Nothing Special   »   [go: up one dir, main page]

Jump to content

Y chromosome

From Wikipedia, the free encyclopedia
(Redirected from YDNA)

Human Y chromosome
Human Y chromosome (after G-banding)
Y chromosome in human male karyogram
Features
Length (bp)62,460,029 bp (CHM13)
No. of genes63 (CCDS)[1]
TypeAllosome
Centromere positionAcrocentric[2]
(10.4 Mbp[3])
Complete gene lists
CCDSGene list
HGNCGene list
UniProtGene list
NCBIGene list
External map viewers
EnsemblChromosome Y
EntrezChromosome Y
NCBIChromosome Y
UCSCChromosome Y
Full DNA sequences
RefSeqNC_000024 (FASTA)
GenBankCM000686 (FASTA)

The Y chromosome is one of two sex chromosomes in therian mammals and other organisms. Along with the X chromosome, it is part of the XY sex-determination system, in which the Y is the sex-determining chromosome because the presence of the Y chromosome causes offspring produced in sexual reproduction to be of male sex. In mammals, the Y chromosome contains the SRY gene, which triggers development of male gonads. The Y chromosome is passed only from male parents to male offspring.

Overview

[edit]

Discovery

[edit]

The Y chromosome was identified as a sex-determining chromosome by Nettie Stevens at Bryn Mawr College in 1905 during a study of the mealworm Tenebrio molitor. Edmund Beecher Wilson independently discovered the same mechanisms the same year, working with Hemiptera. Stevens proposed that chromosomes always existed in pairs and that the smaller chromosome (now labelled "Y") was the pair of the X chromosome discovered in 1890 by Hermann Henking. She realized that the previous idea of Clarence Erwin McClung, that the X chromosome determines sex, was wrong and that sex determination is, in fact, due to the presence or absence of the Y chromosome. In the early 1920s, Theophilus Painter determined that X and Y chromosomes determined sex in humans (and other mammals).[4]

The chromosome was given the name "Y" simply to follow on from Henking's "X" alphabetically.[5][6] The idea that the Y chromosome was named after its similarity in appearance to the letter "Y" is mistaken. All chromosomes normally appear as an amorphous blob under the microscope and only take on a well-defined shape during mitosis. This shape is vaguely X-shaped for all chromosomes. It is entirely coincidental that the Y chromosome, during mitosis, has two very short branches which can look merged under the microscope and appear as the descender of a Y-shape.[5]: 65–66 

Variations

[edit]

Most therian mammals have only one pair of sex chromosomes in each cell. Males have one Y chromosome and one X chromosome, while females have two X chromosomes. In mammals, the Y chromosome contains a gene, SRY, which triggers embryonic development as a male. The Y chromosomes of humans and other mammals also contain other genes needed for normal sperm production.[citation needed]

There are exceptions, however. Among humans, some males are born two Xs and a Y ("XXY", see Klinefelter syndrome), one X and two Ys (see XYY syndrome). Some females have three Xs (Trisomy X), and some have a single X instead of two Xs ("X0", see Turner syndrome). There are other variations in which, during embryonic development, the WNT4 gene[7] is activated and/or the SRY gene is damaged leading to birth of an XY female (Swyer syndrome[7]). A Y chromosome may also be present but fail to result in the development of a male phenotype in individuals with androgen insensitivity syndrome, instead resulting in a female or ambiguous phenotype. In other cases, the SRY gene is copied to the X, leading to birth of an XX male.[8]

Origins and evolution

[edit]

Before Y chromosome

[edit]

Many ectothermic vertebrates have no sex chromosomes.[9] If these species have different sexes, sex is determined environmentally rather than genetically. For some species, especially reptiles, sex depends on the incubation temperature.[10] Some vertebrates are hermaphrodites, though hermaphroditic species are most commonly sequential, meaning the organism switches sex, producing male or female gametes at different points in its life, but never producing both at the same time. This is opposed to simultaneous hermaphroditism, where the same organism produces male and female gametes at the same time. Most simultaneous hermaphrodite species are invertebrates, and among vertebrates, simultaneous hermaphroditism has only been discovered in a few orders of fish.[11]

Origin

[edit]

The X and Y chromosomes are thought to have evolved from a pair of identical chromosomes,[12][13] termed autosomes, when an ancestral animal developed an allelic variation (a so-called "sex locus") and simply possessing this allele caused the organism to be male.[14] The chromosome with this allele became the Y chromosome, while the other member of the pair became the X chromosome. Over time, genes that were beneficial for males and harmful to (or had no effect on) females either developed on the Y chromosome or were acquired by the Y chromosome through the process of translocation.[15]

Until recently, the X and Y chromosomes in mammals were thought to have diverged around 300 million years ago.[16] However, research published in 2008 analyzing the platypus genome[17] suggested that the XY sex-determination system would not have been present more than 166 million years ago, when monotremes split from other mammals.[18] This re-estimation of the age of the therian XY system is based on the finding that sequences that are on the X chromosomes of marsupials and eutherian mammals are not present on the autosomes of platypus and birds.[18] The older estimate was based on erroneous reports that the platypus X chromosomes contained these sequences.[19][20]

Recombination inhibition

[edit]

Most chromosomes recombine during meiosis. However, in males, the X and Y pair in a shared region known as the pseudoautosomal region (PAR).[21] The PAR undergoes frequent recombination between the X and Y chromosomes,[21] but recombination is suppressed in other regions of the Y chromosome.[14] These regions contain sex-determining and other male-specific genes.[22] Without this suppression, these genes could be lost from the Y chromosome from recombination and cause issues such as infertility.[23]

The lack of recombination across the majority of the Y chromosome makes it a useful tool in studying human evolution, since recombination complicates the mathematical models used to trace ancestries.[24]

Degeneration

[edit]

By one estimate, the human Y chromosome has lost 1,393 of its 1,438 original genes over the course of its existence, and linear extrapolation of this 1,393-gene loss over 300 million years gives a rate of genetic loss of 4.6 genes per million years.[25] Continued loss of genes at the rate of 4.6 genes per million years would result in a Y chromosome with no functional genes – that is the Y chromosome would lose complete function – within the next 10 million years, or half that time with the current age estimate of 160 million years.[14][26] Comparative genomic analysis reveals that many mammalian species are experiencing a similar loss of function in their heterozygous sex chromosome. Degeneration may simply be the fate of all non-recombining sex chromosomes, due to three common evolutionary forces: high mutation rate, inefficient selection, and genetic drift.[14]

With a 30% difference between humans and chimpanzees, the Y chromosome is one of the fastest-evolving parts of the human genome.[27] However, these changes have been limited to non-coding sequences and comparisons of the human and chimpanzee Y chromosomes (first published in 2005) show that the human Y chromosome has not lost any genes since the divergence of humans and chimpanzees between 6–7 million years ago.[28] Additionally, a scientific report in 2012 stated that only one gene had been lost since humans diverged from the rhesus macaque 25 million years ago.[29] These facts provide direct evidence that the linear extrapolation model is flawed and suggest that the current human Y chromosome is either no longer shrinking or is shrinking at a much slower rate than the 4.6 genes per million years estimated by the linear extrapolation model.[citation needed]

High mutation rate

[edit]

