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BIOL 235 Human Anatomy and Physiology Assignment 3 Questions and correct Answers (Correctly Explained).

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BIOL 235 Human Anatomy and Physiology Assignment 3 Questions and correct Answers (Correctly Explained). 1. Some patients who suffer from hypertension (high blood pressure) are prescribed medications that are in the category of angiotensin-converting enzyme (ACE) inhibitors. Explain why these drugs are used to combat hypertension. When blood volume falls or blood flow to the kidneys decreases, juxtaglomerular cells in the kidneys secrete renin into the bloodstream. In sequence, renin and angiotensinconverting enzyme (ACE) act on their substrates to produce the active hormone angiotensin II, which raises blood pressure in two ways. First, angiotensin II is a potent vasoconstrictor; it raises blood pressure by increasing systemic vascular resistance. Second, it stimulates secretion of aldosterone, which increases reabsorption of sodium ions (Na+) and water by the kidneys. The water reabsorption increases total blood volume, which increases blood pressure. ACE inhibitor prevents an enzyme in the body from producing angiotensin II, a substance that increases blood pressure. 2. Describe the fate of an RBC traveling from the heart to the left elbow and back to the heart. Usually blood passes from the heart and then in sequence through arteries, arterioles, capillaries, venules, and veins and then back to the heart. In some parts of the body, however, blood passes from one capillary network into another through a vein called a portal vein. Such a circulation of blood is called a portal system. The name of the portal system gives the name of the second capillary location. For example, there are portal systems associated with the liver (hepatic portal circulation; and the pituitary gland. Unlike their thick-walled arterial counterparts, venules and veins have thin walls that do not readily maintain their shape. Venules drain the capillary blood and begin the return flow of blood back toward the heart. Although veins are composed of essentially the same three layers as arteries, the relative thicknesses of the layers are different. The tunica interna of veins is thinner than that of arteries; the tunica media of veins is much thinner than in arteries, with relatively little smooth muscle and elastic fibers. The tunica externa of veins is the thickest layer and consists of collagen and elastic fibers. Veins lack the internal or external elastic laminae found in arteries. They are distensible enough to adapt to variations in the volume and pressure of blood passing through them, but are not designed to withstand high pressure. The lumen of a vein is larger than that of a comparable artery, and veins oft en appear collapsed (flattened) when sectioned. The pumping action of the heart is a major factor in moving venous blood back to the heart. The contraction of skeletal muscles in the lower limbs also helps boost venous return to the heart. The average blood pressure in veins is considerably lower than in arteries. The difference in pressure can be noticed when blood flows from a cut vessel. Blood leaves a cut vein in an even, slow flow but spurts rapidly from a cut artery. Most of the structural differences between arteries and veins reflect this pressure difference. For example, the walls of veins are not as strong as those of arteries. Many veins, especially those in the limbs, also contain valves, thin folds of tunica interna that form flaplike cusps. The valve cusps project into the lumen, pointing toward the heart. The low blood pressure in veins allows blood returning to the heart to slow and even back up; the valves aid in venous return by preventing the backflow of blood. 3. Explain the steps that result in antibody production and describe the process that results in an activated B-cell. An antibody (Ab) can combine specifically with the epitope on the antigen that triggered its production. The antibody’s structure matches its antigen much as a lock accepts a specific key. In theory, plasma cells could secrete as many different antibodies as there are different B-cell receptors because the same recombined gene segments code for both the BCR and the antibodies eventually secreted by plasma cells. The body contains not only millions of different T cells but also millions of different B cells, each capable of responding to a specific antigen. Cytotoxic T cells leave lymphatic tissues to seek out and destroy a foreign antigen, but B cells stay put. In the presence of a foreign antigen, a specific B cell in a lymph node, the spleen, or mucosa-associated lymphatic tissue becomes activated. Then it undergoes clonal selection, forming a clone of plasma cells and memory cells. During activation of a B cell, an antigen binds to B-cell receptors (BCRs). These integral transmembrane proteins are chemically similar to the antibodies that eventually are secreted by plasma cells. Although B cells can respond to an unprocessed antigen present in lymph or interstitial fluid, their response is much more intense when they process the antigen. Antigen processing in a B cell occurs in the following way: The antigen is taken into the B cell, broken down into peptide fragments and combined with MHC-II selfantigens, and moved to the B cell plasma membrane. Helper T cells recognize the antigen–MHC-II complex and deliver the costimulation needed for B cell proliferation and differentiation. The helper T cell produces interleukin-2 and other cytokines that function as costimulators to activate B cells. Once activated, a B cell undergoes clonal selection. The result is the formation of a clone of B cells that consists of plasma cells and memory B cells. Plasma cells secrete antibodies. A few days after exposure to an antigen, a plasma cell secretes hundreds of millions of antibodies each day for about 4 or 5 days, until the plasma cell dies. Most antibodies travel in lymph and blood to the invasion site. Interleukin-4 and interleukin-6, also produced by helper T cells, enhance B cell proliferation, B cell differentiation into plasma cells, and secretion of antibodies by plasma cells. Memory B cells do not secrete antibodies. Instead, they can quickly proliferate and differentiate into more plasma cells and more memory B cells should the same antigen reappear at a future time. Different antigens stimulate different B cells to develop into plasma cells and their accompanying memory B cells. All of the B cells of a particular clone are capable of secreting only one type of antibody, which is identical to the antigen receptor displayed by the B cell that first responded. Each specific antigen activates only those B cells that are predestined (by the combination of gene segments they carry) to secrete antibody specific to that antigen. Antibodies produced by a clone of plasma cells enter the circulation and form antigen–antibody complexes with the antigen that initiated their production.

