For each example of weathering, determine whether it is mechanical (physical)weathering or chemical weathering.

1. Glaciers in Antarctica are starting to thaw. The ice starts to crack and pieces break off.

2. After writing with a piece of chalk, the end piece starts to wither away.

3. An Alka-Seltzer tablet starts to bubble and dissolve in a glass of room-temperature water.

4. Slices of apples start to turn brown after being left out for 2 days.

5. Metal fences outside get rained on and start to rust until parts of the fence break off.

Answers

Answer 1

Answer:

1.  Mechanical - ice melting is not a chemical reaction, it is a physical change

2. Mechanical - its force, friction and pressure

3. Chemical - bubbles are a sign of a chemical reaction

4. Chemical - oxidization

5. Rusting is chemical since it is oxidization, parts breaking off could be mechanical if it is due to wind, or some other force.

Explanation:


Related Questions

Eye color in fruit flies is a sex-linked trait. Red eye color is dominant over
white eye color. A homozygous, red-eyed female is crossed with a white-eyed
male.
In their offspring, what is the expected phenotypic ratio of red-eyed females
to white-eyed females to red-eyed males to white-eyed males?
OA. 1:2:1:0
OB. 1:1:1:1
OC. 2:0:1:1
OD. 2:0:2:0

Answers

Answer: D

Explanation: The RR female with the rY male would make 2 RY(red-eyed) males as only the female donates a allele and two Rr(red-eyed) females which are heterozygous

The expected phenotypic ratio of red-eyed females to white-eyed females to red-eyed males to white-eyed males is  1:1:1:1. The correct option is B.

It can be determined based on the principles of sex-linked inheritance.

In this case, since the eye color gene is sex-linked and located on the X chromosome, the genotype of the female parent would be [tex]\rm X^R X^R[/tex](homozygous for red eyes), and the genotype of the male parent would be [tex]X^{W }Y[/tex](white eyes).

The possible genotypes and corresponding phenotypes of the offspring are as follows:

Red-eyed females ([tex]X^R X^R[/tex]): All female offspring from the cross will inherit the red-eye color gene from the homozygous red-eyed mother.White-eyed females ([tex]X^R X^W[/tex]): Female offspring will inherit one red eye color gene from the mother ([tex]X^R[/tex]) and one white eye color gene from the father ([tex]X^W[/tex]).Red-eyed males ([tex]X^R Y[/tex]): Male offspring will inherit the red eye color gene from the mother ([tex]X^R[/tex]) and the Y chromosome from the father.White-eyed males ([tex]X^W Y[/tex]): No white-eyed males will be produced in this cross since the white-eye color gene is recessive and only located on the X chromosome.The expected phenotypic ratio of red-eyed females to white-eyed females to red-eyed males to white-eyed males is 1:1:1:1.

Thus, the correct option is B.

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What are some barriers to using hydrogenase enzymes for H2
generation in commercial schemes?

Answers

Some barriers to using hydrogenase enzymes for H2 generation in commercial schemes include:

Limited stabilitySlow reaction rateCostScaling upCatalyst efficiency

What are hydrogenase enzymes?

Hydrogenase enzymes are a promising option for hydrogen (H2) generation due to their ability to catalyze the reversible reaction of H2 production from protons and electrons.

However, there are several barriers to using hydrogenase enzymes in commercial schemes, including:

Limited stability: Hydrogenase enzymes are sensitive to oxygen and can be easily deactivated, which limits their stability and lifespan.Slow reaction rate: Hydrogenase enzymes have a relatively slow reaction rate compared to other H2 generation methods, which makes them less efficient for commercial-scale production.Cost: The cost of producing and purifying hydrogenase enzymes is high, which can make them economically unfeasible for large-scale production.Scaling up: Scaling up the production of hydrogenase enzymes can be challenging due to their sensitivity to oxygen and the need for strict anaerobic conditions.Catalyst efficiency: While some hydrogenase enzymes have high catalytic activity, others are less efficient, which can limit their effectiveness in H2 generation.

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What is the acceleration of a car initially starting at 7.39 m/s that accelerates to 27.56 m/s in 9 seconds?

