Cell Division Mitosis & Meiosis
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Transcript Cell Division Mitosis & Meiosis
Genetic Disorders
INTRODUCTION:
DEFINITION OF TERMS
CHROMOSOMES- cellular structures where
genes are located
GENES- basic units of heredity
carry information necessary to determine
specific biologic structures & functions
ex. ABO Ag in RBC membrane coded by
chromosome 9
LOCUS- position in the chr where
particular gene is located; all gene loci occur
in pairs except X & Y genes
INTRODUCTION:
DEFINITION OF TERMS
ALLELES- alternative genes in a single locus
ex. Kell blood group system
alleles K & k
KK- homozygous
Kk- heterozygous
HOMOZYGOUS GENES- gene pair that are alike
HETEROZYGOUS GENES- gene pair that are not
alike
GENOTYPE- actual gene composition that make the
trait
PHENOTYPE- manifestation of the structure/
form produced by the genes
INTRODUCTION:
DEFINITION OF TERMS
DOMINANT GENES- genes that
are always expressed in the phenotype
whether homozygous or heterozygous
RECESSIVE (AMORPH) GENES- genes that
are masked if paired w/ a dominant gene,
thereby only expressed when paired w/
another recessive gene
INTRODUCTION:
DEFINITION OF TERMS
EUPLOIDY- multiples of the haploid # that is
considered normal
HAPLOID
(N)= 23- OCCURS IN MEIOSIS
DIPLOID
(2N)= 46- OCCURS IN MITOSIS
ANEUPLOID- not exact multiples of the
haploid #; only 1 pair of chr involved,
therefore, germ cells have 2 copies of the
same chr or lack the affected chr entirely
HYPODIPLOID 2N- 1, -2, ETC. (MONOSOMY)
HYPERDIPLOID 2N+ 1, +2, ETC. (TRISOMY)
INTRODUCTION:
DEFINITION OF TERMS
POLYPLOID- multiples of haploid #;
entire set of chrs fail to divide & all the chrs
are segregated in a single daughter cell
TRIPLOID (3N)= 69
TETRAPLOID (4N)= 92
Congenital Disorders
Non Genetic:
Developmental defects – Malformations
Genetic Disorders
Chromosomal
Gene - Mendelian
Multifactorial
Mutations:
Genome: whole set – Polyploidy 4n, 8n etc.
Chromosomal: change in chromosome
Number: Trisomy, monosomy
Structure: Deletion, Translocation etc.
Gene: Submicroscopic
Point mutation – single base sequence
Deletions
Insertions
Cytogenetic Abnormalities:
Abnormal # of chrs:
Non-disjunction - Down’s Syndrome
Anaphase lag - Turner’s xxx
Abnormal Structure: (normal #)
Deletion - 5q- Cri - du - chat syndrome
Inversion -
Translocation - Ph Chromosome - t(9:22) CML,
GENETIC PATHOLOGY:
DEFINITION: Abnormalities or disease states that
may or may not be congenital, transmitted by genes
or chromosomal aberrations, that may be heritable
(familial) or mutational
If mutational, may give the following outcomes:
Heritable
Disappear
Lethal
Sterility
Malignancy
CATEGORIES:
CHROMOSOMAL ABNORMALITIES/
MUTATIONS
GENE ABNORMALITIES/ MUTATIONS
POLYGENIC/ MULTIFACTORIAL
ABNORMALITIES
I. CHROMOSOMAL ABNORMALITIES/
MUTATIONS
GENERAL CONCEPTS:
Children born to older women show more
chromosomal aberrations than children born
to younger women
Most major chromosomal abnormalities are
incompatible w/ life
Detectable by karyotyping (chromosomal
analysis) w/ or w/o banding techniques (use
of stains)
I. CHROMOSOMAL ABNORMALITIES/
MUTATIONS::: TYPES:
NONDISJUNCTION (Chromosomal numerical
aberration)- failure of chrs to sort themselves
in equal #s into daughter cells
SUBTYPES:
POLYPLOIDY- see previous definition
ANEUPLOIDY- see previous definition
MOSSAICISM/ MYXOPLOIDY
Non-disjunction:
I. ANEUPLOIDY: TRISOMY
TRISOMY- presence of 3 homologous
chromosome in a cell
AUTOSOMAL TRISOMY- viable throughout
pregnancy, even live born but die soon after
birth except Down's syndrome
TRISOMY 21- DOWN'S SYNDROME
TRISOMY 18- EDWARD'S SYNDROME
TRISOMY 13- PATAU'S SYNDROME
I. ANEUPLOIDY: TRISOMY
SEX CHR. TRISOMY- abnormal
development but non lethal; # of X chr. is
