Neonatal heel prick

(Redirected from Guthrie test)

The neonatal heel prick is a blood collection procedure done on newborns. It consists of making a pinprick puncture in one heel of the newborn to collect their blood. This technique is used frequently as the main way to collect blood from neonates. Other techniques include venous or arterial needle sticks, cord blood sampling, or umbilical line collection. This technique is often utilized for the Guthrie test, where it is used to soak the blood into pre-printed collection cards known as Guthrie cards.[1][2]

The blood of a two-week-old infant is collected for a Phenylketonuria, or PKU, screening

The classical Guthrie test is named after Robert Guthrie, an American bacteriologist and physician who devised it in 1962. The test has been widely used throughout North America and Europe as one of the core newborn screening tests since the late 1960s. The test was initially a bacterial inhibition assay, but is gradually being replaced in many areas by newer techniques such as tandem mass spectrometry that can detect a wider variety of congenital diseases.

Detected diseases edit

The blood samples can be used for a variety of metabolic tests to detect genetic conditions, including:

Mechanism edit

The test uses the growth of a strain of bacteria on a specially-prepared agar plate as a sign for the presence of high levels of phenylalanine, phenylpyruvate, and/or phenyllactate. The compound B-2-thienylalanine will inhibit the growth of the bacterium Bacillus subtilis (ATCC 6051) on minimal culture media. If phenylalanine, phenylpyruvate, and/or phenyllactate is added to the medium, then growth is restored. Such compounds will be present in excess in the blood or urine of patients with PKU. If a suitably-prepared sample of blood or urine is applied to the seeded agar plate, the growth of the bacteria in the test will be a positive indicator for PKU in the patient.[4]

To prepare the sample for application, a small amount of blood (from a heel puncture, for example) or urine (from a diaper, for example) is applied to a piece of filter paper. Then a small disc is punched from the center of the spot of blood or urine, and the disc applied to the surface of a seeded, minimal-medium agar plate that contains added beta-2-thienylalanine. If the sample contains phenylalanine, phenylpyruvate, and/or phenyllactate then these compounds will diffuse into the agar medium. If their concentrations are high enough (as with the excess levels seen with PKU), bacteria will grow under the disc, but not elsewhere. Generally an overnight incubation is enough to determine whether phenylalanine, phenylpyruvate, and/or phenyllactate are present in unusual concentrations in blood or urine.[4]

Timing edit

The blood spot sample should be taken between 48 and 72 hours of age for all babies regardless of medical condition, milk feeding and prematurity. For the purpose of screening, date of birth is day 0 (some IT systems record date of birth as day 1).[5] False positives and false negatives can sometimes occur when the screening tests are performed before 48 hours.[6]

When the immunoassay method is utilized as a screening method for quantifying 17α-hydroxyprogesterone (17OHP) in dried blood spots, it exhibits a significant rate of false positive results. As per the clinical practice guideline issued by the Endocrine Society in 2018, employing LC-MS/MS to measure 17OHP and other adrenal steroid hormones (such as 21-deoxycortisol and androstenedione) is recommended as a supplementary screening approach to enhance the accuracy of positive predictions.[7]

With genetic tests becoming more common, a wide variety of tests may use the blood drawn by this method. Many neonatal units (SCBUs) now use this method to carry out the daily blood tests (blood count, electrolytes) required to check the progress of ill neonates.[citation needed]

Data retention controversy edit

In Ireland, a controversy emerged in 2012 whereby a number of hospitals retained heel prick test cards and thereby a DNA database with over a million samples from 1984, without consent or notification of parents. This resulted in a ten-year rolling destruction cycle being introduced. Similar practices exist in the United Kingdom, New Zealand, and several states of the United States. [8]

See also edit

References edit

  1. ^ Guthrie Cards Archived 2016-12-01 at the Wayback Machine, Catalyst (ABC1), 29 May 2003.
  2. ^ Julia A. McMillan; Ralph D. Feigin; Catherine DeAngelis; M. Douglas Jones (1 April 2006). Oski's pediatrics: principles & practice. Lippincott Williams & Wilkins. pp. 162–. ISBN 978-0-7817-3894-1. Retrieved 16 April 2010.
  3. ^ "NHS Screening antenatal and newborn". Archived from the original on 2009-02-12. Retrieved 2009-02-26.
  4. ^ a b "PHE-TST001". uic.edu. Archived from the original on 2013-09-27.
  5. ^ "Standards". screening.nhs.uk. Archived from the original on 2009-05-01. Retrieved 2015-02-07.
  6. ^ "Newborn screening guidelines". health.vic.gov.au (via archive.org). Archived from the original on 2006-03-08.{{cite web}}: CS1 maint: bot: original URL status unknown (link)
  7. ^ Mu D, Sun D, Qian X, Ma X, Qiu L, Cheng X, Yu S (December 2023). "Steroid profiling in adrenal disease". Clin Chim Acta. 553: 117749. doi:10.1016/j.cca.2023.117749. PMID 38169194.
  8. ^ "International standards for storing samples vary wildly". Irish Times. Archived from the original on 2015-04-02. Retrieved 2015-03-25.

External links edit