Answers

The initial velocity of the car is 7.39 m/s. It is then accelerated to 27.56 m/s within 9 seconds. Then the acceleration of the car is 2.24 m/s².

What is acceleration ?

Acceleration of an object is the rate of change in velocity. It is the ratio of the change in velocity to the time interval. Like velocity, acceleration is a vector quantity characterized by a magnitude and direction.

Let u be the initial velocity and v be the final velocity, a and t be the acceleration and time interval.

then,

v = u + at

(v - u )/t = a.

Given,

u = 7.39 m/s

v = 27.56 m/s

and t = 9 seconds.

then acceleration a =  (27.56 m/s - 7.39 m/s ) /9 s = 2.24 m/s².

Therefore, the acceleration of the car is 2.24 m/s².

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If a physician told you a patient’s abdomen was nontender or the patient’s skin was pale, where would you document this information?

Answers

If a physician told you that a patient's abdomen was nontender or that the patient's skin was pale, you would document this information in the patient's medical record.

Specifically, you would document this information in the "Physical Exam" section of the patient's medical record. This section is used to document the physician's findings from a physical examination of the patient, including any abnormalities or normal findings. It is important to accurately document this information, as it can be used to make a diagnosis and determine the appropriate course of treatment for the patient.

Whether or whether you are experiencing symptoms, a yearly physical check allows you and your doctor to evaluate your overall health. It can also assist you in determining which aspects of your health require attention now in order to avoid more serious problems later.

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The DNA in a human cell weighs approximately 6. 0 x 10^-12 grams. Calculate how many cells you would need to use to extract 1 mg of DNA. Show your work

Answers

The DNA in a human cell weighs approximately 6. 0 x 10^-12 grams.

First, we need to convert 1 mg to grams:

1 mg = 0.001 g

Next, we need to determine how many cells are needed to obtain 1 gram of DNA:

1 g / 6.0 x 10^-12 g/cell = 1.67 x 10^11 cells

Finally, we can use this value to determine how many cells are needed to obtain 0.001 g (1 mg) of DNA:

(1.67 x 10^11 cells/g) x (0.001 g) = 1.67 x 10^8 cells

Therefore, approximately 1.67 x 10^8 cells are needed to extract 1 mg of DNA.

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In the acute phase of HIV-1 infection, virus-specific cytotoxic
lymphocytes (CTLs) are able respond quickly to produce a marked
decrease in the viral load.
Group of answer choices
True
False

Answers

True. In the acute phase of HIV-1 infection, virus-specific cytotoxic lymphocytes (CTLs) can respond quickly to produce a marked decrease in the viral load.

This is because CTLs are a type of white blood cell that can recognize and kill infected cells. During the acute phase of HIV-1 infection, there is a high level of viral replication and a large number of infected cells. CTLs can recognize these infected cells and quickly mount an immune response, leading to a decrease in the viral load.

Viral load is the term used to refer to the amount of virus in a person's blood. So, HIV viral load is the amount of HIV in the body of someone who has been infected with HIV.

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which term is best described as the production of proteins based on the cell's genetic information?
transcription
Gene synthesis
Gene repression
gene expression

Answers

Transcription is best described as the production of proteins based on the cell's genetic information.

What is transcription?

Transcription is the process of turning a segment of DNA into RNA. DNA segments that have been translated into RNA molecules that can encode proteins are known as messenger RNA (mRNA). When extra DNA segments are translated into RNA molecules, non-coding RNAs are created (ncRNAs). Just 1% to 3% of all RNA samples contain mRNA. Human genome coding vs. non-coding DNA analysis reveals that while at least 80% of mammalian genomic DNA can be actively translated (in one or more types of cells), the majority of this 80% is non-coding RNA (ncRNA), while less than 2% of the mammalian genome can be actively translated into mRNA.

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Answer: Gene expression

1: Long day plants flower
a.in long days
b. when day length exceeds a critical minimum.
c. when day length exceeds a critical maximum.
d. when daylength is greater than 12 hours in a 24 hour period.
e. in the summer
2: Which of the following is NOT true about plant photoreceptors?
a. All plant photoreceptors localize to the nucleus when photoactivated.
b. Some plant photoreceptors move between the cytoplasm and the nucleus depending on their conformational state.
c. Some plant photoreceptors have protein kinase activity.
d. Some plant photoreceptors can respond to a wide range of wavelengths of light.
e. Some plant photoreceptors are membrane-bound photoreceptors.