directly proportional to mental retardation
while number of Y chr. is directly proportional
to aggressive behavior
TRIPLE X
I. ANEUPLOIDY: MONOSOMY
MONOSOMY- absence of one of a pair of
homologous chr
AUTOSOMAL MONOSOMY- IUFD is the usual
outcome
SEX CHR. MONOSOMY- compatible w/ life only
if the conserved chr is an X, if not it will be less
viable
• TURNER'S SYNDROME- 45, XO
Hydrops Fetalis – Monosomy X:
I. ANEUPLOIDY:
MOSSAICISM/ MYXOPLOIDY
MOSSAICISM/ MYXOPLOIDYnondisjunction at a later cell division resulting
to population of normal & trisomic or
monosomic cells coexisting in an individual
AUTOSOMAL MOSSAICISM- rare & lethal
SEX CHR. MOSSAICISM- common
• GONADAL DYSGENESIS- TURNER'S
SYNDROME 45, XO
• KLINEFELTER'S SYNDROME 47 XXY
I. CHROMOSOMAL ABNORMALITIES/
MUTATIONS::: TYPES: I. MORPHOLOGIC/
STRUCTURAL SUBTYPES:
DELETION- loss of chromosomal material
following a break in the chr arm or partial
monosomy
CRI DU CHAT- partial monosomy of p5
RETINOBLASTOMA- q13
WILM'S TUMOR ANIRIDIA SYNDROME- p11
I. MORPHOLOGIC/
STRUCTURAL SUBTYPES:
TRANSLOCATION- transfer of segment of
chromosomal material to another chromosome
leading to imbalance of material in each daughter
cell between non homologous chr
RECIPROCAL- acentric segments of chr exchanged for
similar segment from a heterologous chr; use banding
techniques for detection
ROBERTSONIAN (CENTRIC FUSION)- 2 acrocentric chr
broken near centromere, exchange 2 arms and form new
large metacentric chr and a small fragment, devoid of
centromere & lost during subsequent division
I. MORPHOLOGIC/
STRUCTURAL SUBTYPES:
TRANSLOCATION
BALANCED- transfer w/ no loss of genetic
material; individuals are normal except for
infertility & if fertile, have a high risk of having
malformed offspring
UNBALANCED- transmitted in the haploid
gamete & paired w/ a new set of genes from the
other parent
• MALIGNANT LYMPHOMA- between 8 & 14
• LEUKEMIAS- between 22 & 9
• DOWN'S SYNDROME- chr 21
I. MORPHOLOGIC/
STRUCTURAL SUBTYPES:
TRANSLOCATION
ISOCHROMOSOMAL- faulty division of
centromere at the transverse plane of the long
axis w/ formation of a pair of isochromosome (one
short arm & one long arm)
• TURNER'S SYNDROME
I. MORPHOLOGIC/
STRUCTURAL SUBTYPES:
INVERSION- break of a chr at 2 points,
followed by inversion of the intermediate
segments & reunion results in the formation of
a chr w/ rearranged distribution of genes
PERICENTRIC- rotation occurs around the
centromere
PARACENTRIC- rotation occurs only on the
acentric portion of the arm
I. MORPHOLOGIC/
STRUCTURAL SUBTYPES:
RING CHROMOSOME- break in the
telomeric ends of the chr followed by deletion
of the broken acentric segments & end to end
fusion of the remaining portion
II. GENE ABNORMALITIES/ MUTATIONS
GENERAL CONCEPTS:
Single gene defect detectable in the phenotype
Modified by penetrance, expressivity & whether
defect is dominant, intermediate, recessive or X
linked
Dominant pattern of inheritance usually due to
alteration of aa sequence in the gene
Recessive pattern of inheritance (inborn errors of
metabolism) usually is due to manufacture of
abnormal enzymes or enzyme deficiencies
Follows Mendelian patterns of inheritance
PATTERNS OF INHERITANCE:
AUTOSOMAL DOMINANT
Autosome- gene location
Gene expression- both homozygous & heterozygous
state
Transmission of traits in every generation unless
Low penetrance or modified by gene mutations
Unaffected family members do not transmit trait to
offspring; affected family members usually
heterozygous & transmit trait to only half of the
offspring
M=F
PATTERNS OF INHERITANCE: AUTOSOMAL
DOMINANT
Pp x pp
Pp : Pp : pp : pp
DIABETIS INSIPIDUS
MUSCULAR DYSTROPHY
POLYDACTYLISM
MARFAN'S SYNDROME
ACHONDROPLASTIC DWARFISM
HUNTINGTON'S CHOREA
GARDNER'S SYNDROME
GOUT