The human Y chromosome is particularly exposed to high mutation rates due to the environment in which it is housed. The Y chromosome is passed exclusively through sperm, which undergo multiple cell divisions during gametogenesis. Each cellular division provides further opportunity to accumulate base pair mutations. Additionally, sperm are stored in the highly oxidative environment of the testis, which encourages further mutation. These two conditions combined put the Y chromosome at a greater opportunity of mutation than the rest of the genome.[14] The increased mutation opportunity for the Y chromosome is reported by Graves as a factor 4.8.[14] However, her original reference obtains this number for the relative mutation rates in male and female germ lines for the lineage leading to humans.[30]

The observation that the Y chromosome experiences little meiotic recombination and has an accelerated rate of mutation and degradative change compared to the rest of the genome suggests an evolutionary explanation for the adaptive function of meiosis with respect to the main body of genetic information. Brandeis[31] proposed that the basic function of meiosis (particularly meiotic recombination) is the conservation of the integrity of the genome, a proposal consistent with the idea that meiosis is an adaptation for repairing DNA damage.[32]

Inefficient selection

[edit]

Without the ability to recombine during meiosis, the Y chromosome is unable to expose individual alleles to natural selection. Deleterious alleles are allowed to "hitchhike" with beneficial neighbors, thus propagating maladapted alleles into the next generation. Conversely, advantageous alleles may be selected against if they are surrounded by harmful alleles (background selection). Due to this inability to sort through its gene content, the Y chromosome is particularly prone to the accumulation of "junk" DNA. Massive accumulations of retrotransposable elements are scattered throughout the Y.[14] The random insertion of DNA segments often disrupts encoded gene sequences and renders them nonfunctional. However, the Y chromosome has no way of weeding out these "jumping genes". Without the ability to isolate alleles, selection cannot effectively act upon them.[citation needed]

A clear, quantitative indication of this inefficiency is the entropy rate of the Y chromosome. Whereas all other chromosomes in the human genome have entropy rates of 1.5–1.9 bits per nucleotide (compared to the theoretical maximum of exactly 2 for no redundancy), the Y chromosome's entropy rate is only 0.84.[33] From the definition of entropy rate, the Y chromosome has a much lower information content relative to its overall length, and is more redundant.

Genetic drift

[edit]

Even if a well adapted Y chromosome manages to maintain genetic activity by avoiding mutation accumulation, there is no guarantee it will be passed down to the next generation. The population size of the Y chromosome is inherently limited to 1/4 that of autosomes: diploid organisms contain two copies of autosomal chromosomes while only half the population contains 1 Y chromosome. Thus, genetic drift is an exceptionally strong force acting upon the Y chromosome. Through sheer random assortment, an adult male may never pass on his Y chromosome if he only has female offspring. Thus, although a male may have a well adapted Y chromosome free of excessive mutation, it may never make it into the next gene pool.[14] The repeat random loss of well-adapted Y chromosomes, coupled with the tendency of the Y chromosome to evolve to have more deleterious mutations rather than less for reasons described above, contributes to the species-wide degeneration of Y chromosomes through Muller's ratchet.[34]

Gene conversion

[edit]

As has been already mentioned, the Y chromosome is unable to recombine during meiosis like the other human chromosomes; however, in 2003, researchers from MIT discovered a process which may slow down the process of degradation. They found that human Y chromosome is able to "recombine" with itself, using palindrome base pair sequences.[35] Such a "recombination" is called gene conversion.

In the case of the Y chromosomes, the palindromes are not noncoding DNA; these strings of nucleotides contain functioning genes important for male fertility. Most of the sequence pairs are greater than 99.97% identical. The extensive use of gene conversion may play a role in the ability of the Y chromosome to edit out genetic mistakes and maintain the integrity of the relatively few genes it carries. In other words, since the Y chromosome is single, it has duplicates of its genes on itself instead of having a second, homologous, chromosome. When errors occur, it can use other parts of itself as a template to correct them.[35]

Findings were confirmed by comparing similar regions of the Y chromosome in humans to the Y chromosomes of chimpanzees, bonobos and gorillas. The comparison demonstrated that the same phenomenon of gene conversion appeared to be at work more than 5 million years ago, when humans and the non-human primates diverged from each other.[35]

Gene conversion tracts formed during meiosis are long, about 2,068 base pairs, and significantly biased towards the fixation of G or C nucleotides (GC biased).[36] The recombination intermediates preceding gene conversion were found to rarely take the alternate route of crossover recombination.[36] The Y-Y gene conversion rate in humans is about 1.52 x 10-5 conversions/base/year.[37] These gene conversion events may reflect a basic function of meiosis, that of conserving the integrity of the genome.

Future evolution

[edit]

According to some theories, in the terminal stages of the degeneration of the Y chromosome, other chromosomes may increasingly take over genes and functions formerly associated with it and finally, within the framework of this theory, the Y chromosome disappears entirely, and a new sex-determining system arises.[14][neutrality is disputed][improper synthesis?]

Several species of rodent in the sister families Muridae and Cricetidae have reached a stage where the XY system has been modified,[38][39] in the following ways:

  • The Transcaucasian mole vole, Ellobius lutescens, the Zaisan mole vole, Ellobius tancrei, and the Japanese spinous country rats Tokudaia osimensis and Tokudaia tokunoshimensis, have lost the Y chromosome and SRY entirely.[14][40][41] Tokudaia spp. have relocated some other genes ancestrally present on the Y chromosome to the X chromosome.[41] Both sexes of Tokudaia spp. and Ellobius lutescens have an XO genotype (Turner syndrome),[41] whereas all Ellobius tancrei possess an XX genotype.[14] The new sex-determining system(s) for these rodents remains unclear.
  • The wood lemming Myopus schisticolor, the Arctic lemming, Dicrostonyx torquatus, and multiple species in the grass mouse genus Akodon have evolved fertile females who possess the genotype generally coding for males, XY, in addition to the ancestral XX female, through a variety of modifications to the X and Y chromosomes.[38][42][43]
  • In the creeping vole, Microtus oregoni, the females, with just one X chromosome each, produce X gametes only, and the males, XY, produce Y gametes, or gametes devoid of any sex chromosome, through nondisjunction.[44]

Outside of the rodents, the black muntjac, Muntiacus crinifrons, evolved new X and Y chromosomes through fusions of the ancestral sex chromosomes and autosomes.[45]

Modern data cast doubt on the hypothesis that the Y-chromosome will disappear.[16] This conclusion was reached by scientists who studied the Y chromosomes of rhesus monkeys. When genomically comparing the Y chromosome of rhesus monkeys and humans, scientists found very few differences, given that humans and rhesus monkeys diverged 30 million years ago.[46][clarification needed]

Outside of mammals, some organisms have lost the Y chromosome, such as most species of Nematodes. However, in order for the complete elimination of Y to occur, it was necessary to develop an alternative way of determining sex (for example, by determining sex by the ratio of the X chromosome to autosomes), and any genes necessary for male function had to be moved to other chromosomes.[16] In the meantime, modern data demonstrate the complex mechanisms of Y chromosome evolution and the fact that the disappearance of the Y chromosome is not guaranteed.

