Thrombocytopenia Clinical Trial
— CATCHOfficial title:
Characterization of New Candidate Genes in Cases of Human Inherited Thrombocytopenia (CATCH). Molecular Etiologies in Cases of Thrombocytopenia
Verified date | February 2020 |
Source | Institut National de la Santé Et de la Recherche Médicale, France |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
Circulating blood platelets are small cellular elements that help to control bleeding (a
process called hemostasis) and to avoid hemorrhage when blood vessels are injured. Platelets
originate from cells in the bone marrow, the megakaryocytes (MKs), following a complex
process of morphological transformation and maturation, which finally leads to the production
of blood platelets. Multiple genes are implicated in this process. Constitutive
thrombocytopenia (CT) are rare hematological diseases characterized by a decreased number of
circulating platelets that are often larger than normal, that may lead to more or less severe
hemorrhagic events. However, CT can be difficult to diagnose and differentiate from various
forms of acquired thrombocytopenia. The ultimate diagnosis for CT is thus based on the
molecular diagnosis, obtained by identifying and characterizing the abnormal gene and
protein. About 40 genes / proteins have been identified so far as causal in CT, however, in
about half of the patients suspected to have CT, genomic analysis does not detect a variant
in one of these genes, and etiology of CT thus remains unknown. But insuring the diagnosis of
CT is important: it will avoid misdiagnosis and inefficient or deleterious therapeutic
interventions, while allowing a proposal of an adapted curative/preventive medical action. At
the Resource and Competence Center for Constitutional Hemorrhagic Diseases (CRCMHC)
(University Hospital Robert Debré, Paris, France), the investigating team has evidenced in
unrelated patients presenting with familial forms of thrombocytopenia and no known molecular
diagnosis, variants of genes not yet described as formally implicated in the occurrence of
CT. Molecular genetic evidence must be completed by functional studies. Such functional
studies are conducted in a research laboratory from the National Institute for Health and
Medical Research (Inserm), "Innovative Therapies in Haemostasis (IThEM)" (Faculty of Medical
Sciences, University of Paris, Paris, France), and include:
- an evaluation of how blood progenitor cells mature into MKs, by comparing cells obtained
from patients to those of members free of the disease (the latter taken as normal
control subjects);
- an evaluation of platelet functionalities, such as ability to form a blood clot similar
to what happens during hemostasis, with the aim to detect not only quantitative (number
and size) but also any qualitative (functions) defects;
- an evaluation of the ultrastructure (the structure of intracellular components) and
biochemistry of MKs and platelets, focusing on the molecular pathways the variant
protein is implicated in.
This clinical trial is aimed to precisely delineate the mechanism of action of newly
identified CT genetic variants, and will fulfill the aims of (1) offering the patient(s) a
formal molecular diagnosis of CT, (2) ameliorating patients' medical support, both for
diagnosis and therapy, (3) providing patients and family members with a pertinent genetic
counseling, and (4) expanding the validated panel of genes implicated in CT to be explored in
new suspected cases of CT. It will also help in extending the basic knowledge of the process
of MK and platelet formation.
Status | Enrolling by invitation |
Enrollment | 40 |
Est. completion date | December 2024 |
Est. primary completion date | July 2024 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 11 Years to 65 Years |
Eligibility |
Inclusion Criteria: - platelet count < 150.000/µl for at least 6 months - thrombocytopenia in at least one family member - weight > 35 kg - no pathogenic variant (already reported or suspected) in genes causative for inherited CT - harboring a variant potentially pathogenic in a gene potentially implicated in the megakaryopoiesis or platelet production, this variant being harbored also by the affected family members, and not by the non-affected family members . Exclusion Criteria: - Pregnant woman - Subject with an anemia: Hb < 8g/dl - Subject with a behavior disorder - Subject with a hemostasis disease added (Willebrand disease, hemophilia, ...) - Subject with another suspected cause of thrombopenia (drug, infection, ...) - Subject taking a drug interfering on the platelet production - Subject protected by a legal measure - Subject participating to another program research, leading to larger blood volume than authorized |
Country | Name | City | State |
---|---|---|---|
France | Resource and Competence Center for Constitutional Hemorrhagic Diseases (CRCMHC), University Hospital Robert Debré | Paris | |
France | Resource and Competence Center for Constitutional Hemorrhagic Diseases (CRCMHC), University Hospital Pontchaillou | Rennes |
Lead Sponsor | Collaborator |
---|---|
Institut National de la Santé Et de la Recherche Médicale, France |
France,
Balduini CL, Melazzini F, Pecci A. Inherited thrombocytopenias-recent advances in clinical and molecular aspects. Platelets. 2017 Jan;28(1):3-13. doi: 10.3109/09537104.2016.1171835. Epub 2016 May 9. Review. — View Citation
Boutroux H, David B, Guéguen P, Frange P, Vincenot A, Leverger G, Favier R. ACTN1-related Macrothrombocytopenia: A Novel Entity in the Progressing Field of Pediatric Thrombocytopenia. J Pediatr Hematol Oncol. 2017 Nov;39(8):e515-e518. doi: 10.1097/MPH.0000000000000885. — View Citation
Guillet B, Bayart S, Pillois X, Nurden P, Caen JP, Nurden AT. A Glanzmann thrombasthenia family associated with a TUBB1-related macrothrombocytopenia. J Thromb Haemost. 2019 Dec;17(12):2211-2215. doi: 10.1111/jth.14622. Epub 2019 Sep 29. — View Citation
Vincenot A, Saultier P, Kunishima S, Poggi M, Hurtaud-Roux MF, Roussel A, Actn Study Coinvestigators, Schlegel N, Alessi MC. Novel ACTN1 variants in cases of thrombocytopenia. Hum Mutat. 2019 Dec;40(12):2258-2269. doi: 10.1002/humu.23840. Epub 2019 Nov 6. — View Citation
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Validation of new genes potentially involved in the occurrence of CT by determination of the amount of the protein produced and its effect on the megakaryocytes producing platelets aspect in culture | Functional study of variants altering these new genes, identified in patients and their family members presenting a CT. This study will include the determination of the amount of the protein produced by the new identified gene variants (qualitative and quantitative) and its effect on the platelet production by megakaryocytes in culture. | 6 months | |
Secondary | Description of the phenotype of these new CT entities | Gathering information on a potentially associated clinical syndrome by a medical questionnaire reporting any organ dysfunction or pathology (renal impairment, deafness, malignancy, …) and collection of data of the blood cells counts. Blood cells counts will be compared to normal controls and data of the medical questionnaire will be compared between affected patients, in the aim to highlight the potential implication of the new gene variants in haematological or non haematological diseases. | 6 months | |
Secondary | Search of a potentially platelet dysfunction | Platelet function study by specialized techniques : activation and aggregation of cells (velocity, rate) in the presence of different platelet activators (ADP, collagen, thrombin) measured with aggregometer and flow immunocytometry, secretion measured with ELISA kits for specific platelet-secreted molecules and with flow immunocytometry, cell adhesion measured with optic and electronic microscopy. | 6 months |
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