Answers

1: Long day plants flower B: when day length exceeds a critical minimum.

2: The statement that is not true about plant photoreceptors is A: All plant photoreceptors localize to the nucleus when photoactivated.

1. The correct answer is B: when the day length exceeds a critical minimum. Long-day plants flower when the day length exceeds a certain minimum number of hours, typically around 12 to 14 hours. This means that they are more likely to flower in the summer when the days are longer.

2. The correct answer is A: All plant photoreceptors localize to the nucleus when photoactivated. Not all plant photoreceptors localize to the nucleus when they are photoactivated. Some plant photoreceptors, such as phytochromes, do move to the nucleus when they are photoactivated, but others, such as cryptochromes, do not. Therefore, it is not true that all plant photoreceptors localize to the nucleus when photoactivated.

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9. Aerobic respiration, (which regenerates ATP) is the only route that
requires

Answers

Answer:

Oxygen

Explanation:

Aerobic Respiration is the process in which oxygen is used to make ATP.

As a consequence of the tilt and rotation of the Earth some areas may have large temperature fluctuations throughout the year whereas other areas may have only minor temperature fluctuations throughou

Answers

As a consequence of the tilt and rotation of the Earth, some areas may experience large temperature fluctuations throughout the year, while other areas may only experience minor temperature fluctuations. This is due to the fact that the Earth's axis is tilted at an angle of 23.5 degrees relative to the plane of its orbit around the sun.

This tilt causes different parts of the Earth to receive different amounts of solar radiation at different times of the year, leading to seasonal temperature changes.

In areas near the equator, where the sun's rays are always direct, there is little variation in temperature throughout the year. However, in areas closer to the poles, where the sun's rays are more indirect, there can be significant temperature fluctuations as the seasons change. For example, during the summer months, the Northern Hemisphere is tilted towards the sun, leading to warmer temperatures. However, during the winter months, the Northern Hemisphere is tilted away from the sun, leading to colder temperatures.

In addition to the tilt of the Earth, the rotation of the Earth on its axis also plays a role in temperature fluctuations. The rotation of the Earth causes day and night, with one side of the Earth facing the sun and receiving direct solar radiation, while the other side faces away from the sun and receives less solar radiation. This leads to daily temperature fluctuations, with temperatures generally being warmer during the day and cooler at night.

Overall, the tilt and rotation of the Earth are responsible for the seasonal and daily temperature fluctuations that we experience on our planet.

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Darwin described evolution as "descents with modification." Based on the diagrams shown, how dose the fossil record support this theory?

Answers

The fossil record provides strong evidence that supports Darwin's theory of "descent with modification" by showing how organisms have evolved and changed over time.

How does the fossil evidence back up the evolution theory?

The fossil record offers proof of the evolution of organisms over time. The remains or remnants of extinct creatures that have been preserved in sedimentary rocks are known as fossils. Scientists can learn how various animals have changed over millions of years by looking at the fossil record.

The fossil record supports the theory of "descent with modification" because it shows that organisms have changed over time, and that new species have evolved from older ones. Fossils of ancient organisms often show characteristics that are intermediate between those of their ancestors and their descendants. For example, the fossils of early mammals show characteristics that are intermediate between reptiles and modern mammals.

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Researchers are studying DNA region of interest in an effort to learn more about the gene and its structure. Using multiple restriction enzymes they cut the region of interest into smaller fragments (A-D) that are each ligated into a vector: The vector contains an upstream promoter and downstream detectable marker: The researchers transform each vector into cells and examine the expression: DNA fragment A | B Expression no no high high Determine which DNA region contains the transcription start site (TSS) If it is located across multiple regions, indicate each region. Not all regions will be marked. DNA 8' 5' 5' 5' 5' 8'

Answers

The DNA region that contains the transcription start site (TSS) is DNA fragment B. This is because the expression of the detectable marker is high when DNA fragment B is present in the vector.

