Theme 5: How Do We Control Our Fertility?
The process in which an organism develops from a single-celled zygote to a multi-cellular organism is complex and well-regulated. The early stages of embryonic development are also crucial for ensuring the fitness of the organism.
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Fertilization
Fertilization, pictured inFigure 1ais the process in which gametes (an egg and sperm) fuse to form a zygote. The egg and sperm each contain one set of chromosomes. To ensure that the offspring has only one complete diploid set of chromosomes, only one sperm must fuse with one egg. In mammals, the egg is protected by a layer of extracellular matrix consisting mainly of glycoproteins called thezona pellucida. When a sperm binds to the zona pellucida, a series of biochemical events, called theacrosomal reactions, take place. In placental mammals, the acrosome contains digestive enzymes that initiate the degradation of the glycoprotein matrix protecting the egg and allowing the sperm plasma membrane to fuse with the egg plasma membrane, as illustrated inFigure 1b. The fusion of these two membranes creates an opening through which the sperm nucleus is transferred into the ovum. The nuclear membranes of the egg and sperm break down and the two haploid genomes condense to form a diploid genome.
To ensure that no more than one sperm fertilizes the egg, once the acrosomal reactions take place at one location of the egg membrane, the egg releases proteins in other locations to prevent other sperm from fusing with the egg. If this mechanism fails, multiple sperm can fuse with the egg, resulting inpolyspermy. The resulting embryo is not genetically viable and dies within a few days.
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Cleavage and Blastula Stage
The development of multi-cellular organisms begins from a single-celled zygote, which undergoes rapid cell division to form the blastula. The rapid, multiple rounds of cell division are termed cleavage. Cleavage is illustrated in Figure 2a. After the cleavage has produced over 100 cells, the embryo is called a blastula. The blastula is usually a spherical layer of cells (the blastoderm) surrounding a fluid-filled or yolk-filled cavity (the blastocoel). Mammals at this stage form a structure called the blastocyst, characterized by an inner cell mass that is distinct from the surrounding blastula, shown inFigure 2b. During cleavage, the cells divide without an increase in mass; that is, one large single-celled zygote divides into multiple smaller cells. Each cell within the blastula is called a blastomere.
In mammals, the blastula forms theblastocystin the next stage of development. Here the cells in the blastula arrange themselves in two layers: theinner cell mass, and an outer layer called thetrophoblast. The inner cell mass is also known as the embryoblast and this mass of cells will go on to form the embryo. At this stage of development, illustrated inFigure 3the inner cell mass consists of embryonic stem cells that will differentiate into the different cell types needed by the organism. The trophoblast will contribute to the placenta and nourish the embryo.
Link to Learning
Visit theVirtual Human Embryo projectat the Endowment for Human Development site to step through an interactive that shows the stages of embryo development, including micrographs and rotating 3-D images.
Gastrulation
The typical blastula is a ball of cells. The next stage in embryonic development is the formation of the body plan. The cells in the blastula rearrange themselves spatially to form three layers of cells. This process is calledgastrulation. During gastrulation, the blastula folds upon itself to form the three layers of cells. Each of these layers is called a germ layer and each germ layer differentiates into different organ systems.
The three germs layers, shown inFigure 4, are the endoderm, the ectoderm, and the mesoderm. The ectoderm gives rise to the nervous system and the epidermis. The mesoderm gives rise to the muscle cells and connective tissue in the body. The endoderm gives rise to columnar cells found in the digestive system and many internal organs.
Are Designer Babies in Our Future?
If you could prevent your child from getting a devastating genetic disease, would you do it? Would you select the sex of your child or select for their attractiveness, strength, or intelligence? How far would you go to maximize the possibility of resistance to disease? The genetic engineering of a human child, the production of “designer babies” with desirable phenotypic characteristics, was once a topic restricted to science fiction. This is the case no longer: science fiction is now overlapping into science fact. Many phenotypic choices for offspring are already available, with many more likely to be possible in the not too distant future. Which traits should be selected and how they should be selected are topics of much debate within the worldwide medical community. The ethical and moral line is not always clear or agreed upon, and some fear that modern reproductive technologies could lead to a new form of eugenics.
Eugenics is the use of information and technology from a variety of sources to improve the genetic makeup of the human race. The goal of creating genetically superior humans was quite prevalent (although controversial) in several countries during the early 20th century (Figure 5), but fell into disrepute when Nazi Germany developed an extensive eugenics program in the 1930’s and 40’s. As part of their program, the Nazis forcibly sterilized hundreds of thousands of the so-called “unfit” and killed tens of thousands of institutionally disabled people as part of a systematic program to develop a genetically superior race of Germans known as Aryans. Ever since, eugenic ideas have not been as publicly expressed, but there are still those who promote them.
Efforts have been made in the past to control traits in human children using donated sperm from men with desired traits. In fact, eugenicist Robert Klark Graham established a sperm bank in 1980 that included samples exclusively from donors with high IQs. The “genius” sperm bank failed to capture the public’s imagination and the operation closed in 1999.
In more recent times, the procedure known as prenatal genetic diagnosis (PGD) has been developed. PGD involves the screening of human embryos as part of the process ofin vitrofertilization, during which embryos are conceived and grown outside the mother’s body for some period of time before they are implanted. The term PGD usually refers to both the diagnosis, selection, and the implantation of the selected embryos.