1:1 sex ratio

[edit]

Fisher's principle outlines why almost all species using sexual reproduction have a sex ratio of 1:1. W. D. Hamilton gave the following basic explanation in his 1967 paper on "Extraordinary sex ratios",[47] given the condition that males and females cost equal amounts to produce:

  1. Suppose male births are less common than female.
  2. A newborn male then has better mating prospects than a newborn female, and therefore can expect to have more offspring.
  3. Therefore, parents genetically disposed to produce males tend to have more than average numbers of grandchildren born to them.
  4. Therefore, the genes for male-producing tendencies spread, and male births become more common.
  5. As the 1:1 sex ratio is approached, the advantage associated with producing males dies away.
  6. The same reasoning holds if females are substituted for males throughout. Therefore, 1:1 is the equilibrium ratio.

Non-therian Y chromosome

[edit]

Many groups of organisms in addition to therian mammals have Y chromosomes, but these Y chromosomes do not share common ancestry with therian Y chromosomes. Such groups include monotremes, Drosophila, some other insects, some fish, some reptiles, and some plants. In Drosophila melanogaster, the Y chromosome does not trigger male development. Instead, sex is determined by the number of X chromosomes. The D. melanogaster Y chromosome does contain genes necessary for male fertility. So XXY D. melanogaster are female, and D. melanogaster with a single X (X0), are male but sterile. There are some species of Drosophila in which X0 males are both viable and fertile.[citation needed]

ZW chromosomes

[edit]

Other organisms have mirror image sex chromosomes: where the homogeneous sex is the male, with two Z chromosomes, and the female is the heterogeneous sex with a Z chromosome and a W chromosome.[48] For example, the ZW sex-determination system is found in birds, snakes, and butterflies; the females have ZW sex chromosomes, and males have ZZ sex chromosomes.[48][49][50]

Non-inverted Y chromosome

[edit]

There are some species, such as the Japanese rice fish, in which the XY system is still developing and cross over between the X and Y is still possible. Because the male specific region is very small and contains no essential genes, it is even possible to artificially induce XX males and YY females to no ill effect.[51]

Multiple XY pairs

[edit]

Monotremes like platypuses possess four or five pairs of XY sex chromosomes, each pair consisting of sex chromosomes with homologous regions. The chromosomes of neighboring pairs are partially homologous, such that a chain is formed during mitosis.[19] The first X chromosome in the chain is also partially homologous with the last Y chromosome, indicating that profound rearrangements, some adding new pieces from autosomes, have occurred in history.[52][53]: fig. 5 

Platypus sex chromosomes have strong sequence similarity with the avian Z chromosome, (indicating close homology),[17] and the SRY gene so central to sex-determination in most other mammals is apparently not involved in platypus sex-determination.[18]

Human Y chromosome

[edit]

The human Y chromosome is composed of about 62 million base pairs of DNA, making it similar in size to chromosome 19 and represents almost 2% of the total DNA in a male cell.[54][55] The human Y chromosome carries 693 genes, 107 of which are protein-coding.[56] However, some genes are repeated, making the number of exclusive protein-coding genes just 42.[56] The Consensus Coding Sequence (CCDS) Project only classifies 63 out of 107 genes, though CCDS estimates are often considered lower bounds due to their conservative classification strategy.[57] All single-copy Y-linked genes are hemizygous (present on only one chromosome) except in cases of aneuploidy such as XYY syndrome or XXYY syndrome. Traits that are inherited via the Y chromosome are called Y-linked traits, or holandric traits (from Ancient Greek ὅλος hólos, "whole" + ἀνδρός andrós, "male").[58]

Sequence of the human Y chromosome

[edit]

At the end of the Human Genome Project (and after many updates) almost half of the Y chromosome remained un-sequenced even in 2021; a different Y chromosome from the HG002 (GM24385) genome was completely sequenced in January 2022 and is included in the new "complete genome" human reference genome sequence, CHM13.[56] The complete sequencing of a human Y chromosome was shown to contain 62,460,029 base pairs and 41 additional genes.[56] This added 30 million base pairs,[56] but it was discovered that the Y chromosome can vary a lot in size between individuals, from 45.2 million to 84.9 million base pairs.[59]

Since almost half of the human Y sequence was unknown before 2022, it could not be screened out as contamination in microbial sequencing projects. As a result, the NCBI RefSeq bacterial genome database mistakenly includes some Y chromosome data.[56]

Structure

[edit]

Cytogenetic band

[edit]
G-banding ideograms of human Y chromosome
G-banding ideogram of human Y chromosome in resolution 850 bphs. Band length in this diagram is proportional to base-pair length. This type of ideogram is generally used in genome browsers (e.g. Ensembl, UCSC Genome Browser).
G-banding patterns of human Y chromosome in three different resolutions (400,[60] 550[61] and 850[3]). Band length in this diagram is based on the ideograms from ISCN (2013).[62] This type of ideogram represents actual relative band length observed under a microscope at the different moments during the mitotic process.[63]
G-bands of human Y chromosome in resolution 850 bphs[3]
Chr. Arm[64] Band[65] ISCN
start[66]
ISCN
stop[66]
Basepair
start
Basepair
stop
Stain[67] Density
Y p 11.32 0 149 1 300,000 gneg
Y p 11.31 149 298 300,001 600,000 gpos 50
Y p 11.2 298 1043 600,001 10,300,000 gneg
Y p 11.1 1043 1117 10,300,001 10,400,000 acen
Y q 11.1 1117 1266 10,400,001 10,600,000 acen
Y q 11.21 1266 1397 10,600,001 12,400,000 gneg
Y q 11.221 1397 1713 12,400,001 17,100,000 gpos 50
Y q 11.222 1713 1881 17,100,001 19,600,000 gneg
Y q 11.223 1881 2160 19,600,001 23,800,000 gpos 50
Y q 11.23 2160 2346 23,800,001 26,600,000 gneg
Y q 12 2346 3650 26,600,001 57,227,415 gvar

Non-combining region of Y (NRY)

[edit]

The human Y chromosome is normally unable to recombine with the X chromosome, except for small pieces of pseudoautosomal regions (PARs) at the telomeres (which comprise about 5% of the chromosome's length). These regions are relics of ancient homology between the X and Y chromosomes. The bulk of the Y chromosome, which does not recombine, is called the "NRY", or non-recombining region of the Y chromosome.[68] Single-nucleotide polymorphisms (SNPs) in this region are used to trace direct paternal ancestral lines.