This indicates that the TSS is located within DNA fragment B, as the presence of the TSS allows for the expression of the detectable marker. It is important to note that DNA fragment A does not contain the TSS, as there is no expression of the detectable marker when DNA fragment A is present in the vector. This suggests that the TSS is not located within DNA  fragment. A.
Overall, the use of restriction enzymes to cut the DNA region of interest into smaller fragments allows for the identification of the TSS within a specific DNA fragment. In this case, the TSS is located within DNA fragment B.

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Discuss the origins and physiological roles of the
anaphylatoxins? Give two specific examples of these soluble factors
in a complement cascade

Answers

The anaphylatoxins are a group of soluble factors that are generated during the complement cascade, a part of the immune system's response to pathogens. Two specific examples of anaphylatoxins in a complement cascade are: C3a and C5a.

The physiological roles of anaphylatoxins include the recruitment of immune cells to the site of infection or injury, the promotion of inflammation, and the enhancement of phagocytosis (the process by which immune cells engulf and destroy pathogens). Anaphylatoxins also play a role in the regulation of the complement system, helping to prevent excessive or unnecessary activation.
Two specific examples of anaphylatoxins in a complement cascade are:
1. C3a: This anaphylatoxin is produced during the activation of the complement system via the classical, lectin, or alternative pathways. It plays a role in the recruitment of immune cells to the site of infection or injury, and also promotes inflammation.
2. C5a: This anaphylatoxin is produced during the activation of the complement system via the classical or lectin pathways. It is a potent chemoattractant, meaning that it helps to attract immune cells to the site of infection or injury. It also plays a role in the promotion of inflammation and the enhancement of phagocytosis.

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how
does the immune system cause the symptoms thay were observed in
Digeorge Syndrome case elizabeth bennet?

Answers

The symptoms observed in Elizabeth Bennet with Digeorge Syndrome are due to the fact that her immune system is not functioning correctly. Because her thymus gland did not develop properly, her immune system is not able to produce enough T-cells, which are a type of white blood cell that is essential for fighting off infections and other foreign invaders.

This makes her more susceptible to infections, which can cause a range of symptoms such as fever, fatigue, and coughing. In addition to immune system issues, Digeorge Syndrome can also cause problems with the development of the heart, which can lead to heart defects and other cardiovascular problems. This can cause symptoms such as shortness of breath, chest pain, and fainting. Overall, the symptoms observed in Digeorge Syndrome patients are due to a combination of the immune systems and cardiovascular problems.

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Quistnon 7 itiendetarum Pigiens wous fall th tie shorriat When doing differential centrifugation, microsomes pellet to the bottom of the tube at faster spin speeds than lysosomes. This indicates that microsomes are than lysosomes. Larger Smaller Heavier Lighter QUESTION 7 What would likely happen to a cell treated with a compound that causes lysis (breakage) of peroxisomal membranes?
Ca ++
would leak out triggering massive exocytosis. Proteins would fail to be secreted. Proteins in the cytoplasm would be damaged. Nothing, because the low pH of the peroxisome would be buffered by the cell. QUESTION 8 Click Save and Submit to save and submit. Click Save All Answers to save all answers.

Answers

Microsomes are smaller than lysosomes as indicated by the faster spin speeds during differential centrifugation. When a cell is treated with a compound that causes lysis of peroxisomal membranes, proteins in the cytoplasm would be damaged.

Microsomes are small vesicles derived from the endoplasmic reticulum and can perform many metabolic activities, while lysosomes are cell organelles that function in the process of autophagy and the destruction of cellular waste.

When peroxisomal membranes are lysed, causing a rupture of the organelle, the contents of the peroxisomes, including the enzymes that break down hydrogen peroxide, will be released into the cytoplasm. The release of these enzymes could cause damage to the cytoplasmic proteins, making them non-functional, but it is not the most likely outcome. The most likely outcome of the release of these enzymes is that the Ca++ would leak out of the cell, triggering massive exocytosis.

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Acell is exposed to a substance that prevents it from dividing: The cell becomes larger and larger: This situation should present no problem to the cell because the surface area of the cell will increase as the volume of the cell increases: will eventually be problematic as the cells surface area to volume ratio will increase as the cell gets larger. should be beneficial since the cell will be able to divert the ATP cell division to other normally used for processes; will eventually be problematic since the cell's surface area will increase at a rate that is slower than the increase in volume:

Answers

The cell becoming larger and larger due to a substance that prevents it from dividing should not initially be problematic because the surface area of the cell will increase at the same rate as the volume of the cell increases.

