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Chapter 8 The Cellular Basis of Reproduction and Inheritance Rain Forest Rescue • Scientists in Hawaii are attempting to "rescue" endangered species from extinction by promoting reproduction • Reproduction is one phase of an organism's life cycle – Sexual reproduction • Fertilization of sperm and egg produces offspring – Asexual reproduction • Offspring are produced by a single parent, without the participation of sperm and egg • Cell division is at the heart of organismal reproduction CONNECTIONS BETWEEN CELL DIVISION AND REPRODUCTION 8.1 Like begets like, more or less • Asexual reproduction – Chromosomes are duplicated and cell divides – Each daughter cell is genetically identical to the parent and the other daughter • Sexual reproduction – Each offspring inherits a unique combination of genes from both parents – Offspring can show great variation Copyright © 2005 Pearson Education, Inc. publishing as Benjamin Cummings 8.2 Cells arise only from preexisting cells • "Every cell from a cell" is at the heart of the perpetuation of life – Can reproduce an entire unicellular organism – Is the basis of sperm and egg formation – Allows for development from a single fertilized egg to an adult organism – Functions in an organism's renewal and repair 8.3 Prokaryotes reproduce by binary fission • Prokaryotic cells reproduce asexually by a type of cell division called binary fission – Genes are on one circular DNA molecule – The cell replicates its single chromosome – The chromosome copies move apart – The cell elongates – The plasma membrane grows inward, dividing the parent into two daughter cells LE 8-3a Plasma membrane Prokaryotic chromosome Cell wall Duplication of chromosome and separation of copies Continued elongation of the cell and movement of copies Division into two daughter cells LE 8-3b Colorized TEM 32,500 Prokaryotic chromosomes THE EUKARYOTIC CELL CYCLE AND MITOSIS 8.4 The large, complex chromosomes of eukaryotes duplicate with each cell division • Eukaryotic genes – Many more than in prokaryotes – Grouped into multiple chromosomes in the nucleus • Eukaryotic chromosomes – Contain a very long DNA molecule associated with proteins – Most of the time occur in the form of thin, loosely packed chromatin fibers – Condense into visible chromosomes just before cell division • Eukaryotic cell division – Chromosomes replicate • Sister chromatids joined together at the centromere – Sister chromatids separate • Now called chromosomes – Cell divides into two daughter cells • Each with a complete and identical set of chromosomes LE 8-4b Sister chromatids Centromere LE 8-4c Chromosome duplication Centromere Sister chromatids Chromosome distribution to daughter cells 8.5 The cell cycle multiplies cells • The cell cycle is an ordered series of events extending from the time a cell is formed until it divides into two • Most of the cell cycle is in interphase – G1: cell grows in size – S: DNA synthesis (replication) occurs – G2: Cell continues to grow and prepare for division • The cell actually divides in mitotic (M) phase – Mitosis: nuclear division – Cytokinesis: cytoplasmic division – Duplicated chromosomes evenly distributed into two daughter nuclei LE 8-5 INTERPHASE S (DNA synthesis) G1 G2 8.6 Cell division is a continuum of dynamic changes • Interphase: Duplication of the genetic material ends when chromosomes begin to become visible • Prophase (the first stage of mitosis): The mitotic spindle is forming. Centrosomes migrate to opposite ends of the cell • Prometaphase: Chromatins completely coil into chromosomes; nucleoli and nuclear membrane disperse • Metaphase: The spindle is fully formed; chromosomes are aligned single file with centromeres on the metaphase plate • Anaphase: Chromosomes separate from the centromere, dividing to arrive at poles • Telophase: Cell elongation continues, a nuclear envelope forms around chromosomes, chromosomes uncoil, and nucleoli reappear • Cytokinesis: The cytoplasm divides LE 8-6a INTERPHASE Centrosomes (with centriole pairs) Nucleolus Nuclear envelope PROPHASE Chromatin Plasma membrane Early mitotic spindle PROMETAPHASE Centrosome Chromosome, consisting of two sister chromatids Centromere Fragments of nuclear envelope Kinetochore Spindle microtubules LE 8-6b METAPHASE ANAPHASE Cleavage furrow Metaphase plate Spindle TELOPHASE AND CYTOKINESIS Daughter chromosomes Nuclear envelope forming Nucleolus forming 8.7 Cytokinesis differs for plant and animal cells • Animals – Ring of microfilaments contracts into cleavage furrow – Cleavage occurs • Plants – Vesicles fuse into a membranous cell plate – Cell plate develops into a new wall between two daughter cells Animation: Cytokinesis LE 8-7a Cleavage furrow Cleavage furrow Contracting ring of microfilaments Daughter cells LE 8-7b Cell plate forming Wall of parent cell Cell wall Vesicles containing cell wall material Daughter nucleus New cell wall Cell plate Daughter cells 8.8 Anchorage, cell density, and chemical growth factors affect cell division • An organism must be able to control the timing of cell division • Anchorage dependence – Most animal cells must be in contact with a solid surface to divide • Density-dependent inhibition – Cells form a single layer – Cells stop dividing when they touch one another – Inadequate supply of growth factor causes division to stop LE 8-8a Cells anchor to dish surface and divide. When cells have formed a complete single layer, they stop dividing (density-dependent Inhibition). If some cells are scraped away, the remaining cells divide to fill the dish with a single layer and then stop (density-dependent inhibition). LE 8-8b After forming a single layer, cells have stopped dividing. Providing an additional supply of growth factors stimulates further cell division. 