More specifically, PAR1 is at 0.1–2.7 Mb. PAR2 is at 56.9–57.2 Mb. The non-recombining region (NRY) or male-specific region (MSY) sits between. Their sizes is now known perfectly from CHM13: 2.77 Mb and 329.5 kb. Until CHM13 the data in PAR1 and PAR2 was just copied over from X chromosome.[59]

Sequence classes

[edit]

Genes

[edit]

Number of genes

[edit]

The following are some of the gene count estimates of human Y chromosome. Because researchers use different approaches to genome annotation their predictions of the number of genes on each chromosome varies (for technical details, see gene prediction). Among various projects, CCDS takes an extremely conservative strategy. So CCDS's gene number prediction represents a lower bound on the total number of human protein-coding genes.[69]

Estimated by Protein-coding genes Non-coding RNA genes Pseudogenes Source Release date
CCDS 63 [1] 2016-09-08
HGNC 45 55 381 [70] 2017-05-12
Ensembl 63 109 392 [71] 2017-03-29
UniProt 47 [72] 2018-02-28
NCBI 73 122 400 [73][74][75] 2017-05-19

Gene list

[edit]

In general, the human Y chromosome is extremely gene poor—it is one of the largest gene deserts in the human genome. Disregarding pseudoautosomal genes, genes encoded on the human Y chromosome include:

Genes on the non-recombining portion of the Y chromosome[76]
Name X paralog Note
SRY SOX3 Sex-determining region. This is the p arm [Yp].
ZFY ZFX Zinc finger.
RPS4Y1 RPS4X Ribosomal protein S4.
AMELY AMELX Amelogenin.
TBL1Y TBL1X
PCDH11Y PDCH11X X-transposed region (XTR) from Xq21, one of two genes. Once dubbed "PAR3"[77] but later refuted.[78]
TGIF2LY TGIF2LX The other X-transposed gene.
TSPY1, TSPY2 TSPX Testis-specific protein.
AZFa (none) Not a gene. First part of the AZF (Azoospermia factor) region on arm q. Contains the four following genes. X counterparts escape inactivation.
USP9Y USP9X Ubiquitin protease.
DDX3Y DDX3X Helicase.
UTY UTX Histone demethylase.
TB4Y TB4X
AZFb (none) Second AZF region on arm q. Prone to NAHR [non-allelic homologous recombination] with AZFc. Overlaps with AZFc. Contains three single-copy gene regions and repeats.
CYorf15 CXorf15
RPS4Y2 RPS4X Another copy of ribosomal protein S4.
EIF1AY EIF4AX
KDM5D KDM5C
XKRY XK (protein) Found in the "yellow" amplicon.
HSFY1, HSFY2 HSFX1, HSFX2 Found in the "blue" amplicon.
PRY, PRY2 Found in the "blue" amplicon. Identified by similarity to PTPN13 (Chr. 4).
RBMY1A1 RBMY Large number of copies. Part of an RBM gene family of RNA recognition motif (RRM) proteins.
AZFc (none) Final (distal) part of the AZF. Multiple palindromes.
DAZ1, DAZ2, DAZ3, DAZ4 RRM genes in two palindromic clusters. BOLL and DAZLA are autosomal homologs.
CDY1, CDY2 CDY1 is actually two identical copies. CDY2 is two closely related copies in palindrome P5. Probably derived from autosomal CDYL.
VCY1, VCY2 VCX1 through 3 Three copies of VCX2 (BPY2). Part of the VCX/VCY family. The two copies of BPY1 are instead in Yq11.221/AZFa.

Y-chromosome-linked diseases

[edit]

Diseases linked to the Y chromosome typically involve an aneuploidy, an atypical number of chromosomes.

Loss of Y chromosome

[edit]

Males can lose the Y chromosome in a subset of cells, known as mosaic loss. Mosaic loss is strongly associated with age,[79] and smoking is another important risk factor for mosaic loss.[80]

Mosaic loss may be related to health outcomes, indicating that the Y chromosome plays important roles outside of sex determination.[80][81] Males with a higher percentage of hematopoietic stem cells lacking the Y chromosome have a higher risk of certain cancers and have a shorter life expectancy.[81] In many cases, a cause and effect relationship between the Y chromosome and health outcomes has not been determined, and some propose loss of the Y chromosome could be a "neutral karyotype related to normal aging".[82] However, a 2022 study showed that mosaic loss of the Y chromosome causally contributes to fibrosis, heart risks, and mortality.[83]

Further studies are needed to understand how mosaic Y chromosome loss may contribute to other sex differences in health outcomes, such as how male smokers have between 1.5 and 2 times the risk of non-respiratory cancers as female smokers.[84][85] Potential countermeasures identified so far include not smoking or stopping smoking and at least one potential drug that "may help counteract the harmful effects of the chromosome loss" is under investigation.[86][87][better source needed]

Y chromosome microdeletion

[edit]

Y chromosome microdeletion (YCM) is a family of genetic disorders caused by missing genes in the Y chromosome. Many affected men exhibit no symptoms and lead normal lives. However, YCM is also known to be present in a significant number of men with reduced fertility or reduced sperm count.[citation needed]

Defective Y chromosome

[edit]

This results in the person presenting a female phenotype (i.e., is born with female-like genitalia) even though that person possesses an XY karyotype. The lack of the second X results in infertility. In other words, viewed from the opposite direction, the person goes through defeminization but fails to complete masculinization.[citation needed]

The cause can be seen as an incomplete Y chromosome: the usual karyotype in these cases is 45X, plus a fragment of Y. This usually results in defective testicular development, such that the infant may or may not have fully formed male genitalia internally or externally. The full range of ambiguity of structure may occur, especially if mosaicism is present. When the Y fragment is minimal and nonfunctional, the child is usually a girl with the features of Turner syndrome or mixed gonadal dysgenesis.

XXY

[edit]

Klinefelter syndrome (47, XXY) is not an aneuploidy of the Y chromosome, but a condition of having an extra X chromosome, which usually results in defective postnatal testicular function. The mechanism is not fully understood; it does not seem to be due to direct interference by the extra X with expression of Y genes.[citation needed]

XYY

[edit]

47, XYY syndrome (simply known as XYY syndrome) is caused by the presence of a single extra copy of the Y chromosome in each of a male's cells. 47, XYY males have one X chromosome and two Y chromosomes, for a total of 47 chromosomes per cell. Researchers have found that an extra copy of the Y chromosome is associated with increased stature and an increased incidence of learning problems in some boys and men, but the effects are variable, often minimal, and the vast majority do not know their karyotype.[88]

In 1965 and 1966 Patricia Jacobs and colleagues published a chromosome survey of 315 male patients at Scotland's only special security hospital for the developmentally disabled, finding a higher than expected number of patients to have an extra Y chromosome.[89] The authors of this study wondered "whether an extra Y chromosome predisposes its carriers to unusually aggressive behaviour", and this conjecture "framed the next fifteen years of research on the human Y chromosome".[90]

Through studies over the next decade, this conjecture was shown to be incorrect: the elevated crime rate of XYY males is due to lower median intelligence and not increased aggression,[91] and increased height was the only characteristic that could be reliably associated with XYY males.[92] The "criminal karyotype" concept is therefore inaccurate.[88]

There are also XXXY syndrome and XXXXY syndrome.

Rare

[edit]

The following Y-chromosome-linked diseases are rare, but notable because of their elucidation of the nature of the Y chromosome.