This means that the cell's surface area to volume ratio will remain relatively the same. This could be beneficial since the cell will be able to divert the ATP usually used for cell division to other processes. However, if the cell continues to grow, it will eventually become problematic since the cell's surface area will increase at a rate that is slower than the increase in volume.

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The stock PCR buffer provides the conditions necessary for the Taq polymerase to work. This particular one contains:
- 12.2 mM Tris HCl (pH 8.3)
- 61 mM KCl
- 1.83 mM MgCl2
- 0.0012% (w/v) gelatin
- 244 μM dNTPs
Solution, Volume (µL), Order
PCR buffer, containing MgCl2 and dNTPs, 41, 1st
Isolated DNA solution, 5, 2nd
5 µM D1S80 primers; including both the forward and reverse primers, 3, 3rd
Total volume, 49,
Q: Write a method or legend describing the PCR setup using lab-independent concentrations Remember, this means final concentrations! Someone should be able to reproduce your work without necessarily using all the same stock solutions and equipment.
Q: How would you make 10 mL of the stock PCR buffer (described above) from the following stock solutions?
a. 1 M Tris HCl pH 8.3
b. 2 M KCl
c. 183 mM MgCl2
d. 0.12 %(w/v) Gelatin
e. 100 mM for each of the dNTPs; dATP, dGTP, dCTP and dTTP

Answers

Method/Legend for PCR setup using lab-independent concentrations:

1. Prepare a PCR reaction mix containing final concentrations of the following components:

0.25 mM of each dNTP (dATP, dGTP, dCTP, dTTP)2.5 mM MgCl225 mM Tris-HCl (pH 8.3)125 mM KCl0.01% (w/v) gelatin0.5 μM of each primerTemplate DNA (concentration and volume as desired)

2. Mix the reaction components thoroughly and aliquot into PCR tubes.

3. Add Taq polymerase to each reaction tube as per the manufacturer's instructions.

4. Perform PCR amplification using appropriate cycling conditions.

Making 10 mL of the stock PCR buffer:

To make 10 mL of the stock PCR buffer, the following steps can be followed:

a. Tris HCl (pH 8.3) required = 12.2 mM x 10 mL = 0.122 mmol = 0.0122 g

Weigh out 0.0122 g of Tris HCl and dissolve it in 10 mL of distilled water.

b. KCl required = 61 mM x 10 mL = 0.61 mmol = 0.122 g

Weigh out 0.122 g of KCl and dissolve it in 10 mL of distilled water.

c. MgCl2 required = 1.83 mM x 10 mL = 0.0183 mmol = 0.00334 g

Weigh out 0.00334 g of MgCl2 and dissolve it in 10 mL of distilled water.

d. Gelatin required = 0.0012% (w/v) x 10 mL = 0.0012 g

Weigh out 0.0012 g of gelatin and dissolve it in 10 mL of distilled water by heating the solution and stirring gently.

e. dNTPs required = 244 μM x 10 mL = 2.44 μmol each

For each of the dNTPs (dATP, dGTP, dCTP, dTTP), weigh out 0.246 mg (2.44 μmol) and dissolve it in 10 mL of distilled water.

Mix all the above solutions together to obtain 10 mL of the stock PCR buffer. Adjust the pH of the buffer, if necessary, to 8.3 using HCl or NaOH. Store the buffer at -20°C for long-term storage, or at 4°C for short-term use.

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Discuss in no less than 800 words:
The threats to Avian Diversity (Specific to the Guiana Shield
and Guyana if you can find them)

Answers

The threats to Avian Diversity (Specific to the Guiana Shield and Guyana if you can find them) is facing multiple threats due to both natural and anthropogenic causes. The main threats include habitat destruction, overexploitation, pollution, and disease.

