The SOLID Platelet Study

National Institutes of Health Clinical Center (CC)

Status and phase

Terminated

Phase 2

Conditions

Platelet Transfusion Refractoriness (PTR)

Thrombocytopenia

Treatments

Biological: Platelet Transfusion - SHORT Platelet Transfusion

Biological: Platelet Transfusion - LONG Platelet Transfusion

Study type

Interventional

Funder types

NIH

Identifiers

NCT03712618

19-CC-0005

190005

Details and patient eligibility

About

Background:

Platelets are cell fragments in the blood that help it clot. Some people get very low platelet counts during a disease or treatment. Low platelet counts can cause severe bleeding. Some people are not helped by platelet transfusions at the standard transfusion rate. This is called platelet transfusion refractoriness (PTR). Researchers want to learn more about transfusing platelets so they can make transfusions more effective.

Objectives:

To study the effects of transfusing platelets more slowly than the standard rate. To obtain data to improve the effectiveness of platelet transfusions in people with PTR and decrease the risk of bleeding in some people.

Eligibility:

Adults ages 18-100 who have very low platelet counts requiring platelet transfusion, and have evidence of PTR

Design:

Participants will be screened with a review their recent NIH medical records. They will have blood drawn.

Participants will have up to three 12-hour treatment blocks. They can have only one block per day. During each block, they will have 2 platelet transfusions in those 12 hours.

One transfusion will take place over 1 hour (SHORT infusion). The other will take place over 4 hours (LONG infusion).

Participants will be randomly put in 1 of 2 treatment groups. This will dictate whether they get the SHORT or LONG infusion first.

Participants will have blood drawn:

When they enroll
Right before each transfusion
2, 4, and 6 hours after each transfusion

Each blood draw will consist of a complete blood count. Smaller tubes that require only small amounts of blood will be used to minimize the amount of blood drawn.

Full description

Platelet transfusion can be a life-saving procedure in preventing or treating serious bleeding in patients who have low and/or dysfunctional platelets. Treatment of blood cancer and other blood diseases, as well as bone marrow transplantation, is not possible without platelet transfusion support. Unfortunately, 15- 25% of chronically transfused patients platelet counts will stop responding to these transfusions, putting them at risk for serious bleeding complications. The development of human leukocyte antigen (HLA) antibodies is responsible for 4- 8% of this platelet transfusion refractoriness. The presence of HLA antibodies is a clinical complication that is generally managed by the selection of products that are negative for the antigens for which the patient has antibodies. Often, for patients with chronic and ongoing need, this selection is facilitated by targeted recruitment of donors with known HLA types (i.e., types that lack antigens cognate to the patients known antibodies and are thus predicted to be compatible). However, for very broadly HLA- alloimmunized patients, compatible products may be exceedingly scarce or completely unavailable, precluding the ability to consistently provide products the patient will likely increment from. This research protocol is designed to evaluate the efficacy of a 4-hour continuous infusion of single donor, apheresis platelets in overcoming both alloimmune-mediated and non-alloimmune-mediated platelet refractoriness. We hypothesize that when we transfuse patients over a long duration, who have platelet refractoriness, the platelet counts will increase to higher numbers for an extended period of time in the peri-transfusion period when compared to shorter transfusion intervals.

Enrollment

2 patients

Sex

All

Ages

18 to 100 years old

Volunteers

No Healthy Volunteers

Inclusion and exclusion criteria

INCLUSION CRITERIA:
Ability to comprehend the investigational nature of the study and provide informed consent
Thrombocytopenia
- Causes of thrombocytopenia may be due to:
  1. Congenital causes
  2. Bone marrow
  3. Hematologic malignancies
  4. Treatment related
- Thrombocytopenia is generally defined as one of the following:
  1. Platelet count <10K/uL without bleeding
  2. Platelet count <20K/uL for "complicated prophylaxis" in patients determined to be at increased risk of bleeding or other complications
  3. Platelet count <50K/uL with evidence of active bleeding, such as intracranial hemorrhage, GI bleeding, pulmonary hemorrhage, uncontrolled epistaxis, hematuria.
    
    The treating provider may change the platelet transfusion threshold based on the clinical circumstance, patient population, and/or concurrent primary protocol considerations - similar to the PLADO study.
Diagnosed with PTR, characterized by the following:
- Lack of adequate post-transfusion platelet count increment, defined by, Corrected Count Increment (CCI) <5000/ul at 10-60 min after each of at least 2 consecutive platelet transfusions
- Presence of anti-HLA class 1 type A and/or type B antibody, in the setting of PTR, as defined above, constitutes the HLA alloimmune-mediated subtype of PTR. Presence of one or more HPA antibodies in the setting of PTR, as defined above, constitutes the HPA alloimmune-mediated subtype of PTR. Failure to detect HLA or HPA antibodies will be categorized as non-alloimmune-mediated PTR. .

EXCLUSION CRITERIA:

Less than 18-years-old
Lack of ability to obtain informed consent
Pregnant female
Presence of ITP/autoimmune thrombocytopenia
Immune platelet refractoriness responsive to treatment with IVIg or eculizumab, or other immunosuppressive therapy within the 3 preceding months. This is based on the wide variation in the duration therapeutic antibodies, with the upper limit frequently cited as 3 months.

Trial design

Primary purpose

Treatment

Allocation

Randomized

Interventional model

Crossover Assignment

Masking

None (Open label)

2 participants in 2 patient groups

Group A: LONG then SHORT transfusion

Active Comparator group

Description:

Subjects with thrombocytopenia (due to congenital causes, bone marrow failure, hematologic malignancies, and treatment-related) randomized to receive LONG platelet transfusion (Transfused over 4-HOURS via infusion pump or gravity) with follow up until 6 hours and then SHORT platelet transfusion (Transfused over 60-minutes via infusion pump or gravity) with follow up until 6 hours for a combined total of 12 hours. Subjects may receive up to two further subsequent blocks (one per day) to be administered to a subject in alternating order of SHORT and LONG platelet transfusions, for a maximum number of three blocks per subject.

Treatment:

Biological: Platelet Transfusion - LONG Platelet Transfusion

Biological: Platelet Transfusion - SHORT Platelet Transfusion

Group B: SHORT then LONG transfusion

Active Comparator group

Description:

Subjects with thrombocytopenia (due to congenital causes, bone marrow failure, hematologic malignancies, and treatment-related) randomized to receive SHORT platelet transfusion (Transfused over 60-minutes via infusion pump or gravity) with follow up until 6 hours and then LONG platelet transfusion (Transfused over 4-HOURS via infusion pump or gravity) with follow up until 6 hours for a combined total of 12 hours. Subjects may receive up to two further subsequent blocks (one per day) to be administered to a subject in alternating order of LONG and SHORT platelet transfusions, for a maximum number of three blocks per subject.

Treatment:

Biological: Platelet Transfusion - LONG Platelet Transfusion

Biological: Platelet Transfusion - SHORT Platelet Transfusion

Trial documents

Study Protocol and Statistical Analysis Plan: Prot_SAP_000.pdf

Trial contacts and locations

Central trial contact

Willy A Flegel, M.D.; Sarah Pogue, R.N.

Data sourced from clinicaltrials.gov

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