Plemel v. Walter

735 P.2d 1209, 303 Or. 262
CourtOregon Supreme Court
DecidedApril 21, 1987
Docket549; CA A34015; SC S33117
StatusPublished
Cited by21 cases

This text of 735 P.2d 1209 (Plemel v. Walter) is published on Counsel Stack Legal Research, covering Oregon Supreme Court primary law. Counsel Stack provides free access to over 12 million legal documents including statutes, case law, regulations, and constitutions.

Bluebook
Plemel v. Walter, 735 P.2d 1209, 303 Or. 262 (Or. 1987).

Opinion

*264 LENT, J.

In this filiation proceeding the jury, by a 9-3 vote, found that Brent Walter was the father of Dena Plemel’s child. Plemel’s expert witness testified that blood tests of Plemel, Walter and the child did not exclude the possibility that Walter was the father. Walter did not challenge the validity of the tests or the failure of the tests to exclude him but did object, on grounds of irrelevance and prejudice, to testimony by the expert regarding the probability that he was the father. The trial court permitted the testimony, and the Court of Appeals affirmed, Plemel v. Walter, 80 Or App 250, 721 P2d 474 (1986). Because we hold that the testimony was inadmissible in the form that it was presented, we reverse and remand for a new trial.

I.

Plemel’s child was born on June 9,1983. Pursuant to ORS 109.125, she initiated filiation proceedings against Walter, alleging that he was the father of the child. Subsequently, the state intervened as a petitioner. Walter denied paternity.

Plemel testified that she and Walter had intercourse on one occasion, September 11,1982. Walter admitted having intercourse with Plemel but testified that it had occurred on the night of August 13-14, 1982. Both Plemel and Walter introduced the testimony of witnesses to corroborate their respective versions of when they had been together. A nurse practitioner who had examined Plemel testified that conception of the child would have been impossible in mid-August; she estimated that conception occurred between September 9 and September 16.

Plemel also called as a witness Dr. E. W. Lovrien, the director of the Oregon Health Sciences University Phenotype Laboratory. The laboratory had conducted blood tests of Plemel, Walter and the child. Lovrien testified that: (1) the tests did not exclude the possibility that Walter was the father; (2) the probability that the tests would have excluded a “falsely accused father” was 97.5 percent; (3) Walter’s “paternity index” was 178; (4) Walter’s “chance of paternity” was 99.4 percent; (5) Walter’s “chance of nonpaternity” was 0.6 percent; and (6) it was “extremely likely” that Walter was the father. The last three statements were essentially equivalent to, and derived from, the paternity index. The “chance of *265 paternity” was the “paternity index” stated as a percentage chance (i.e., odds of 178 to 1 are equal to a 99.4 percent chance); the “chance of nonpaternity” was the “chance of paternity” stated negatively; the expression “extremely likely” was taken from a table developed by a joint committee of the American Medical Association and the American Bar Association 1 to express the significance of any given “chance of paternity.”

Walter, by way of a motion in limine and an objection, sought to exclude that portion of Lovrien’s testimony related to the paternity index and its equivalents. He argued that the testimony was irrelevant because the “probability of excluding a falsely accused father” provided the jury with all of the information that could be obtained from the blood tests. The argument was premised on his contention that in order to derive the paternity index, Lovrien had made an arbitrary assumption about the strength of the other evidence presented in the case. Walter also argued that the testimony was prejudicial in that the jury would be too confused by it to understand its proper significance. The trial court, without stating its reasons, denied Walter’s motion in limine and overruled his objection. The Court of Appeals affirmed, holding that the testimony regarding the paternity index helped the jury to interpret the blood test results and that Lovrien’s testimony minimized any potential for jury confusion by clearly explaining the limited significance of the statistics he presented. 80 Or App at 253-54.

Because courts have so frequently misinterpreted the meaning and significance of paternity test results, see, e.g., McCormick, Evidence § 211 (3rd ed 1984) (and cases cited therein); Ellman & Kaye, Probabilities and Proof: Can HLA and Blood Group Testing Prove Paternity?, 54 NYU L Rev 1131 (1979) (and cases cited therein), we believe that some background is appropriate before we analyze Walter’s arguments. 2

*266 Lovrien referred to the group of blood tests performed in this case as an “extended red cell enzyme” test. This group of tests reveals the presence of various antigens, red cell enzymes and plasma proteins in the blood. By knowing which of these substances are in the blood of the mother, child and putative father, a geneticist can state whether it is possible for the putative father to be the true father.

Each person has a large number of inherited traits, such as eye color and facial features. Different versions of a particular trait are known as phenotypes. For the inherited trait of eye color, for example, blue eyes are one phenotype, brown eyes are another. The antigens, enzymes and proteins in a person’s blood are also inherited traits. One set, or “system,” of antigens are the ABO antigens, which have been widely used in the classification of blood. Because no individual possesses every antigen in the ABO system, the ABO antigens that an individual does possess determine that individual’s “blood type,” or phenotype, for the ABO system. The ABO system can be divided into six phenotypes: O, A1; A2, B, AjB or A2B. See Joint AMA-ABA .Guidelines: Present Status of Serological Testing in Problems of Disputed Parentage, 10 Fam LQ 247, 263 (1976). If a person has the phenotype Aj, this means that a blood test revealed the presence of the Ax antigen. Similarly, if a person has the phenotype AXB, the blood test revealed the presence of both the A1 antigen and the B antigen. If the person’s phenotype is O, the blood test was unable to detect the presence of any of the antigens for the ABO system.

The specific set of phenotypes that a person possesses is determined by that person’s genes. Genes occur in pairs that contain one gene from each parent. A specific gene pair or a specific group of gene pairs control a particular body trait, and an individual’s phenotype for that trait will reflect the nature of the genes that make up the controlling pair or pairs. If a person has the phenotype AXB, that person’s ABO gene pair consists of an A1 gene and a B gene. If the phenotype is A2, the pair consists of an A1 gene and either another Ax gene or an O gene. This is because the 0 gene does not produce a detectable antigen. See Reisner & Bolk, A Layman’s Guide to the Use of Blood Group Analysis in Paternity Testing, 20 J Fam L 657, 662 (1982). If the phenotype is O, both genes are O.

*267 Information about a person’s phenotypes, then, can be used to derive information concerning that person’s corresponding gene pairs.

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Bluebook (online)
735 P.2d 1209, 303 Or. 262, Counsel Stack Legal Research, https://law.counselstack.com/opinion/plemel-v-walter-or-1987.