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BIOL 235 Human Anatomy and Physiology Assignment 3
Questions and correct Answers (Correctly Explained).
1. Some patients who suffer from hypertension (high blood pressure) are prescribed
medications that are in the category of angiotensin-converting enzyme (ACE) inhibitors.
Explain why these drugs are used to combat hypertension.

When blood volume falls or blood flow to the kidneys decreases, juxtaglomerular cells in
the kidneys secrete renin into the bloodstream. In sequence, renin and angiotensin-
converting enzyme (ACE) act on their substrates to produce the active hormone
angiotensin II, which raises blood pressure in two ways. First, angiotensin II is a potent
vasoconstrictor; it raises blood pressure by increasing systemic vascular resistance.
Second, it stimulates secretion of aldosterone, which increases reabsorption of sodium
ions (Na+) and water by the kidneys. The water reabsorption increases total blood
volume, which increases blood pressure.

ACE inhibitor prevents an enzyme in the body from producing angiotensin II, a substance
that increases blood pressure.

2. Describe the fate of an RBC traveling from the heart to the left elbow and back to the
heart.

Usually blood passes from the heart and then in sequence through arteries, arterioles,
capillaries, venules, and veins and then back to the heart. In some parts of the body,
however, blood passes from one capillary network into another through a vein called a
portal vein. Such a circulation of blood is called a portal system. The name of the portal
system gives the name of the second capillary location. For example, there are portal
systems associated with the liver (hepatic portal circulation; and the pituitary gland.

Unlike their thick-walled arterial counterparts, venules and veins have thin walls that do
not readily maintain their shape. Venules drain the capillary blood and begin the return
flow of blood back toward the heart.

Although veins are composed of essentially the same three layers as arteries, the relative
thicknesses of the layers are different. The tunica interna of veins is thinner than that of
arteries; the tunica media of veins is much thinner than in arteries, with relatively little
smooth muscle and elastic fibers. The tunica externa of veins is the thickest layer and
consists of collagen and elastic fibers. Veins lack the internal or external elastic laminae
found in arteries. They are distensible enough to adapt to variations in the volume and
pressure of blood passing through them, but are not designed to withstand high pressure.
The lumen of a vein is larger than that of a comparable artery, and veins oft en appear
collapsed (flattened) when sectioned.

, The pumping action of the heart is a major factor in moving venous blood back to the
heart. The contraction of skeletal muscles in the lower limbs also helps boost venous
return to the heart. The average blood pressure in veins is considerably lower than in
arteries. The difference in pressure can be noticed when blood flows from a cut vessel.
Blood leaves a cut vein in an even, slow flow but spurts rapidly from a cut artery. Most of
the structural differences between arteries and veins reflect this pressure difference. For
example, the walls of veins are not as strong as those of arteries.

Many veins, especially those in the limbs, also contain valves, thin folds of tunica interna
that form flaplike cusps. The valve cusps project into the lumen, pointing toward the
heart. The low blood pressure in veins allows blood returning to the heart to slow and
even back up; the valves aid in venous return by preventing the backflow of blood.

3. Explain the steps that result in antibody production and describe the process that results
in an activated B-cell.

An antibody (Ab) can combine specifically with the epitope on the antigen that triggered
its production. The antibody’s structure matches its antigen much as a lock accepts a
specific key. In theory, plasma cells could secrete as many different antibodies as there
are different B-cell receptors because the same recombined gene segments code for both
the BCR and the antibodies eventually secreted by plasma cells.

The body contains not only millions of different T cells but also millions of different B
cells, each capable of responding to a specific antigen. Cytotoxic T cells leave lymphatic
tissues to seek out and destroy a foreign antigen, but B cells stay put. In the presence of a
foreign antigen, a specific B cell in a lymph node, the spleen, or mucosa-associated
lymphatic tissue becomes activated. Then it undergoes clonal selection, forming a clone
of plasma cells and memory cells.

During activation of a B cell, an antigen binds to B-cell receptors (BCRs). These integral
transmembrane proteins are chemically similar to the antibodies that eventually are
secreted by plasma cells. Although B cells can respond to an unprocessed antigen present
in lymph or interstitial fluid, their response is much more intense when they process the
antigen. Antigen processing in a B cell occurs in the following way: The antigen is taken
into the B cell, broken down into peptide fragments and combined with MHC-II self-
antigens, and moved to the B cell plasma membrane. Helper T cells recognize the
antigen–MHC-II complex and deliver the costimulation needed for B cell proliferation
and differentiation. The helper T cell produces interleukin-2 and other cytokines that
function as costimulators to activate B cells.

Once activated, a B cell undergoes clonal selection. The result is the formation of a clone
of B cells that consists of plasma cells and memory B cells. Plasma cells secrete
antibodies. A few days after exposure to an antigen, a plasma cell secretes hundreds of
millions of antibodies each day for about 4 or 5 days, until the plasma cell dies. Most
antibodies travel in lymph and blood to the invasion site. Interleukin-4 and interleukin-6,
also produced by helper T cells, enhance B cell proliferation, B cell differentiation into

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