Platelet transfusion refractoriness is the repeated failure to achieve the desired level of

blood platelet Platelets, also called thrombocytes (from Greek θρόμβος, "clot" and κύτος, "cell"), are a component of blood whose function (along with the coagulation factors) is to react to bleeding from blood vessel injury by clumping, thereby ini ...

s in a patient following a platelet transfusion. The cause of refractoriness may be either

immune In biology, immunity is the capability of multicellular organisms to resist harmful microorganisms. Immunity involves both specific and nonspecific components. The nonspecific components act as barriers or eliminators of a wide range of pathogens ...

or non-immune. Among immune-related refractoriness, antibodies against HLA antigens are the primary cause. Non-immune causes include

splenomegaly Splenomegaly is an enlargement of the spleen. The spleen usually lies in the left upper quadrant (LUQ) of the human abdomen. Splenomegaly is one of the four cardinal signs of ''hypersplenism'' which include: some reduction in number of circulating ...

(enlargement of the spleen),

fever Fever, also referred to as pyrexia, is defined as having a body temperature, temperature above the human body temperature, normal range due to an increase in the body's temperature Human body temperature#Fever, set point. There is not a single ...

, and sepsis.

Cause

Platelet refractoriness can be due to immune causes or non-immune causes. Non-immune causes account for over 80% of cases of platelet refractoriness, and sepsis is one of the most common non-immune causes. HLA

alloimmunization Alloimmunity (sometimes called isoimmunity) is an immune response to nonself antigens from members of the same species, which are called alloantigens or isoantigens. Two major types of alloantigens are blood group antigens and histocompatibility ...

is the commonest immune cause of platelet refractoriness.

Non-immune causes

Patient-related

Sepsis Sepsis, formerly known as septicemia (septicaemia in British English) or blood poisoning, is a life-threatening condition that arises when the body's response to infection causes injury to its own tissues and organs. This initial stage is follo ...

* Fever *

Disseminated intravascular coagulation Disseminated intravascular coagulation (DIC) is a condition in which blood clots form throughout the body, blocking small blood vessels. Symptoms may include chest pain, shortness of breath, leg pain, problems speaking, or problems moving parts o ...

Splenomegaly Splenomegaly is an enlargement of the spleen. The spleen usually lies in the left upper quadrant (LUQ) of the human abdomen. Splenomegaly is one of the four cardinal signs of ''hypersplenism'' which include: some reduction in number of circulating ...

* Treatment of infection, antibiotics (vancomycin), antifungals (amphotericin B) *

Graft-versus-host disease Graft-versus-host disease (GvHD) is a syndrome, characterized by inflammation in different organs. GvHD is commonly associated with bone marrow transplants and stem cell transplants. White blood cells of the donor's immune system which remain wit ...

Hepatic veno-occlusive disease Hepatic veno-occlusive disease (VOD) or veno-occlusive disease with immunodeficiency is a potentially life-threatening condition in which some of the small veins in the liver are obstructed. It is a complication of high-dose chemotherapy given bef ...

* Bleeding

Platelet component-related

* Age of platelet component * ABO mismatch between platelet component and recipient * Number of platelets within the component if platelet increment (PI) is used to calculate platelet refractoriness * Pathogen-reduced platelet component

Immune causes

* Alloantibodies to platelet antigens ** Human leucocyte antigen (HLA) antibodies ** Human platelet antigen (HPA) antibodies *

Immune complex An immune complex, sometimes called an antigen-antibody complex or antigen-bound antibody, is a molecule formed from the binding of multiple antigens to antibodies. The bound antigen and antibody act as a unitary object, effectively an antigen of ...

es * Other antibodies ** Drug-related antibodies

Diagnosis

Platelet transfusion refractoriness can be defined in several different ways. All measures of platelet refractoriness are defined by the timing of the post-transfusion platelet count, usually 1 hour post transfusion or 24 hours post transfusion or both.

Platelet increment (PI)

This is the simplest method, and only requires data on the platelet count before and after the transfusion. The platelet increment is also known as the absolute count increment and count increment. PI = post-transfusion platelet count - pre-transfusion platelet count However, it is affected by the number of platelets given in the transfusion (platelet dose) and the patient's blood volume. Larger patients and smaller platelet doses decrease the platelet increment. These factors are adjusted for in the other methods of defining platelet refractoriness. A 1-hour post-transfusion PI of less than 5 to 10 x 10⁹/l is considered evidence of platelet refractoriness. Due to lack of data on platelet dose this is often the only measure of platelet refractoriness that can be performed in routine clinical practice.

Percentage platelet recovery (PPR)

Requires data on the platelet increment (PI), the patient's total blood volume (TBV) - estimated using the patient's weight multiplied by 0.075, and the number of platelets transfused (platelet dose) PPR = ((PI x TBV)/PD) x 100 At 1 hour post-transfusion, a PPR < 20% is considered evidence of platelet refractoriness. At 16 hours post-transfusion a PPR < 10% is considered evidence of platelet refractoriness.

Percentage platelet increment (PPI)

PPI is very similar to the percentage platelet recovery (PPR) but there has been an additional adjustment for splenic pooling of platelets (PPR multiplied by 2/3) PPI = PPR/0.67 = ((PI / 0.67) x TBV)/PD x 100

Corrected count increment (CCI)

This requires data on the platelet increment (PI, in platelets/µl), the patient's

Body surface area In physiology and medicine, the body surface area (BSA) is the measured or calculated surface area of a human body. For many clinical purposes, BSA is a better indicator of metabolic mass than body weight because it is less affected by abnormal ad ...

(BSA, in m²), and the number of platelets transfused (PD, in 10¹¹).

= PI * \frac

For example, a PI of 25,000 platelets/µl, a BSA of 1.8m² and a PD of 4x10¹¹ gives a CCI of 11,250 platelets*m²/10¹¹µl At 1 hour post-transfusion a CCI greater than 7500 indicates a sufficient post-transfusion increment, whereas a CCI less than 7500 is considered diagnostic of platelet refractoriness. At 24 hours post transfusion a CCI less than 5000 suggests platelet refractoriness.

Platelet dose

Some blood banks maintain records of the estimated number of platelets in each unit. Current requirements in the US stipulate that a unit of apheresis platelets must contain at least 3.0 x10¹¹ platelets. In England only 1% of adult platelet components are tested to check the number of platelets meet the minimum required standard of 2.4 x 10¹¹ platelets. Only components that contain fewer than 1.6 x 10¹¹ platelets are discarded. This means that there can be a lot of variability in the number of platelets contained within each transfusion.

Treatment

Treatment depends on the underlying cause. Non-immune causes are usually treated by treating the underlying cause e.g.

sepsis Sepsis, formerly known as septicemia (septicaemia in British English) or blood poisoning, is a life-threatening condition that arises when the body's response to infection causes injury to its own tissues and organs. This initial stage is follo ...

. If there is no obvious non-immune cause, a first step can be to use platelet components that are likely to produce the greatest platelet increment (less than 3 days old and ABO-matched), while further investigations are performed (testing for HLA antibodies). If an immune cause is suspected and HLA antibodies are detected, then HLA-selected platelet components can be used. Although HLA-selected platelets lead to improved platelet increments at 1 hour post-transfusion, there is currently insufficient evidence to demonstrate their clinical effectiveness at preventing bleeding. If HLA antibodies are not detected, and HPA antibodies are detected, then HPA-selected or crossmatched platelet components can be used. HLA and HPA-selected components should not be used if no HLA or HPA antibodies are detected.

References

{{reflist Transfusion reactions Coagulopathies Transfusion medicine