More than two Y chromosomes
[edit]

Greater degrees of Y chromosome polysomy (having more than one extra copy of the Y chromosome in every cell, e.g., XYYY) are considerably more rare. The extra genetic material in these cases can lead to skeletal abnormalities, dental abnormalities, decreased IQ, delayed development, and respiratory issues, but the severity features of these conditions are variable.[93]

XX male syndrome
[edit]

XX male syndrome occurs due to a genetic recombination in the formation of the male gametes, causing the SRY portion of the Y chromosome to move to the X chromosome.[8] When such an X chromosome is present in a zygote, male gonads develop because of the SRY gene.[8]

Genetic genealogy

[edit]

In human genetic genealogy (the application of genetics to traditional genealogy), use of the information contained in the Y chromosome is of particular interest because, unlike other chromosomes, the Y chromosome is passed exclusively from father to son, on the patrilineal line. Mitochondrial DNA, maternally inherited to both sons and daughters, is used in an analogous way to trace the matrilineal line.[citation needed]

Brain function

[edit]

Research is currently investigating whether male-pattern neural development is a direct consequence of Y-chromosome-related gene expression or an indirect result of Y-chromosome-related androgenic hormone production.[94]

Microchimerism

[edit]

In 1974, male chromosomes were discovered in fetal cells in the blood circulation of women.[95]

In 1996, it was found that male fetal progenitor cells could persist postpartum in the maternal blood stream for as long as 27 years.[96]

A 2004 study at the Fred Hutchinson Cancer Research Center, Seattle, investigated the origin of male chromosomes found in the peripheral blood of women who had not had male progeny. A total of 120 subjects (women who had never had sons) were investigated, and it was found that 21% of them had male DNA in their peripheral blood. The subjects were categorised into four groups based on their case histories:[97]

  • Group A (8%) had had only female progeny.
  • Patients in Group B (22%) had a history of one or more miscarriages.
  • Patients Group C (57%) had their pregnancies medically terminated.
  • Group D (10%) had never been pregnant before.

The study noted that 10% of the women had never been pregnant before, raising the question of where the Y chromosomes in their blood could have come from. The study suggests that possible reasons for occurrence of male chromosome microchimerism could be one of the following:[97]

  • miscarriages,
  • pregnancies,
  • vanished male twin,
  • possibly from sexual intercourse.

A 2012 study at the same institute has detected cells with the Y chromosome in multiple areas of the brains of deceased women.[98]

See also

[edit]

