Familial Alzheimer Disease

Approximately 25% of all AD is familial (i.e., ≥3 persons in a family have AD) and 75% is nonfamilial (i.e., an individual with AD and no known family history of AD). Because familial AD and nonfamilial AD appear to have the same clinical and pathologic phenotypes, they can only be distinguished by family history and/or by molecular genetic testing.

Risk to Family Members – Nonfamilial Alzheimer Disease

Genetic counseling for people with late-onset nonfamilial AD (i.e., an individual with AD and no known family history) and their family members must be empiric and relatively nonspecific. First-degree relatives of a person with nonfamilial AD have a cumulative lifetime risk of developing AD of approximately 15%-39%, which is typically reported as a 20%-25% risk [Farrer et al 1989, Silverman et al 1994, Lautenschlager et al 1996]. This risk is approximately two to three times that of the background risk (~27% vs 10.4%) [Cupples et al 2004].

Disagreement exists as to whether the age of onset of AD in a person with nonfamilial AD changes the risk to first-degree relatives. Silverman et al [2005] found that the risk to relatives of a proband with nonfamilial AD decreases with increasing age of onset of the proband.

Risk to Family Members – Late-Onset Familial Alzheimer Disease (LOFAD)

Inheritance of LOFAD (i.e., ≥3 persons in a family have AD) is thought to be multifactorial and potentially involve multiple susceptibility genes [Van Cauwenberghe et al 2016]. First-degree relatives of a person with LOFAD have a cumulative lifetime risk of developing AD of ~15%-25%, which is ~1.5-2 times the risk of the general population. When both parents have AD (i.e., conjugal AD) risk to their children is at least twice that of the general population risk [Jayadev et al 2008].

Risk to Family Members – APP-, PSEN1-, or PSEN2-Related Early-Onset Familial Alzheimer Disease (EOFAD)

EOFAD in which an individual has a pathogenic variant in APP, PSEN1, or PSEN2 represents an autosomal dominant disease. This section refers only to families having a known EOFAD-causing APP, PSEN1, or PSEN2 pathogenic variant. Guidelines for counseling these families have been published [Goldman et al 2011].

Parents of a proband

• Most individuals diagnosed as having APP-, PSEN1-, or PSEN2-related EOFAD have had an affected parent.
  • Because the onset of EOFAD is typically in early adulthood and the progression is rapid, affected parents are not alive at the time of diagnosis of their children.
  • Occasionally, neither parent is identified as having had AD, but a second-degree relative (e.g., an uncle, aunt, and/or grandparent) has or had EOFAD. In this instance, a parent of the proband is presumed to be heterozygous for a familial AD-causing pathogenic variant associated with reduced (age-related) penetrance.
• A proband with EOFAD may have the disorder as the result of a de novo pathogenic variant, although this has not been documented.
• The family history of some individuals diagnosed with EOFAD may appear to be negative because of failure to recognize the disorder in family members, early death of the parent before the onset of symptoms, or reduced (age-related) penetrance. Therefore, an apparently negative family history cannot be considered confirmed unless appropriate clinical evaluation and/or molecular genetic testing has been performed on the parents of the proband.

Sibs of a proband. The risk to sibs depends on the clinical/genetic status of the parents:

• If a parent of the proband was affected and/or is known to be heterozygous for an APP-, PSEN1-, or PSEN2-related EOFAD pathogenic variant, the risk to sibs of having inherited the variant is 50%.
• Sibs of a proband with clinically unaffected parents are still presumed to be at increased risk for EOFAD because of the possibility of reduced (age-related) penetrance in a parent.

Offspring of a proband. Each child of an individual with APP-, PSEN1-, or PSEN2-related EOFAD has a 50% chance of inheriting the EOFAD-causing pathogenic variant.

Other family members. The risk to other family members depends on the status of the proband's parents: if a parent has the pathogenic variant, the parent's family members may be at risk.

Related Genetic Counseling Issues

Predictive testing for APP-, PSEN1-, or PSEN2-related EOFAD (i.e., testing of asymptomatic at-risk individuals)

• Predictive testing for asymptomatic adults at risk for APP-, PSEN1-, or PSEN2-related EOFAD is possible if the pathogenic variant has been identified in an affected family member. It should be remembered that testing of asymptomatic at-risk individuals with nonspecific or equivocal symptoms is predictive testing, not diagnostic testing.
• Potential consequences of such testing (including, but not limited to, socioeconomic changes and the need for long-term follow up and evaluation arrangements for individuals with a positive test result) as well as the capabilities and limitations of predictive testing should be discussed in the context of formal genetic counseling prior to testing.

Predictive testing for APP-, PSEN1-, or PSEN2-related EOFAD in minors (i.e., testing of asymptomatic at-risk individuals younger than age 18 years)

• For asymptomatic minors at risk for adult-onset conditions for which early treatment would have no beneficial effect on disease morbidity and mortality, predictive genetic testing is considered inappropriate, primarily because it negates the autonomy of the child with no compelling benefit. Further, concern exists regarding the potential unhealthy adverse effects that such information may have on family dynamics, the risk of discrimination and stigmatization in the future, and the anxiety that such information may cause.
• For more information, see the National Society of Genetic Counselors position statement on genetic testing of minors for adult-onset conditions and the American Academy of Pediatrics and American College of Medical Genetics and Genomics policy statement: ethical and policy issues in genetic testing and screening of children.

In a family with an established diagnosis of EOFAD, it is appropriate to consider testing of symptomatic individuals regardless of age.

APOE genotyping. At this time, it is generally agreed that APOE genotyping has little role in predictive testing. The presence of one or two copies of the APOE e4 allele increases the lifetime risk of AD in an asymptomatic individual but does not constitute a diagnosis of AD (i.e., an individual may have one or two copies of the APOE e4 allele and never develop AD). Likewise, absence of one or two copies of the APOE e4 allele does not eliminate the risk for AD in an asymptomatic individual (~42% of persons with AD do not have an APOE e4 allele).

• APOE e4/e4
  • A young asymptomatic female who is homozygous for the APOE e4 allele has a 40%-45% probability of developing AD by age 75 years, compared with 10%-15% probability in the general female population.
  • A young asymptomatic homozygous male has a 25%-30% risk of developing AD by age 80 years, compared with 10%-15% probability in the general male population [Breitner et al 1999, Qian et al 2017, Liu & Caselli 2018].
• APOE e3/e4. For an asymptomatic person heterozygous for an APOE e4 allele, the lifetime risk of developing AD is lower (15%-25%) and the likely age of onset is later (peak age 80s) [Breitner et al 1999, Neu et al 2017, Qian et al 2017].

See the Statement of The Alzheimer's Foundation of America (AFA) and AFA's Medical, Scientific and Memory Screening Advisory Board on Genetic Testing to Determine Risk of Alzheimer's Disease and Frank et al [2018] for further discussion of predictive testing for AD.

Revision History

• 20 December 2018 (bp) Comprehensive update posted live
• 30 March 2010 (me) Comprehensive update posted live
• 9 May 2007 (me) Comprehensive update posted live
• 10 February 2005 (me) Comprehensive update posted live
• 29 January 2003 (me) Comprehensive update posted live
• 23 October 1998 (me) Overview posted live
• Spring 1996 (tb) Original submission

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