Kleihauer-Betke test

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The Kleihauer-Betke ("KB") test, Kleihauer-Betke ("KB") stain or Kleihauer test, is a blood test used to measure the amount of fetal hemoglobin transferred from a fetus to an Rh-negative mother's bloodstream.[1] The results of the test are used to determine the required dose of Rh immune globulin (RhIg) to inhibit formation of Rh antibodies in the mother and prevent Rh disease in future Rh-positive children.

In this test, hemoglobin is eluted from the mother's red blood cells, whereas the fetal hemoglobin is resistant to this acid elution. When the slides are stained, the maternal cells appear very pale, whereas fetal cells are stained and appear bright pink. Simple comparative counts allow an estimate of whether a significant fetal-maternal hemorrhage has occurred.

In those with positive tests (25% or more of estimated fetal blood volume lost), follow up testing (at a postpartum check) should be done to rule out the possibility of a false positive because of a process, e.g. sickle cell trait, in the mother which causes persistent elevation of fetal hemoglobin.

The KB test is the standard method of detecting fetal-maternal hemorrhage (FMH). This takes advantage of the differential resistance of fetal hemoglobin to acid. A standard blood smear is prepared from the mother's blood. An acid bath is then used to remove all adult hemoglobin but does not remove fetal hemoglobin. Subsequent staining makes fetal cells (containing fetal hemoglobin) appear rose-pink in color, while adult cells are only seen as 'ghosts'. A large number N \geq 5000 of cells are counted under the microscope and a ratio of fetal to maternal cells generated.

Comparison with other more expensive or technologically advanced methods such as flow cytometry has shown that the KB stain, like the more advanced methods, is sensitive in its detection of FMH.[1] Background counting errors can result in estimates of as much as 5 ml fetal blood loss when there actually is no such blood loss, but standard methods available in most laboratories admit an extremely low probability of the return of a false positive when more severe FMH has taken place.

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[edit] Estimating the Severity of FMH

To determine if a positive test for FMH should be considered as the likely cause of fetal death, the percent of total fetal blood volume lost should be calculated, making appropriate adjustments based on the following known relationships:

    • the size of a fetal red blood cell is 1.22 times that of an adult red blood cell;
    • the KB stain is known to have a mean success rate of 92% in detecting fetal red blood cells;
    • in a woman at or near term in her pregnancy, the mean volume of maternal red blood cells is approximately 1800 ml;
    • the mean fetal hematocrit is 50%; and
    • at stillbirth, the mean fetal blood volume is 150 \frac{ml}{kg}

These constraints can then be applied to yield the formula

PFB = \frac{(3200)(FC)}{(FW)(MC)}

where

    • PFB is the percentage of fetal blood lost;
    • FC is the observed number of fetal red blood cells;
    • MC is the observed number of maternal red blood cells (N.B. we have that MC = TCFC, where TC is the total observed number of red blood cells, both maternal and fetal);
    • FW is the stillbirth weight of the fetus in kilograms.

[edit] An Example of How This Formula is Used in Resolving a Stillbirth

Suppose that a KB stain is performed and TC = 5000 total red blood cells are observed, FC = 200 of which are found to be fetal red blood cells. Suppose further that the stillbirth weight of the fetus under consideration is FW = 2.0kg. Then we would conclude that the total percentage of fetal blood lost is approximately

PFB = \frac{(3200)(FC)}{(FW)(MC)} = \frac{(3200)(200)}{(2.0)(4800)} = \frac{200}{3} = 66.667

to five significant digits. We would hence conclude that the fetus under consideration lost 66.667% (two thirds) of its blood via FMH. Generally, stillbirth is highly probable for any value of PFB \geq 20, particularly if the fetus abruptly loses this much blood; in this example, we would hence be likely to suspect FMH as the cause of the stillbirth. It is important to note, however, that such a diagnosis is still not completely conclusive; fetuses losing large quantities of blood over long periods of time are able to compensate for this slower blood loss; since the KB stain tells us nothing with regard to the level of acuity of FMH. This means that it is not possible to entirely correlate a positive KB stain and high PFB with a stillbirth, though in many cases, such as the stillbirth of Breanna Lynn Bartlett-Stewart in 2000, given other information, such as known hereditary complications of pregnancy, extremely high positive correlation coefficients r \approx +1.000 between FMH and stillbirth have been observed.

[edit] Problems in the Detection of Fetal Red Blood Cells

Since fetal and maternal blood cells have the same life expectancy in the maternal bloodstream, it is possible to obtain informative results from a KB stain for a fair period of time after a stillbirth. However, if the mother and fetus are ABO incompatible, it is more crucial to quickly perform the KB stain following a stillbirth, as the fetal red blood cells will be eliminated from the maternal bloodstream very quickly, causing the KB stain to underestimate the degree of FMH, if any.

Lots of concern has been raised in the literature concerning false positives when sampling is done after delivery. In general this is not a problem. Delivery does result in higher frequency of detection of micro-hemorrhages but this should not confound interpretation of FMH as a possible cause of stillbirth. It is not necessary to draw the sample before induction, onset of labor, delivery, placental delivery etc. despite what some published literature purports. However, if caesarean section is to be used, failure to draw the sample prior to that will result in a 2% false positive rate.

Finally, anything which causes persistence of fetal hemoglobin in maternal blood cells will make interpretation much trickier. Certain hemoglobinopathies, the most common of which is sickle cell trait, do this. Overall, somewhere around 1-3% of the time this could result in false interpretation.

[edit] See also

[edit] References

  1. ^ a b Katiyar R, Kriplani A, Agarwal N, Bhatla N, Kabra M (2007). "Detection of fetomaternal hemorrhage following chorionic villus sampling by Kleihauer Betke test and rise in maternal serum alpha feto protein". Prenat. Diagn. 27 (2): 139–42. doi:10.1002/pd.1632. PMID 17191260. 
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