References

[edit]
  1. ^ a b "Homo sapiens Y chromosome genes". CCDS Release 20 for Homo sapiens. 2016-09-08. Retrieved 2017-05-28.
  2. ^ Strachan T, Read A (2 April 2010). Human Molecular Genetics. Garland Science. p. 45. ISBN 978-1-136-84407-2.
  3. ^ a b c "Ideogram data for Homo sapience (850 bphs, Assembly GRCh38.p3)". Genome Decoration Page. U.S. National Center for Biotechnology Information (NCBI). 2014-06-03. Retrieved 2017-04-26.
  4. ^ Glass B (1990). "Theophilus Shickel Painter: August 22, 1889-October 5, 1969" (PDF). Biographical Memoirs of the National Academy of Sciences. 59: 309–37. PMID 11616163.
  5. ^ a b Bainbridge D (2003). X in Sex : How the X Chromosome Controls. Cambridge, Mass.: Harvard University Press. ISBN 978-0-674-01621-7.
  6. ^ Schwartz J (2009). In Pursuit of the Gene: From Darwin to DNA. Cambridge, Mass.: Harvard University Press. pp. 170–2. ISBN 978-0-674-03491-4.
  7. ^ a b "Swyer syndrome — Symptoms, Causes, Treatment | NORD". rarediseases.org. Retrieved 2023-09-12.
  8. ^ a b c "XX Male Syndrome — an overview". Science Direct. 2023-09-12.
    Dominguez AA, Reijo Pera RA (2013-01-01). "Infertility". In Maloy S, Hughes K (eds.). Brenner's Encyclopedia of Genetics (2nd ed.). Academic Press. pp. 71–74. doi:10.1016/B978-0-12-374984-0.00793-2. ISBN 978-0-12-374984-0. Retrieved 2023-09-12.
  9. ^ Devlin RH, Nagahama Y (2002-06-21). "Sex determination and sex differentiation in fish: an overview of genetic, physiological, and environmental influences". Aquaculture. Sex determination and sex differentation in fish. 208 (3): 191–364. Bibcode:2002Aquac.208..191D. doi:10.1016/S0044-8486(02)00057-1. ISSN 0044-8486.
  10. ^ Barresi MJ, Gilbert SF (2023). "6. Sex Determination and Gametogenesis §6.4 Environmental Sex Determination in Reptiles". Developmental Biology (13th ed.). Oxford University Press. ISBN 978-0-19-757459-1.
    Gilbert SF (2000). "Environmental Sex Determination". Developmental Biology (6th ed.). Sinauer Associates. p. 60. ISBN 0-87893-243-7. NBK9989.
  11. ^ Kuwamura T, Sunobe T, Sakai Y, Kadota T, Sawada K (2020-07-01). "Hermaphroditism in fishes: an annotated list of species, phylogeny, and mating system". Ichthyological Research. 67 (3): 341–360. Bibcode:2020IchtR..67..341K. doi:10.1007/s10228-020-00754-6. ISSN 1616-3915. S2CID 254168012.
  12. ^ Muller HJ (1914). "A gene for the fourth chromosome of Drosophila". Journal of Experimental Zoology. 17 (3): 325–336. Bibcode:1914JEZ....17..325M. doi:10.1002/jez.1400170303.
  13. ^ Lahn BT, Page DC (October 1999). "Four evolutionary strata on the human X chromosome". Science. 286 (5441): 964–7. doi:10.1126/science.286.5441.964. PMID 10542153.
  14. ^ a b c d e f g h i j k Graves JA (March 2006). "Sex chromosome specialization and degeneration in mammals". Cell. 124 (5): 901–914. doi:10.1016/j.cell.2006.02.024. PMID 16530039. S2CID 8379688.
  15. ^ Graves JA, Koina E, Sankovic N (June 2006). "How the gene content of human sex chromosomes evolved". Current Opinion in Genetics & Development. 16 (3): 219–224. doi:10.1016/j.gde.2006.04.007. PMID 16650758.
  16. ^ a b c Bachtrog D (February 2013). "Y-chromosome evolution: emerging insights into processes of Y-chromosome degeneration". Nature Reviews. Genetics. 14 (2): 113–124. doi:10.1038/nrg3366. PMC 4120474. PMID 23329112.
  17. ^ a b Warren WC, Hillier LW, Marshall Graves JA, Birney E, Ponting CP, Grützner F, et al. (May 2008). "Genome analysis of the platypus reveals unique signatures of evolution". Nature. 453 (7192): 175–183. Bibcode:2008Natur.453..175W. doi:10.1038/nature06936. PMC 2803040. PMID 18464734.
  18. ^ a b c Veyrunes F, Waters PD, Miethke P, Rens W, McMillan D, Alsop AE, et al. (June 2008). "Bird-like sex chromosomes of platypus imply recent origin of mammal sex chromosomes". Genome Research. 18 (6): 965–973. doi:10.1101/gr.7101908. PMC 2413164. PMID 18463302.
  19. ^ a b Grützner F, Rens W, Tsend-Ayush E, El-Mogharbel N, O'Brien PC, Jones RC, et al. (December 2004). "In the platypus a meiotic chain of ten sex chromosomes shares genes with the bird Z and mammal X chromosomes". Nature. 432 (7019): 913–7. Bibcode:2004Natur.432..913G. doi:10.1038/nature03021. PMID 15502814. S2CID 4379897.
  20. ^ Watson JM, Riggs A, Graves JA (October 1992). "Gene mapping studies confirm the homology between the platypus X and echidna X1 chromosomes and identify a conserved ancestral monotreme X chromosome". Chromosoma. 101 (10): 596–601. doi:10.1007/BF00360536. PMID 1424984. S2CID 26978106.
  21. ^ a b LeMieux J (2020-05-29). "On PAR: How X and Y Chromosomes Recombine During Meiosis". GEN — Genetic Engineering and Biotechnology News. Retrieved 2023-11-13.
  22. ^ Peneder P, Wallner B, Vogl C (October 2017). "Exchange of genetic information between therian X and Y chromosome gametologs in old evolutionary strata". Ecology and Evolution. 7 (20): 8478–8487. Bibcode:2017EcoEv...7.8478P. doi:10.1002/ece3.3278. PMC 5648654. PMID 29075464.
  23. ^ Dhanoa JK, Mukhopadhyay CS, Arora JS (July 2016). "Y-chromosomal genes affecting male fertility: A review". Vet World. 9 (7): 783–91. doi:10.14202/vetworld.2016.783-791. PMC 4983133. PMID 27536043.
  24. ^ Brookfield JF (October 1995). "Human evolution. Y-chromosome clues to human ancestry". Current Biology. 5 (10): 1114–1115. Bibcode:1995CBio....5.1114B. doi:10.1016/S0960-9822(95)00224-7. PMID 8548280. S2CID 16081591.
  25. ^ Graves JA (2004). "The degenerate Y chromosome--can conversion save it?". Reproduction, Fertility, and Development. 16 (5): 527–534. doi:10.1071/RD03096. PMID 15367368.
  26. ^ Goto H, Peng L, Makova KD (February 2009). "Evolution of X-degenerate Y chromosome genes in greater apes: conservation of gene content in human and gorilla, but not chimpanzee". Journal of Molecular Evolution. 68 (2): 134–144. Bibcode:2009JMolE..68..134G. doi:10.1007/s00239-008-9189-y. PMID 19142680. S2CID 24010421.
  27. ^ Wade N (January 13, 2010). "Male Chromosome May Evolve Fastest". New York Times.
  28. ^ Hughes JF, Skaletsky H, Pyntikova T, Minx PJ, Graves T, Rozen S, et al. (September 2005). "Conservation of Y-linked genes during human evolution revealed by comparative sequencing in chimpanzee". Nature. 437 (7055): 100–103. Bibcode:2005Natur.437..100H. doi:10.1038/nature04101. PMID 16136134. S2CID 4418662.
  29. ^ Hsu C. "Biologists Debunk the 'Rotting' Y Chromosome Theory, Men Will Still Exist". Medical Daily. Archived from the original on 2012-02-25. Retrieved 2012-02-23.
  30. ^ Lindblad-Toh K, Wade CM, Mikkelsen TS, Karlsson EK, Jaffe DB, Kamal M, et al. (December 2005). "Genome sequence, comparative analysis and haplotype structure of the domestic dog". Nature. 438 (7069): 803–819. Bibcode:2005Natur.438..803L. doi:10.1038/nature04338. PMID 16341006.
  31. ^ Brandeis M (May 2018). "New-age ideas about age-old sex: separating meiosis from mating could solve a century-old conundrum". Biological Reviews of the Cambridge Philosophical Society. 93 (2): 801–810. doi:10.1111/brv.12367. PMID 28913952. S2CID 4764175.
  32. ^ Bernstein H, Hopf FA, Michod RE (1987). "The molecular basis of the evolution of sex". Molecular Genetics of Development. Advances in Genetics. Vol. 24. pp. 323–70. doi:10.1016/S0065-2660(08)60012-7. ISBN 9780120176243. PMID 3324702.