HEMOCHROMATOSIS
PATTERNS OF INHERITANCE: AUTOSOMAL
RECESSIVE
Autosome- gene location
Gene expression only in the homozygous state
Both parents usually heterozygous for the trait &
clinically unaffected
Symptoms appear in 25% of offspring
50% of all siblings will be heterozygous for the trait
thus assymptomatic
M=F
PATTERNS OF INHERITANCE: AUTOSOMAL
RECESSIVE
Nn x Nn
CYSTIC FIBROSIS
NN : Nn : Nn : nn
GLYCOGEN STORAGE
DISEASES
ANDROGENITAL
SYNDROME
ALBINISM
ALKAPTONURIA
DEAF MUTISM
MUCOPOLYSACCHARI
DOSIS
LIPID STORAGE
DISEASE
GALACTOSEMIA
WILSON'S DISEASE
PHENYLKETONURIA
TYROSINOSIS
FAMILIAL GOITROUS
CRETINISM
BILIRUBIN METABOLIC
ABNORMALITIES
PATTERNS OF INHERITANCE:
X LINKED RECESSIVE
X chromosome - Gene location
Expression of traits
100% heterozygous male
Rare homozygous female
Partial heterozygous female if X Chromosome inactivation
occurs
Transmission via asymptomatic female
Each son of heterozygous female carrier has 1 in 2 chances of
having the disease
Affected males do not transmit trait to their sons, only to their
daughters; Unaffected males do not transmit the gene
PATTERNS OF INHERITANCE:
X LINKED RECESSIVE
FEMALE
X
MALE
(HEMOPHILIAC)
XX
x
Xh Y
XXh : XY : XXh : XY
FEMALE (CARRIER) x
MALE (NORMAL)
Xh X
x
XY
Xh X : Xh Y : XX : XY
HEMOPHILIC
COLOR
BLINDNESS
G6 PD
DEFICIENCY
MUSCULAR
DYSTROPHYDUCHENNE
TYPE
PATTERNS OF INHERITANCE:
X LINKED DOMINANT
Rare
Affected heterozygous female transmit to 50%
sons & 50% daughters
Affected males transmit to 100% daughters &
none to their sons
VIT. D RESISTANT RICKETS
PATTERNS OF INHERITANCE:
Y LINKED
Not clinically significant
Hairy ears
III. POLYGENIC/ MULTIFACTORIAL
ABNORMALITIES
GENERAL CONCEPTS:
Environmentally influenced interactions of a
number of different gene pairs
HYPERTENSION
DIABETIS MELLITUS
PEPTIC ULCER
OTHER CONGENITAL HEART DISEASES
CHROMOSOMAL DISEASES:
SEX CHROMOSOMAL ABNORMALITIES
X DEFICIENCY
TURNER'S SYNDROME 45, XO
• Short stature female w/ webbed neck, cubitus
valgus, immature genitalia w/ small fibrotic (streak)
ovaries, coarctation of aorta; mostly abort; no Barr
Bodies; almost 50% are mossaics w/ less stigmata
ULLRICH NOONAN SYNDROME (46, XX or XY
::: 46, X(Xq)
• Turner like phenotype; often w/ pulmonary stenosis;
giant Barr Bodies
CHROMOSOMAL DISEASES:
SEX CHROMOSOMAL ABNORMALITIES
KLINEFELTER'S SYNDROME 47, XXY
Most common of X chromosomal abnormality
Tall eunuchoid male w/ gynecomastia, small
testis w/o spermatogenesis (infertile)
Mossaics occur
CHROMOSOMAL DISEASES:
SEX CHROMOSOMAL ABNORMALITIES
MISCELLANEOUS SYNDROMES
TRIPLE X (47 XXX)- mildly retarded; normal
female phenotype
47 XYY- tall, aggressive, mildly retarded male;
increased incidence among criminal
CHROMOSOMAL DISEASES:
SEX CHROMOSOMAL ABNORMALITIES
INTERSEX STATES- HERMAPHRODITISM
TRUE HERMAPHRODITE- XX or XY or both;
variable phenotype, both ovaries & testis are
present
PSEUDOHERMAPHRODITES (NORMAL
GENECITY)
• Male phenotypically female; testicular feminization
• Female phenotypically male; virilizing ovarian or
adrenal tumors
CHROMOSOMAL DISEASES:
AUTOSOMAL ABNORMALITIES
More severe effects than X chr anomalies
Monosomies more severe than trisomies
The larger chromosome involved, the more
serious the phenotypic disorder
CHROMOSOMAL DISEASES:
AUTOSOMAL ABNORMALITIES
DOWN'S SYNDROME- TRISOMY 21,
MONGOLISM; 47 G21+
Most common of the trisomies; maternal risks
increases w/ age; incidence equal in both sexes;
usually due to maternal nondisjunction
Floppy infants w/ psychomotor retardation,
mongoloid facies, epicanthic folds, flat nose,
cardiovascular anomalies, simian palm creases,
cryptorchidism, increased incidence of leukemia
Variant - Translocation type (heritable)- occurs at any
maternal age; 46 XY -D; +tDqGq
Downs Karyotype: Trisomy-21
Downs
Sy.