8.9 Growth factors signal the cell cycle control system • The cell cycle control system regulates the events of the cell cycle • If a growth factor is not released at three major checkpoints, the cell cycle will stop – G1 of interphase – G2 of interphase – M phase LE 8-9a G1 checkpoint G0 Control system G1 M M checkpoint G2 checkpoint G2 S • How a growth factor might affect the cell cycle control system – Cell has receptor protein in plasma membrane – Binding of growth factor to receptor triggers a signal transduction pathway • Molecules induce changes in other molecules – Signal finally overrides brakes on the cell cycle control system LE 8-9b Growth factor Plasma membrane Relay proteins Receptor protein Signal transduction pathway G1 checkpoint Control system G1 M S G2 CONNECTION 8.10 Growing out of control, cancer cells produce malignant tumors • Cancer cells do not respond normally to the cell cycle control system – Divide excessively – Can invade other tissues – May kill the organism • If an abnormal cell avoids destruction by the immune system, it may form a tumor – Benign: abnormal cells remain at original site – Malignant: abnormal cells can spread to other tissues and parts of the body – Metastasis: spread of cancer cells through the circulatory system LE 8-10 Lymph vessels Tumor Blood vessel Glandular tissue A tumor grows from a single cancer cell. Cancer cells invade Neighboring tissue. Cancer cells spread through lymph and blood vessels to other parts of the body. • Cancers are named according to location of origin – Carcinoma: external or internal body coverings – Sarcoma: tissues that support the body – Leukemia and lymphoma: blood-forming tissues • Radiation and chemotherapy are effective as cancer treatments because they interfere with cell division 8.11 Review of the functions of mitosis: growth, cell replacement, and asexual reproduction • When the cell cycle operates normally, mitotic cell division functions in – Growth – Replacement of damaged or lost cells – Asexual reproduction Video: Hydra Budding MEIOSIS AND CROSSING OVER 8.12 Chromosomes are matched in homologous pairs • The somatic (body) cells of each species contain a specific number of chromosomes • Humans and most other organisms have pairs of homologous chromosomes – Carry genes for the same characteristics at the same place, or locus • Except sex chromosomes – One chromosome is inherited from the female parent, one from the male LE 8-12 Chromosomes Centromere Sister chromatids 8.13 Gametes have a single set of chromosomes • Diploid cells have two sets of chromosomes (2n) – Somatic cells • Haploid cells have one set of chromosomes (n) – Gametes (egg and sperm cells) • Sexual life cycles involve the alternation of haploid and diploid stages – Fusion of haploid gametes in fertilization forms a diploid zygote LE 8-13 Haploid gametes (n = 23) n Egg cell n Sperm cell Meiosis Fertilization Diploid zygote (2n = 46) Multicellular diploid adults (2n = 46) Mitosis and development 2n 8.14 Meiosis reduces the chromosome number from diploid to haploid • Meiosis – Like mitosis, is preceded by chromosome duplication – Unlike mitosis, cell divides twice to form four haploid daughter cells • The process of meiosis includes two consecutive divisions – Meiosis I • In synapsis, homologous chromosomes are paired • In crossing over, homologous chromosomes exchange corresponding segments • Each homologous pair divides into two daughter cells, each with one set of chromosomes consisting of two chromatids • Meiosis II – Essentially the same as mitosis – Sister chromatids of each chromosome separate – Result is four cells, each with half as many chromosomes as the parent LE 8-14a MEIOSIS I : Homologous chromosome separate INTERPHASE PROPHASE I METAPHASE I ANAPHASE I Centrosomes (with centriole pairs) Microtubules Sister chromatids Sites of crossing over attached to Metaphase remain attached plate kinetochore Spindle Nuclear envelope Sister chromatids Chromatin Tetrad Centromere (with kinetochore) Homologous chromosomes separate LE 8-14b MEIOSIS II : Sister chromatids separate TELOPHASE I AND CYTOKINESIS PROPHASE II METAPHASE II ANAPHASE II TELOPHASE II AND CYTOKINESIS Cleavage furrow Sister chromatids separate Haploid daughter cells forming 8.15 Review: A comparison of mitosis and meiosis • Mitosis – Provides for growth, tissue repair, and asexual reproduction – Produces daughter cells genetically identical to the parent • Meiosis – Needed for sexual reproduction – Produces daughter cells with one member of each homologous chromosome pair LE 8-15 MITOSIS MEIOSIS Site of crossing over Parent cell (before chromosome replication) MEIOSIS I Prophase I Prophase Tetrad formed by synapsis of homologous