  33. ^ Liu Z, Venkatesh SS, Maley CC (October 2008). "Sequence space coverage, entropy of genomes and the potential to detect non-human DNA in human samples". BMC Genomics. 9 (1): 509. doi:10.1186/1471-2164-9-509. PMC 2628393. PMID 18973670. Fig. 6, using the Lempel-Ziv estimators of entropy rate.
  34. ^ Charlesworth B, Charlesworth D (November 2000). "The degeneration of Y chromosomes". Philosophical Transactions of the Royal Society of London. Series B, Biological Sciences. 355 (1403): 1563–1572. doi:10.1098/rstb.2000.0717. PMC 1692900. PMID 11127901.
  35. ^ a b c Rozen S, Skaletsky H, Marszalek JD, Minx PJ, Cordum HS, Waterston RH, et al. (June 2003). "Abundant gene conversion between arms of palindromes in human and ape Y chromosomes". Nature. 423 (6942): 873–876. Bibcode:2003Natur.423..873R. doi:10.1038/nature01723. PMID 12815433. S2CID 4323263.
  36. ^ a b Hallast P, Balaresque P, Bowden GR, Ballereau S, Jobling MA (2013). "Recombination dynamics of a human Y-chromosomal palindrome: rapid GC-biased gene conversion, multi-kilobase conversion tracts, and rare inversions". PLOS Genet. 9 (7): e1003666. doi:10.1371/journal.pgen.1003666. PMC 3723533. PMID 23935520.
  37. ^ Bonito M, D'Atanasio E, Ravasini F, Cariati S, Finocchio A, Novelletto A, Trombetta B, Cruciani F (November 2021). "New insights into the evolution of human Y chromosome palindromes through mutation and gene conversion". Hum Mol Genet. 30 (23): 2272–2285. doi:10.1093/hmg/ddab189. PMC 8600007. PMID 34244762.
  38. ^ a b Marchal JA, Acosta MJ, Bullejos M, Díaz de la Guardia R, Sánchez A (2003). "Sex chromosomes, sex determination, and sex-linked sequences in Microtidae". Cytogenetic and Genome Research. 101 (3–4): 266–273. doi:10.1159/000074347. PMID 14684993. S2CID 10526522.
  39. ^ Wilson MA, Makova KD (2009). "Genomic analyses of sex chromosome evolution". Annual Review of Genomics and Human Genetics. 10 (1): 333–354. doi:10.1146/annurev-genom-082908-150105. PMID 19630566.
  40. ^ Just W, Baumstark A, Süss A, Graphodatsky A, Rens W, Schäfer N, et al. (2007). "Ellobius lutescens: sex determination and sex chromosome". Sexual Development. 1 (4): 211–221. doi:10.1159/000104771. PMID 18391532. S2CID 25939138.
  41. ^ a b c Arakawa Y, Nishida-Umehara C, Matsuda Y, Sutou S, Suzuki H (2002). "X-chromosomal localization of mammalian Y-linked genes in two XO species of the Ryukyu spiny rat". Cytogenetic and Genome Research. 99 (1–4): 303–9. doi:10.1159/000071608. PMID 12900579. S2CID 39633026.
  42. ^ Hoekstra HE, Edwards SV (September 2000). "Multiple origins of XY female mice (genus Akodon): phylogenetic and chromosomal evidence". Proceedings. Biological Sciences. 267 (1455): 1825–31. doi:10.1098/rspb.2000.1217. PMC 1690748. PMID 11052532.
  43. ^ Ortiz MI, Pinna-Senn E, Dalmasso G, Lisanti JA (2009). "Chromosomal aspects and inheritance of the XY female condition in Akodon azarae (Rodentia, Sigmodontinae)". Mammalian Biology. 74 (2): 125–9. Bibcode:2009MamBi..74..125O. doi:10.1016/j.mambio.2008.03.001.
  44. ^ Charlesworth B, Dempsey ND (April 2001). "A model of the evolution of the unusual sex chromosome system of Microtus oregoni". Heredity. 86 (Pt 4): 387–394. doi:10.1046/j.1365-2540.2001.00803.x. PMID 11520338. S2CID 34489270.
  45. ^ Zhou Q, Wang J, Huang L, Nie W, Wang J, Liu Y, et al. (2008). "Neo-sex chromosomes in the black muntjac recapitulate incipient evolution of mammalian sex chromosomes". Genome Biology. 9 (6): R98. doi:10.1186/gb-2008-9-6-r98. PMC 2481430. PMID 18554412.
  46. ^ Hughes JF, Skaletsky H, Page DC (December 2012). "Sequencing of rhesus macaque Y chromosome clarifies origins and evolution of the DAZ (Deleted in AZoospermia) genes". BioEssays. 34 (12): 1035–44. doi:10.1002/bies.201200066. PMC 3581811. PMID 23055411.
  47. ^ Hamilton WD (April 1967). "Extraordinary sex ratios. A sex-ratio theory for sex linkage and inbreeding has new implications in cytogenetics and entomology". Science. 156 (3774): 477–488. Bibcode:1967Sci...156..477H. doi:10.1126/science.156.3774.477. PMID 6021675.
  48. ^ a b Smith JJ, Voss SR (September 2007). "Bird and mammal sex-chromosome orthologs map to the same autosomal region in a salamander (ambystoma)". Genetics. 177 (1): 607–613. doi:10.1534/genetics.107.072033. PMC 2013703. PMID 17660573.
  49. ^ Viana PF, Ezaz T, de Bello Cioffi M, Liehr T, Al-Rikabi A, Goll LG, et al. (July 2020). "Landscape of snake' sex chromosomes evolution spanning 85 MYR reveals ancestry of sequences despite distinct evolutionary trajectories". Scientific Reports. 10 (1): 12499. Bibcode:2020NatSR..1012499V. doi:10.1038/s41598-020-69349-5. PMC 7385105. PMID 32719365.
  50. ^ Sahara K, Yoshido A, Traut W (January 2012). "Sex chromosome evolution in moths and butterflies". Chromosome Research. 20 (1): 83–94. doi:10.1007/s10577-011-9262-z. hdl:2115/49121. PMID 22187366. S2CID 15130561.
  51. ^ Schartl M (July 2004). "A comparative view on sex determination in medaka". Mechanisms of Development. 121 (7–8): 639–645. doi:10.1016/j.mod.2004.03.001. PMID 15210173. S2CID 17401686.
  52. ^ Cortez D, Marin R, Toledo-Flores D, Froidevaux L, Liechti A, Waters PD, et al. (April 2014). "Origins and functional evolution of Y chromosomes across mammals". Nature. 508 (7497): 488–493. Bibcode:2014Natur.508..488C. doi:10.1038/nature13151. PMID 24759410. S2CID 4462870.
  53. ^ Deakin JE, Graves JA, Rens W (2012). "The evolution of marsupial and monotreme chromosomes". Cytogenetic and Genome Research. 137 (2–4): 113–129. doi:10.1159/000339433. hdl:1885/64794. PMID 22777195.
  54. ^ "Ensembl Human MapView release 43". February 2014. Retrieved 2007-04-14.
  55. ^ "National Library of Medicine's Genetic Home Reference". Archived from the original on 2012-03-29. Retrieved 2009-11-09.
  56. ^ a b c d e f Rhie A, Nurk S, Cechova M, Hoyt SJ, Taylor DJ, Altemose N, et al. (September 2023). "The complete sequence of a human Y chromosome". Nature. 621 (7978): 344–354. Bibcode:2023Natur.621..344R. doi:10.1038/s41586-023-06457-y. PMC 10752217. PMID 37612512. S2CID 254181409.
  57. ^ Pertea M, Salzberg SL (2010-05-05). "Between a chicken and a grape: estimating the number of human genes". Genome Biology. 11 (5): 206. doi:10.1186/gb-2010-11-5-206. PMC 2898077. PMID 20441615.
  58. ^ "Definition of holandric". Dictionary.com. Retrieved 2020-01-21.
  59. ^ a b Hallast P, Ebert P, Loftus M, Yilmaz F, Audano PA, Logsdon GA, et al. (September 2023). "Assembly of 43 human Y chromosomes reveals extensive complexity and variation". Nature. 621 (7978): 355–364. Bibcode:2023Natur.621..355H. doi:10.1038/s41586-023-06425-6. PMC 10726138. PMID 37612510. S2CID 261098546.
  60. ^ "Ideogram data for Homo sapience (400 bphs, Assembly GRCh38.p3". Genome Decoration Page. U.S. National Center for Biotechnology Information (NCBI). 2014-06-04. Retrieved 2017-04-26.
  61. ^ "Ideogram data for Homo sapience (550 bphs, Assembly GRCh38.p3)". Genome Decoration Page. U.S. National Center for Biotechnology Information (NCBI). 2015-08-11. Retrieved 2017-04-26.
  62. ^ International Standing Committee on Human Cytogenetic Nomenclature (2013). ISCN 2013: An International System for Human Cytogenetic Nomenclature (2013). Karger Medical and Scientific Publishers. ISBN 978-3-318-02253-7.