Trisomy
-21
Downs Syndrome - Trisomy-21
Downs Syndrome - Trisomy-21
Simian Crease
Downs Syndrome:
Mental retardation
Neck folds
Epicanthic folds
Flat facial profile
Simian crease
Hypotonia
Umbilical hernia
Leukemia
CHROMOSOMAL DISEASES:
AUTOSOMAL ABNORMALITIES
EDWARD'S SYNDROME (16 - 18 TRISOMY, E
TRISOMY); 47, E18+
Female predilection; low set ears, epicanthic folds,
micrognathia, CVS anomalies, overlapping 2nd & 5th
finger, rocker bottom feet, renal anomalies, early death
PATAU'S SYNDROME (13 - 15 TRISOMY, D
TRISOMY); 47, D13+
Least common, both sexes equally affected; low set ears,
micropthalmia, brain anomalies, cleft lip & palate,
overlapping 2nd & 5th finger, CVS anomalies, rocker
bottom feet
Cleft Lip - Trisomy 13:
Polydactyly - Trisomy 13:
CHROMOSOMAL DISEASES:
AUTOSOMAL ABNORMALITIES
CRI DU CHAT SYNDROME, 5p Rare, common in females, cat cry, moon faced,
retarded, micrognathia, antimongoloid slant, CVS
anomalies
D13p-, D13q-, E18q-, TRIPLOIDY
Severe anomalies, lethal
PHILADELPHIA CHROMOSOME, G22q Associated w/ CML; good prognosis
Syndactyly - Triploidy
Philadelphia Chromosome (Ph)
Reciprocal translocation t(9;22)
Results in bcr/abl gene fusion
c-abl (Abelson) chr 9
bcr (break point cluster region) chr 22
Protein w/ tyrosine kinase activity - plays
critical role in pathogenesis
CML - t(9;22) - (Ph chr)
DISEASES DUE TO GENE ABNORMALITIES
AND MUTATIONS:
AUTOSOMAL DOMINANT ABNORMALITIES
ACHONDROPLASIA
Defective endocndral ossification
Most common type of dwarfism
High incidence of early death
80% sterility
HUNTINGTON'S CHOREA
Progressive neurologic disorder w/ choreic movements,
seizures, dementia, death
Average onset is 35 years of age so offspring is born
before parent is affected
Reproduction not impaired
DISEASES DUE TO GENE ABNORMALITIES
AND MUTATIONS:
AUTOSOMAL DOMINANT ABNORMALITIES:
MARFAN SYNDROME
Complex defective formation of collagen & elastin
Tall, long extremities (arachnodactyly), subluxation of lens,
cystic medial necrosis of aorta w/ dissecting aneurysm
Mechanism is single gene w/ multiple effects (pleiotropy),
variable expression, forme fruste expression, may skip
generations
GARDNER SYNDROME
Complex cyst of the skin, osteomas, lower intestinal polyps
with development of colonic ca
Pleiotropy
Cell
Cycle
Mitosis
Meiosis
Reduction Division (4n-2n)
Prophase-1(Synapsis, g.rec)
Metaphase-1
Anaphase-1
Telophase-1
Equatorial Division (2n-n)
Prophase-2
Metaphase-2
Anaphase-2
Telophase-2