

Status Verified

November 1, 2024

Enrollment Period

1.3 years

First QC Date

December 3, 2024

Last Update Submit

December 3, 2024

Conditions

Severe Systemic Sclerosis

Keywords

Systemic autoimmune diseaseAllogenic mesenchymal stromal cells infusion

Outcome Measures

Primary Outcomes (1)

  • Rate of treatment-related Serious Adverse Events

    Defined as Adverse Events (AE) of grade equal or above 3 using the NCI Common Terminology Criteria for Adverse Events (CTCAE) v5.0 classification, at one month after each infusion according to arms (M1, M4) An injection will be considered as not tolerated for any toxicity criteria above grade ≥ 3

    After each infusion

Secondary Outcomes (45)

  • Rate of treatment-related Serious Adverse Events (SAE)

    At time of infusion

  • Rate of treatment-related Serious Adverse Events (SAE)

    Within 24 hours of infusion

  • Rate of treatment-related Serious Adverse Events (SAE)

    At 6 months

  • Rate of treatment-related Serious Adverse Events (SAE)

    At 9 months

  • Rate of treatment-related Serious Adverse Events (SAE)

    At 12 months

  • +40 more secondary outcomes

Other Outcomes (2)

  • Exploring immune landscape in SSc skin biopsies and signatures predicting treatment response

    Up to 12 months

  • Evaluating new MSC potency assays interrogating MSC efferocytosis

    Up to 12 months

Study Arms (3)

2 infusions of MSC

EXPERIMENTAL
Biological: 2 infusions of MSC

1 infusion of MSC

EXPERIMENTAL
Biological: 1 infusion of MSC

Placebo

PLACEBO COMPARATOR
Other: Placebo

Interventions

2 infusions of MSCBIOLOGICAL

1 MSC(AT) (2x10\^6 cells/kg) injection at M0 and 1 MSC(AT) (2x10\^6 cells/kg) injection at M3

2 infusions of MSC
1 infusion of MSCBIOLOGICAL

1 MSC(AT) (2x10\^6 cells/kg) injection at M0 and 1 placebo injection at M3

1 infusion of MSC
PlaceboOTHER

Placebo at M0 and M3

Placebo

Eligibility Criteria

Age18 Years - 70 Years
Sexall
Healthy VolunteersNo
Age GroupsAdult (18-64), Older Adult (65+)

You may qualify if:

  • Provide signed and dated informed consent;
  • Willing to comply with all study procedures and be available for the duration of the study;
  • Male or female, aged ≥ 18 and ≤ 70 years of age
  • SSc patients according to American College of Rheumatology/European League Against Rheumatism (ACR/EULAR) 2013 classification criteria for SSc
  • Severe disease with either:
  • disease duration of 2 years or less with a modified Rodnan skin score (mRss) ≥ 20 and (abnormal CRP \> 5 mg/l and/or hemoglobin \< 11 g/dL), or
  • mRSS ≥ 15 without any restriction as to disease duration plus at least one major organ involvement as defined by:
  • respiratory involvement consisting of lung diffusion capacity for carbon monoxide (DLCO) and/or forced vital capacity (FVC) \< 80% predicted and evidence of interstitial lung disease : bronchiolar involvement, areas of ground-glass contusions or fibrosis (chest X-ray and/or high resolution computed tomography (HRCT) scan) and/or moderate Pulmonary hypertension with baseline resting systolic pulmonary arterial pressures \> 35 mmHg and below 50 mmHg by cardiac echocardiography, or mean pulmonary artery pressure \> 20 mmHg and \< 40 mm Hg on right heart catheterization;
  • renal involvement consisting of past renal crisis, microangiopathic hemolytic anemia, and/or renal insufficiency not explained by other causes than SSc;
  • cardiac involvement consisting of reversible congestive heart failure, atrial or ventricular rhythm disturbances such as recurrent episodes of atrial fibrillation or flutter, recurrent atrial paroxysmal tachycardia, 2nd or 3rd degree AV-block, mild to moderate pericardial effusion and/or presence of MRI involvement (Increased T1 or T2 mapping, late gadolinium enhancement, septal D sign). All causes of organ involvement should be attributed to SSc.
  • Contraindication, inadequate response or unwillingness to undergo AHSCT(determined by patient and physician judgement)
  • Contraindication, inadequate response or unwillingness or adverse events necessitating discontinuation of conventional immunosuppressive therapy (MMF, methotrexate);
  • Women of reproductive potential must use highly effective contraception;
  • Men of reproductive potential must use condoms;
  • Health insurance.

You may not qualify if:

  • Age \< 18 years and \> 70 years
  • Pregnancy or unwillingness to use adequate contraception;
  • Life-threatening end-organ damage defined as: DLCO (corrected for hemoglobin) \< 30% predicted; Left ventricular ejection fraction \< 40% by cardiac echocardiography; Pulmonary hypertension with baseline resting systolic pulmonary arterial pressures \> 50 mmHg by cardiac echocardiography, or mean pulmonary artery pressure \> 40 mmHg on right heart catheterization; glomerular filtration rate \< 30mL/min
  • Active Hepatitis (ASAT, ALAT \> 3 normal)
  • Neoplasms of less than 5 years, except for basal cell or in situ cervix carcinoma or concurrent myelodysplasia,
  • Uncontrolled hypertension
  • Uncontrolled acute or chronic infection
  • HIV-1 or HIV-2 infection
  • Body Mass Index \< 16.5 kg/m2
  • Severe psychiatric disorder
  • Bone marrow insufficiency, defined as neutropenia \< 1 x 109/L, thrombopenia \< 50 x 109/L, anemia \< 8 g/dL, lymphopenia \< 0,5 x 109/L
  • Inability to provide informed consent
  • Patient included in another interventional clinical trial
  • Patient under tutelle

Contact the study team to confirm eligibility.

Sponsors & Collaborators

MeSH Terms

Conditions

Scleroderma, Systemic

Condition Hierarchy (Ancestors)

Connective Tissue DiseasesSkin and Connective Tissue DiseasesSkin Diseases

Central Study Contacts

Dominique Farge, MD PhD

CONTACT

0142499764dominique.farge-bancel@aphp.fr

Jérôme Lambert, MD PhD

CONTACT

0142499742jerome.lambert@u-paris.fr

Study Design

Study Type
interventional
Phase
phase 1
Allocation
RANDOMIZED
Masking
DOUBLE
Who Masked
PARTICIPANT, INVESTIGATOR
Masking Details
Double-blind
Purpose
TREATMENT
Intervention Model
PARALLEL
Model Details: Multi-center, three-arm, randomized, double-blind, placebo-controlled trial
Sponsor Type
OTHER
Responsible Party
SPONSOR

Study Record Dates

First Submitted

December 3, 2024

First Posted

December 9, 2024

Study Start

December 1, 2024

Primary Completion

April 1, 2026

Study Completion (Estimated)

May 1, 2027

Last Updated

December 9, 2024

Record last verified: 2024-11