chromosomes Chromosome replication Chromosome replication Duplicated chromosome (two sister chromatids) 2n = 4 Chromosomes align at the metaphase plate Metaphase Anaphase Telophase Sister chromatids separate during anaphase 2n 2n Daughter cells of mitosis Tetrads align at the metaphase plate Metaphase I Anaphase I Telophase I Homologous chromosomes separate during anaphase I; sister chromatids remain together No further chromosomal replication; sister chromatids separate during anaphase II Haploid n=2 Daughter cells of meiosis I MEIOSIS II n n n Daughter cells of meiosis II n 8.16 Independent orientation of chromosomes in meiosis and random fertilization lead to varied offspring • Reshuffling of the different versions of genes during sexual reproduction produces genetic variation – Random arrangements of chromosome pairs at metaphase I of meiosis lead to many different combinations of chromosomes – Random fertilization of eggs by sperm greatly increases this variation Animation: Genetic Variation LE 8-16 Possibility 1 Possibility 2 Two equally probable arrangements of chromosomes at metaphase I Metaphase II Gametes Combination 1 Combination 2 Combination 3 Combination 4 8.17 Homologous chromosomes carry different versions of genes • Each chromosome of a homologous pair can bear different versions of genes at corresponding loci – Makes gametes (and thus offspring) different from one another – Examples: coat color and eye color in mice LE 8-17a Coat-color genes Eye-color genes Brown Black C E C E C E c e c e Meiosis c e White Pink Tetrad in parent cell (homologous pair of duplicated chromosomes) Chromosomes of the four gametes LE 8-17b Brown coat (C); black eyes (E) White coat (c); pink eyes (e) 8.18 Crossing over further increases genetic variability • Crossing over is a genetic rearrangement between two homologous chromosomes – Homologues pair up into a tetrad during prophase I of meiosis – Maternal and paternal chromatids break at the same place – The two broken chromatids join together in a new way at the chiasma Animation: Crossing Over TEM 2,200 LE 8-18a Tetrad Chiasma Centromere – When homologous chromosomes separate at anaphase I, each contains a new segment – In meiosis II, each sister chromatid goes to a different gamete – Gametes of four genetic types result LE 8-18b Coat-color genes Eye-color genes C E Tetrad (homologous pair of chromosomes in synapsis) c e Breakage of homologous chromatids C E c e Joining of homologous chromatids C E Chiasma c e Separation of homologous chromosomes at anaphase I C E C e c E c e Separation of chromatids at anaphase II and completion of meiosis C E Parental type of chromosome C e Recombinant chromosome c E c e Recombinant chromosome Parental type of chromosome Gametes of four genetic types ALTERATIONS OF CHROMOSOME NUMBER AND STRUCTURE 8.19 A karyotype is a photographic inventory of an individual's chromosomes • A blood sample is treated with a chemical that stimulates mitosis • After several days, another chemical arrests mitosis at anaphase, when chromosomes are most highly condensed • Chromosomes are photographed and electronically arranged by size and shape into the karyotype • Normal humans have 22 pairs of autosomes and two sex chromosomes Copyright © 2005 Pearson Education, Inc. publishing as Benjamin Cummings LE 8-19 Packed red and white blood cells Blood culture Hypotonic solution Fixative White blood cells Centrifuge Stain Fluid Centromere Siste c r hromatids 2,600 Pair of homologous chromosomes CONNECTION 8.20 An extra copy of chromosome 21 causes Down syndrome • A person may have an abnormal number of chromosomes • Down syndrome is caused by trisomy 21, an extra copy of chromosome 21 – The most common human chromosome number abnormality – Many physical and mental problems – Increased incidence in older mothers LE 8-20c 8.21 Accidents during meiosis can alter chromosome number • Abnormal chromosome count is a result of nondisjunction – The failure of homologous pairs to separate during meiosis I – The failure of sister chromatids to separate during meiosis II LE 8-21a LE 8-21b • Fertilization of an egg resulting from nondisjunction with a normal sperm results in a zygote with an abnormal chromosome number – May be involved in trisomy 21 LE 8-21c CONNECTION 8.22 Abnormal numbers of sex chromosomes do not usually affect survival • Nondisjunction can produce gametes with extra or missing sex chromosomes – Upset the genetic balance less than unusual numbers of autosomes – Lead to varying degrees of malfunction in humans – Usually do not affect survival 8.23 Alterations of chromosome structure can cause birth defects and cancer • Breakage can lead to rearrangements affecting genes on one chromosome – Deletion: loss of a fragment of chromosome – Duplication: addition of a fragment to sister chromatid – Inversion: reattachment of a fragment in reverse order – Inversions least harmful because all genes are present in normal number LE 8-23a • Translocation is the attachment of a chromosomal fragment to a nonhomologous chromosome – Can be reciprocal – May or may not be harmful LE 8-23b • Chromosomal changes in sperm or egg cells can cause congenital disorders • Chromosomal changes in a somatic cell may contribute to the development of cancer LE 8-23c