In the least controversial use of PGD, embryos are tested for the presence of alleles which cause genetic diseases such as sickle cell disease, muscular dystrophy, and hemophilia, in which a single disease-causing allele or pair of alleles has been identified. By excluding embryos containing these alleles from implantation into the mother, the disease is prevented, and the unused embryos are either donated to science or discarded. There are relatively few in the worldwide medical community that question the ethics of this type of procedure, which allows individuals scared to have children because of the alleles they carry to do so successfully. The major limitation to this procedure is its expense. Not usually covered by medical insurance and thus out of reach financially for most couples, only a very small percentage of all live births use such complicated methodologies. Yet, even in cases like these where the ethical issues may seem to be clear-cut, not everyone agrees with the morality of these types of procedures. For example, to those who take the position that human life begins at conception, the discarding of unused embryos, a necessary result of PGD, is unacceptable under any circ*mstances.
A murkier ethical situation is found in the selection of a child’s sex, which is easily performed by PGD. Currently, countries such as Great Britain have banned the selection of a child’s sex for reasons other than preventing sex-linked diseases. Other countries allow the procedure for “family balancing”, based on the desire of some parents to have at least one child of each sex. Still others, including the United States, have taken a scattershot approach to regulating these practices, essentially leaving it to the individual practicing physician to decide which practices are acceptable and which are not.
Even murkier are rare instances of disabled parents, such as those with deafness or dwarfism, who select embryos via PGD to ensure that they share their disability. These parents usually cite many positive aspects of their disabilities and associated culture as reasons for their choice, which they see as their moral right. To others, to purposely cause a disability in a child violates the basic medical principle ofPrimum non nocere,“first, do no harm.” This procedure, although not illegal in most countries, demonstrates the complexity of ethical issues associated with choosing genetic traits in offspring.
Where could this process lead? Will this technology become more affordable and how should it be used? With the ability of technology to progress rapidly and unpredictably, a lack of definitive guidelines for the use of reproductive technologies before they arise might make it difficult for legislators to keep pace once they are in fact realized, assuming the process needs any government regulation at all. Other bioethicists argue that we should only deal with technologies that exist now, and not in some uncertain future. They argue that these types of procedures will always be expensive and rare, so the fears of eugenics and “master” races are unfounded and overstated. The debate continues.
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Section Summary
The early stages of embryonic development begin with fertilization. The process of fertilization is tightly controlled to ensure that only one sperm fuses with one egg. After fertilization, the zygote undergoes cleavage to form the blastula. The blastula, which in some species is a hollow ball of cells, undergoes a process called gastrulation, in which the three germ layers form. The ectoderm gives rise to the nervous system and the epidermal skin cells, the mesoderm gives rise to the muscle cells and connective tissue in the body, and the endoderm gives rise to columnar cells and internal organs.
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Glossary
- acrosomal reaction
- series of biochemical reactions that the sperm uses to break through the zona pellucida
- blastocyst
- structure formed when cells in the mammalian blastula separate into an inner and outer layer
- gastrulation
- process in which the blastula folds over itself to form the three germ layers
- inner cell mass
- inner layer of cells in the blastocyst
- polyspermy
- condition in which one egg is fertilized by multiple sperm
- trophoblast
- outer layer of cells in the blastocyst
- zona pellucida
- protective layer of glycoproteins on the mammalian egg
I'm an expert in developmental biology, particularly in the intricate processes that govern embryonic development and fertility control. My depth of knowledge extends from the initial stages of fertilization to the formation of germ layers during gastrulation. To demonstrate my expertise, I'll delve into the concepts introduced in the provided article.
Fertilization: Fertilization is the process by which gametes (sperm and egg) fuse to form a zygote. In mammals, this process involves the sperm binding to the zona pellucida, triggering acrosomal reactions. These reactions, facilitated by enzymes in the acrosome, lead to the breakdown of the glycoprotein matrix surrounding the egg. This allows the fusion of the sperm plasma membrane with the egg plasma membrane, resulting in the transfer of the sperm nucleus into the ovum. To prevent polyspermy, the release of proteins by the egg in other locations serves as a mechanism to inhibit additional sperm from fusing with the egg.
Cleavage and Blastula Stage: Following fertilization, the zygote undergoes rapid cell division known as cleavage, producing a blastula. Cleavage leads to the formation of blastomeres, and after around 100 cells have formed, the embryo is termed a blastula. In mammals, this stage progresses to the blastocyst, featuring an inner cell mass (embryoblast) that will give rise to the embryo and an outer layer (trophoblast) that contributes to the placenta. Cleavage is marked by cell division without an increase in mass, resulting in multiple smaller cells from a single large zygote.
Gastrulation: Gastrulation is the next crucial stage in embryonic development. During gastrulation, the blastula undergoes spatial rearrangement to form three germ layers: endoderm, ectoderm, and mesoderm. The ectoderm contributes to the nervous system and epidermis, the mesoderm gives rise to muscle cells and connective tissue, and the endoderm forms columnar cells in the digestive system and internal organs. This process establishes the basic body plan of the developing organism.
Relevance to Fertility Control: The provided article introduces the fascinating topic of controlling fertility, touching on the early stages of embryonic development. While the article doesn't explicitly address fertility control methods, understanding the intricacies of fertilization and embryonic development is essential for advancements in reproductive technologies. The article hints at the ethical considerations and potential future scenarios, such as the controversial concept of "designer babies" and the application of reproductive technologies like prenatal genetic diagnosis (PGD).
In conclusion, my expertise encompasses the processes of fertilization, cleavage, blastula formation, and gastrulation, providing a comprehensive understanding of the early stages of embryonic development and their implications for fertility control and reproductive technologies.
