Genes For Intelligence On The X

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429

JMed Genet 1991; 28: 429-432

LETTERS TO
THE EDITOR

Genes for intelligence


chromosome

on

the X

Some 20 years ago Robert Lehrke, a


psychologist from Minnesota working
in a state hospital for the mentally
retarded, suggested that genes that
determine the major intellectual traits
are carried on the X chromosome.' 2
At that time Lehrke was severely
criticised on the grounds that his hypothesis was inherently improbable,3 and
that the evidence was meagre and could
be interpreted in other ways.4 5 Since
then more medical evidence has
accumulated to support two of the
steps in Lehrke's argument.
(1) "The well documented excess of males
among the mentally retarded (25-500%o)".
Two further studies6 7 have shown that
this male excess results from mutations
on the X chromosome, using as
evidence the excess of affected brothers
over affected sisters and calculating
this as a gene frequency for X linked
forms of mental retardation.
(2) "A review of families published at
that time with mental retardation showing
an X linked pattern of inheritance-which
only numbered 5, together with 5 new
families that he had identifed". In the
former group three were shown later to
have the fragile X syndrome and this
we now know is very common. A
further two had specific features, one
spasticity and the other obesity, and in
the remainder, as best as can be
judged, the clinical description fell into
the non-specific group. As we can see
in

this issue, this

the most common


are now three separate
is

form. There
localisations, MRXI, MRX2, and
MRX3, and it seems likely that more
loci will be defined in the future. His
suggestion, therefore, that X linkage
may be important, is being cemented
by fact.
Lehrke's two other arguments were
the lesser variability and reduced
extremes of intelligence in the female
when compared with the male,
which he suggested resulted from the
averaging out of the effects at different
gene

alleles through Lyonisation. He also


noted that mental retardation was
transmitted more often from mother to
child than from father to child.
If there are genes which directly
determine intellectual traits, then one
would expect that mutations of such
genes would produce phenotypes
showing only effects on intelligence,
perhaps with secondary effects on
behaviour and personality. If so, there
should also be no somatic changes, no
recognisable metabolic abnormalities,
no other neurological signs, and no
progression with age, although the
effects of the mutations would be less
obvious in infancy than in childhood
when intellectual thought becomes
evident. This is the clinical picture
of non-specific mental retardation.
Clinical descriptions of autosomal
dominant and recessive forms of nonspecific mental retardation are rare, ill
defined, and found mainly in older
publications. The X linked forms are
common and are now being mapped on
the X chromosome. We would like to
reawaken Lehrke's hypothesis and
suggest that the mutations that we are
now locating associated with nonspecific mental retardation are those
that have determined the higher intelligence of homo sapiens.
Why should intelligence be coded
primarily on the X chromosome?
Although, as Ohno' and others have
stressed, genes on the X chromosome
have been conserved throughout
mammalian evolution we have to
suppose that, in man, additional genes
for intelligence have arisen there. Once
they had appeared their advantage in a
hunter-gatherer society would assure
male dominance and rapid dissemination throughout the group.9 In recent
correspondence on this subject Ohno
philosophised: "Most mammalian
species, including our own, are noticeably sexually dimorphic. As a rule such
species practice the polygamous, more
precisely the polygynous, mating
system; after exhaustive combat
between adult males, only the victor
gains possession of a large number of
females. Is it not ironic if the reward
of a victor has been to transmit his
intelligence only to his daughters and
never to his sons. If the main genetic
source of intelligence resides on the
X chromosome, man, at least, should
have organised the matriarchial society
with the polyandrous mating system.

Perhaps we are still paying for the


mistake of organising the patriarchal
society of kings and dukes."
GILLIAN TURNER
Department of Medical Genetics,
Prince of Wales Children's
Hospital, Sydney,
NSW 2031, Australia.
MICHAEL W PARTINGTON
Regional Medical Genetics Unit,
Western Suburbs Hospital,
Newcastle, NSW, Australia.
1 Lehrke R. A theory of X-linkage of
major intellectual traits. Am J Ment
Deftc 1972;76:611-9.
2 Lehrke R. X-linked mental retardation
and verbal disability. Birth Defects.
1974;X: 1.
3 Nance WE, Engel E. One X and four
hypotheses: response to Lehrke's 'A
theory of X-linkage of major intellectual
traits'. Am J Ment Defic 1972;76:
623-5.
4 Anastasi A. Four hypotheses with a
dearth of data: response to Lehrke's 'A
theory of X-linkage of major intellectual
traits'. AmJ Ment Defic 1972;76:620-2.
5 Opitz JM. On the gates of hell and a most
unusual gene. Am J Med Genet 1986;
23: 1-20.
6 Turner G, Turner B. X-linked mental
retardation. J Med Genet 1974;11:
109-13.
7 Herbst DS, Miller JR. Non-specific
X-linked mental retardation. The
frequency in British Columbia.
AmJ Med Genet 1980;7:461-9.
8 Ohno S. Sex chromosomes and sex linked
genes. Berlin: Springer Verlag, 1967.
9 Vogel F, Motulsky A. Human genetics.
Berlin: Springer Verlag, 1979:529.

X linked complicated spastic


paraplegia, MASA syndrome, and
X linked hydrocephalus owing to
congenital stenosis of the aqueduct
of Sylvius: variable expression
of the same mutation at Xq28

Hereditary 'pure' spastic paraplegia is a


disorder characterised by progressive
spasticity of the legs in otherwise
normal subjects. In the majority of
families pedigree data are in accordance
with autosomal dominant inheritance,
but X linked recessive transmission has
also been documented.' In the 'complicated' form the spasticity may be
combined with a variety of one or more
symptoms, such as mental retardation,
micro- and macrocephaly, epilepsy,
and ocular symptoms.2 3
In 1974 Blanchine and Lewis4
delineated, on the basis of clinical and

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