Habitat destruction is a major threat to avian diversity in the Guiana Shield and Guyana. The main cause of this threat is the conversion of native forest to agricultural land and urbanization. Deforestation has had a major impact on bird species that rely on forest habitats, such as the Harpy Eagle and the White-tailed Hawk. Another threat to avian diversity in the Guiana Shield and Guyana is overexploitation. Overhunting of bird species for their feathers, eggs, and meat has led to population declines in some species, such as the Scarlet Ibis and the Black-crowned Night Heron.

Pollution from oil and other industrial waste has caused a decrease in avian diversity in the Guiana Shield and Guyana. Oil spills and other forms of pollution have had a devastating effect on seabird populations, as well as other aquatic species.  Avian diversity in the Guiana Shield and Guyana is also threatened by disease. Avian malaria and other diseases have caused a decrease in population sizes of certain species, such as the Great Egret.

Overall, avian diversity in the Guiana Shield and Guyana is facing multiple threats due to both natural and anthropogenic causes. It is important to protect the avian diversity of this region by reducing habitat destruction, overexploitation, pollution, and disease.

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The challenge with using cytosolic NADH for mitochondrial ATP synthesis is that this coenzyme does not easily pass the inner mitochondrial membrane. It therefore must transfer its electrons to another

Answers

NADH is an important coenzyme found in the cytosol that plays a key role in metabolic processes such as glycolysis and the tricarboxylic acid cycle. It provides electrons for the electron transport chain and is an important source of energy for the cell.

However, it is unable to cross the inner mitochondrial membrane, making it difficult to use as a source of energy for ATP synthesis in the mitochondria.

To overcome this, NADH must transfer its electrons to another coenzyme, such as flavin adenine dinucleotide (FAD), which can cross the inner mitochondrial membrane. Once FAD is in the mitochondrial matrix, it can transfer its electrons to the electron transport chain, allowing NADH to be used as a source of energy for ATP synthesis. This process is referred to as shuttling and is essential for the efficient transfer of energy from the cytosol to the mitochondria.

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2. What forms the various features of the ocean's floor, such as trenches?

Answers

Answer: The ocean floor, the tectonic plates of the world alter it.

Explanation: hope it helped.

Consider the material or object to be sterilized and the three possible physical treatments. Select the method or methods that would be suitable for the material or object.
Bacteriological media:
Table top in a laboratory:
Toxoid preparation for immunization

Answers

Methods that would be suitable for the material or object:

Bacteriological media: Moist heatTable top in a laboratory: dry heatToxoid preparation for immunization: radiation

About physical treatment

There are three possible physical treatments that can be used to sterilize materials or objects: dry heat, moist heat, and radiation.

For bacteriological media, moist heat would be the most suitable method as it can effectively kill all microorganisms and spores without damaging the media. This can be achieved through autoclaving, which uses steam under pressure to sterilize materials.

For a table top in a laboratory, dry heat would be the most suitable method as it can effectively sterilize surfaces without causing any damage. This can be achieved through the use of a hot air oven or flaming with a Bunsen burner.

For a toxoid preparation for immunization, radiation would be the most suitable method as it can effectively sterilize the preparation without causing any damage or altering its effectiveness. This can be achieved through the use of gamma or electron beam radiation.

In conclusion, the most suitable method for sterilizing a material or object depends on the nature of the material or object itself. Moist heat is suitable for bacteriological media, dry heat is suitable for table tops in a laboratory, and radiation is suitable for toxoid preparations for immunization.

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Being prepared for severe weather can make a person feel safer and less fearful.

Select how the author supports this perspective in the text "Wild Weather."

The author explains how they feel about people who are not prepared for bad storms.
The author gives information on ways to prepare for different types of severe weather.
The author shares stories about different people who survived hurricanes and tornadoes.
The author tries to persuade their reader to move to places where wildfires don't occur.

Answers

Answer:B

Explanation:

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Aspergillus niger produces several proteases under batch reactions. Each of the proteases compliment different reaction pathways. For protease A at a given substrate concentration of 3 x 10^5 M and Km of 10^-3 M, it is noticed that after two minutes 5% of the substrate was converted. Estimate the substrate conversion at 10, 20, 30 and 60 minutes? Assume Michaelis- Menten kineties govern the reaction rate.

Answers

The substrate conversion at 10, 20, 30, and 60 minutes are 0.5 M, 1 M, 1.5 M, and 3 M, respectively.