  63. ^ Sethakulvichai W, Manitpornsut S, Wiboonrat M, Lilakiatsakun W, Assawamakin A, Tongsima S (2012). "Estimation of band level resolutions of human chromosome images". 2012 Ninth International Conference on Computer Science and Software Engineering (JCSSE). pp. 276–282. doi:10.1109/JCSSE.2012.6261965. ISBN 978-1-4673-1921-8. S2CID 16666470.
  64. ^ "p": Short arm; "q": Long arm.
  65. ^ For cytogenetic banding nomenclature, see article locus.
  66. ^ a b These values (ISCN start/stop) are based on the length of bands/ideograms from the ISCN book, An International System for Human Cytogenetic Nomenclature (2013). Arbitrary unit.
  67. ^ gpos: Region which is positively stained by G banding, generally AT-rich and gene poor; gneg: Region which is negatively stained by G banding, generally CG-rich and gene rich; acen Centromere. var: Variable region; stalk: Stalk.
  68. ^ "Scientists Reshape Y Chromosome Haplogroup Tree Gaining New Insights Into Human Ancestry". Science Daily. 3 April 2008.
  69. ^ Pertea M, Salzberg SL (2010). "Between a chicken and a grape: estimating the number of human genes". Genome Biology. 11 (5): 206. doi:10.1186/gb-2010-11-5-206. PMC 2898077. PMID 20441615.
  70. ^ "Statistics & Downloads for chromosome Y". HUGO Gene Nomenclature Committee. 2017-05-12. Archived from the original on 2017-06-29. Retrieved 2017-05-19.
  71. ^ "Chromosome Y: Chromosome summary — Homo sapiens". Ensembl Release 88. 2017-03-29. Retrieved 2017-05-19.
  72. ^ "Human chromosome Y: entries, gene names and cross-references to MIM". UniProt. 2018-02-28. Retrieved 2018-03-16.
  73. ^ "Homo sapiens Y chromosome coding genes". National Center for Biotechnology Information Gene Database. 2017-05-19. Retrieved 2017-05-20.
  74. ^ "Homo sapiens Y chromosome non-coding genes". 2017-05-19. Retrieved 2017-05-20.
  75. ^ "Homo sapiens Y chromosome non-coding pseudo genes". 2017-05-19. Retrieved 2017-05-20.
  76. ^ Colaco S, Modi D (February 2018). "Genetics of the human Y chromosome and its association with male infertility". Reproductive Biology and Endocrinology. 16 (1): 14. doi:10.1186/s12958-018-0330-5. PMC 5816366. PMID 29454353.
  77. ^ Veerappa AM, Padakannaya P, Ramachandra NB (August 2013). "Copy number variation-based polymorphism in a new pseudoautosomal region 3 (PAR3) of a human X-chromosome-transposed region (XTR) in the Y chromosome". Functional & Integrative Genomics. 13 (3): 285–293. doi:10.1007/s10142-013-0323-6. PMID 23708688. S2CID 13443194.
  78. ^ Raudsepp T, Chowdhary BP (6 January 2016). "The Eutherian Pseudoautosomal Region". Cytogenetic and Genome Research. 147 (2–3): 81–94. doi:10.1159/000443157. hdl:10576/22940. PMID 26730606.
  79. ^ Zeiher A, Braun T (July 2022). "Mosaic loss of Y chromosome during aging". Science. 377 (6603): 266–7. Bibcode:2022Sci...377..266Z. doi:10.1126/science.add0839. PMID 35857599. S2CID 250579530.
  80. ^ a b Forsberg LA (May 2017). "Loss of chromosome Y (LOY) in blood cells is associated with increased risk for disease and mortality in aging men". Human Genetics. 136 (5): 657–663. doi:10.1007/s00439-017-1799-2. PMC 5418310. PMID 28424864.
  81. ^ a b Forsberg LA, Rasi C, Malmqvist N, Davies H, Pasupulati S, Pakalapati G, et al. (June 2014). "Mosaic loss of chromosome Y in peripheral blood is associated with shorter survival and higher risk of cancer". Nature Genetics. 46 (6): 624–8. doi:10.1038/ng.2966. PMC 5536222. PMID 24777449.
  82. ^ Guo X, Dai X, Zhou T, Wang H, Ni J, Xue J, Wang X (April 2020). "Mosaic loss of human Y chromosome: what, how and why". Human Genetics. 139 (4): 421–446. doi:10.1007/s00439-020-02114-w. PMID 32020362. S2CID 211036885.
  83. ^ Sano S, Horitani K, Ogawa H, Halvardson J, Chavkin NW, Wang Y, et al. (July 2022). "Hematopoietic loss of Y chromosome leads to cardiac fibrosis and heart failure mortality". Science. 377 (6603): 292–7. Bibcode:2022Sci...377..292S. doi:10.1126/science.abn3100. PMC 9437978. PMID 35857592.
  84. ^ Coghlan A (13 December 2014). "Y men are more likely to get cancer than women". New Scientist: 17.
  85. ^ Dumanski JP, Rasi C, Lönn M, Davies H, Ingelsson M, Giedraitis V, et al. (January 2015). "Mutagenesis. Smoking is associated with mosaic loss of chromosome Y". Science. 347 (6217): 81–83. Bibcode:2015Sci...347...81D. doi:10.1126/science.1262092. PMC 4356728. PMID 25477213.
  86. ^ "Loss of male sex chromosome leads to earlier death for men". University of Virginia. Retrieved 31 August 2022.
  87. ^ "Loss of male sex chromosome may lead to earlier death for men – study". The Independent. 14 July 2022. Retrieved 31 August 2022.
  88. ^ a b Nussbaum, Robert L. (2007). Thompson & Thompson genetics in medicine. McInnes, Roderick R., Willard, Huntington F., Hamosh, Ada., Thompson, Margaret W. (Margaret Wilson), 1920- (7th. ed.). Philadelphia: Saunders/Elsevier. ISBN 978-1416030805. OCLC 72774424.
  89. ^ Jacobs PA, Brunton M, Melville MM, Brittain RP, McClemont WF (December 1965). "Aggressive behavior, mental sub-normality and the XYY male". Nature. 208 (5017): 1351–2. Bibcode:1965Natur.208.1351J. doi:10.1038/2081351a0. PMID 5870205. S2CID 4145850.
  90. ^ Richardson SS (2013). Sex Itself: The Search for Male & Female in the Human Genome. Chicago: U. of Chicago Press. p. 84. ISBN 978-0-226-08468-8.
  91. ^ Witkin HA, Mednick SA, Schulsinger F, Bakkestrom E, Christiansen KO, Goodenough DR, et al. (August 1976). "Criminality in XYY and XXY men". Science. 193 (4253): 547–555. Bibcode:1976Sci...193..547W. doi:10.1126/science.959813. PMID 959813.
  92. ^ Witkin HA, Goodenough DR, Hirschhorn K (October 1977). "XYY men: are they criminally aggressive?". The Sciences. 17 (6): 10–13. doi:10.1002/j.2326-1951.1977.tb01570.x. PMID 11662398.
  93. ^ Abedi M, Salmaninejad A, Sakhinia E (January 2018). "Rare 48, XYYY syndrome: case report and review of the literature". Clinical Case Reports. 6 (1): 179–184. doi:10.1002/ccr3.1311. PMC 5771943. PMID 29375860.
  94. ^ Kopsida E, Stergiakouli E, Lynn PM, Wilkinson LS, Davies W (2009). "The Role of the Y Chromosome in Brain Function". Open Neuroendocrinology Journal. 2: 20–30. doi:10.2174/1876528900902010020. PMC 2854822. PMID 20396406.
  95. ^ Schröder J, Tiilikainen A, De la Chapelle A (April 1974). "Fetal leukocytes in the maternal circulation after delivery. I. Cytological aspects". Transplantation. 17 (4): 346–354. doi:10.1097/00007890-197404000-00003. PMID 4823382. S2CID 35983351.
  96. ^ Bianchi DW, Zickwolf GK, Weil GJ, Sylvester S, DeMaria MA (January 1996). "Male fetal progenitor cells persist in maternal blood for as long as 27 years postpartum". Proceedings of the National Academy of Sciences of the United States of America. 93 (2): 705–8. Bibcode:1996PNAS...93..705B. doi:10.1073/pnas.93.2.705. PMC 40117. PMID 8570620.
  97. ^ a b Yan Z, Lambert NC, Guthrie KA, Porter AJ, Loubiere LS, Madeleine MM, et al. (August 2005). "Male microchimerism in women without sons: quantitative assessment and correlation with pregnancy history". The American Journal of Medicine. 118 (8): 899–906. doi:10.1016/j.amjmed.2005.03.037. PMID 16084184.
  98. ^ Chan WF, Gurnot C, Montine TJ, Sonnen JA, Guthrie KA, Nelson JL (26 September 2012). "Male microchimerism in the human female brain". PLOS ONE. 7 (9): e45592. Bibcode:2012PLoSO...745592C. doi:10.1371/journal.pone.0045592. PMC 3458919. PMID 23049819.
[edit]