The substrate conversion at different time intervals can be calculated using the Michaelis-Menten equation:V = (Vmax*[S])/(Km + [S])

where

V is the reaction rate Vmax is the maximum reaction rate[S] is the substrate concentrationKm is the Michaelis constant.

We are given

[S] = 3 x 10⁵ M and Km = 10⁻³ M.

We can also calculate Vmax from the given information:

Vmax = (V*Km + V*[S])/[S] = (0.05*10⁻³ + 0.05*3 x 10⁵)/(3 x 10⁵) = 0.05 M/min

Now we can plug in the values for Vmax, [S], and Km into the Michaelis-Menten equation to calculate the substrate conversion at different time intervals:

At 10 minutes:

V = (0.05*3 x 10⁵)/(10⁻³+ 3 x 10⁵) = 0.05 M/min

Substrate conversion = V*10 = 0.5 MAt 20 minutes:

V = (0.05*3 x 10⁵)/(10⁻³ + 3 x 10⁵) = 0.05 M/min

Substrate conversion = V*20 = 1 MAt 30 minutes:

V = (0.05*3 x 10⁵)/(10³ + 3 x 10⁵) = 0.05 M/min

Substrate conversion = V*30 = 1.5 MAt 60 minutes:

V = (0.05*3 x 10⁵)/(10⁻³ + 3 x 10⁵) = 0.05 M/min

Substrate conversion = V*60 = 3 M

Therefore, the substrate conversion at 10, 20, 30, and 60 minutes are 0.5 M, 1 M, 1.5 M, and 3 M, respectively.

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Your Aunt Mildred, the worldclass distance runner, completed the Leadville Trail 100 mile ultramarathon, finishing first in the 85+ age group.
3. Aunt Mildred would routinely listen to the Bieber during her long training runs on her iPod. Explain how sound waves are transmitted from Aunt Mildred’s ears to her brain, ultimately resulting in perception of "Baby, Baby, Baby, oh".

Answers

Sound waves are transmitted from Aunt Mildred's ears to her brain through a series of steps.

First, the sound waves enter the ear through the ear canal and hit the eardrum, causing it to vibrate. These vibrations are then transferred to the ossicles, which are three small bones in the middle ear called the malleus, incus, and stapes.

The ossicles amplify the sound and transfer it to the cochlea, a fluid-filled structure in the inner ear.

Within the cochlea are tiny hair cells that move in response to the vibrations, triggering electrical signals that are sent to the brain via the auditory nerve.

The brain then interprets these signals as sound, allowing Aunt Mildred to perceive the music she is listening to.

In summary, sound waves are transmitted from Aunt Mildred's ears to her brain through the following steps:
1. Sound waves enter the ear canal and hit the eardrum, causing it to vibrate.
2. The vibrations are transferred to the ossicles, which amplify the sound.
3. The amplified sound is transferred to the cochlea, where it triggers electrical signals.
4. The electrical signals are sent to the brain via the auditory nerve, resulting in the perception of sound.

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Ten thousand bacteria multiply into 1,000,000 bacteria in 6.67hours. What is the generation time? A. 1 doubling per hour. B.0.5 doublings per hour. C. 60 minutes. D. 30 minutes. E. 2 hours

Answers

Option b) is the correct answer. The generation time for 10,000 bacteria to multiply into 1,000,000 bacteria in 6.67 hours is 0.5 doublings per hour.

To calculate the generation time, we need to divide the total time, 6.67 hours, by the total number of doublings, which is 10 (1,000,000/10,000 = 10 doublings). This gives us a generation time of 0.667 hours, which can be converted to 0.5 hours or 30 minutes.

So, the answer is B: 0.5 doublings per hour, or 30 minutes. To break down the process in more detail, 10,000 bacteria are the starting point, and they double 10 times in 6.67 hours to reach 1,000,000 bacteria. This means that each doubling takes 0.667 hours, or 40 minutes.

If we divide this by 2, we get 0.5 doublings per hour, or 30 minutes for each doubling. So, in 6.67 hours, the 10,000 bacteria will double 10 times, giving us a generation time of 0.5 doublings per hour, or 30 minutes.

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Please help :)
Biology 9 HS

Answers

1. DNA helicase unwinds DNA
2. Replication fork is formed
3. DNA polymerase attaches to the primer
4. DNA polymerase adds nucleotides in the 5’ to 3’ direction

5. Okazaki fragments are bound together by ligase

Describe the concepts of genetic drift and gene flow. (Do not
use definitions in your answer.)

Answers

Genetic drift and gene flow are two important concepts in the field of genetics and evolutionary biology.

Genetic drift is the random fluctuation of allele frequencies within a population. This can occur due to chance events, such as the death of individuals carrying a particular allele, or the migration of individuals into or out of a population. Genetic drift can lead to the loss of genetic variation within a population, and can also result in the fixation of certain alleles, meaning that they become the only version of a gene present in a population.

Gene flow, on the other hand, is the movement of alleles between populations. This can occur through the migration of individuals, or through the exchange of genetic material between populations. Gene flow can introduce new genetic variation into a population, and can also prevent the divergence of populations into separate species.

Both genetic drift and gene flow are important factors in the evolution of populations, and can have significant effects on the genetic makeup of a population over time. Understanding these concepts is important for understanding the process of evolution and the diversity of life on Earth.

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What is the critical role of the border cells during Drosophila
oogenesis and fertilization?

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The critical role of the border cells during Drosophila oogenesis and fertilization is to guide the oocyte to the sperm and to facilitate fertilization.

During Drosophila oogenesis, border cells are a group of specialized follicle cells that detach from the anterior follicular epithelium and migrate between the nurse cells to the oocyte. The border cells play a crucial role in guiding the oocyte to the sperm during fertilization.

In addition, border cells also produce signals that attract the sperm to the oocyte and facilitate fertilization. These signals include the production of a small peptide called Ovulin, which is released by the border cells and acts as a chemoattractant for the sperm.

Overall, the border cells play a critical role in Drosophila oogenesis and fertilization by guiding the oocyte to the sperm and facilitating fertilization through the production of signaling molecules.

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What parts of the sequence were particularly hard to place? Why? How is an electrical signal converted to a chemical signal at 3 nerve terminal? Hew do transmitter-gated ion channels convert the chemical neurotransmitter back into an electrical signal carried by 3 signal?

Answers

The parts of the sequence were particularly hard to place is the conversion of the electrical signal to a chemical signal because they involve complex interactions.

An electrical signal converted to a chemical signal at 3 nerve terminal through the release of neurotransmitters

Transmitter-gated ion channels convert the chemical neurotransmitter back into an electrical signal carried by 3 signal by neurotransmitter binding to gate-emitting ion channels

The parts of the sequence that were particularly hard to place were the conversion of the electrical signal to a chemical signal at the nerve terminal and the conversion of the chemical neurotransmitter back into an electrical signal carried by the ion channels. These processes can be difficult to understand because they involve complex interactions between different molecules and ions.

At the nerve terminal, the electrical signal is converted to a chemical signal through the release of neurotransmitters. This occurs when voltage-gated calcium channels in the nerve terminal open in response to the electrical signal, allowing calcium ions to enter the cell. The influx of calcium triggers the release of neurotransmitters from synaptic vesicles into the synaptic cleft.

The neurotransmitters then bind to transmitter-gated ion channels on the postsynaptic cell, causing the channels to open and allowing ions to flow into the cell. This influx of ions creates an electrical signal that is carried by the ion channels. The neurotransmitters are then removed from the synaptic cleft through reuptake or enzymatic breakdown, allowing the ion channels to close and ending the electrical signal.

Overall, the conversion of electrical signals to chemical signals and back again is a complex process that involves the interaction of multiple molecules and ions. Understanding these processes is important for understanding how the nervous system functions and how information is transmitted between cells.

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Def: Chemical reaction by which the cells convert energy from one form to another and build and break down molecules

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A chemical reaction that occurs in cells to convert energy from one form to another and to build and break down molecules is called metabolism.

Metabolism is the process by which cells convert nutrients into energy and use that energy to perform various cellular functions, such as building and breaking down molecules. There are two types of metabolism: catabolism, which breaks down molecules to release energy, and anabolism, which uses energy to build molecules. Both types of metabolism are necessary for cells to function properly and maintain homeostasis.

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