Bacteria evade antibiotics with silent mutations to survive

Abstract

Bacteria may develop antibiotic resistance due to unintentional DNA alterations that give them a survival advantage. Bacteria may develop antibiotic resistance due to unintentional DNA alterations that give them a survival advantage. Finding genetic changes and understanding how they enable bacteria to withstand antibiotic attacks will be crucial to our ability to develop new medications to combat them.

Keywords

Antibiotics antibiotic resistance mutation drug-resistant microorganisms

1 Introduction

A world without antibiotics is one of the greatest challenges to humanity in this century. A revolution in human medicine was sparked by Alexander Fleming’s discovery of penicillin in 1928 [1]. Fleming cautioned during his acceptance speech for the Nobel Prize in 1945 that germs can easily become penicillin resistance developed as a result of insufficient dosages of this medication. The known causes of the spread of antibiotic resistance include the misuse of antibiotics in veterinary, human, and agricultural medicine, the use of antibiotics as growth promoters, the existence of unlicensed and illegal markets for antibiotics, and the administration of antibiotics without first having a test for antibiotic resistance. Bacteria are constantly evolving to become resistant to antibiotics [2]. One way they do this is by acquiring mutations that make them “silent” to the drugs. In other words, the mutations don’t change the bacteria’s appearance or behavior, but they do make the bacteria resistant to antibiotics. This is a serious problem because it means that existing antibiotics may become less effective over time. And it’s not just a theoretical problem; we’re already seeing it happen in the real world. For example, methicillin-resistant Staphylococcus aureus (MRSA) is a kind of bacteria that resists various antibiotics. MRSA is a serious concern because it can cause infections that are difficult to treat. And as more and more bacteria become resistant to antibiotics, it becomes more difficult to find drugs that can effectively treat infections [3]. The best way to combat antibiotic resistance is to prevent it from happening in the first place. That means using antibiotics only when they are necessary, and not overusing them. It also means developing new antibiotics to keep ahead of the bacteria’s evolutions. But even if we do all of that, antibiotic resistance will still be a problem. So we need to be prepared for a world in which some infections are much harder to treat than they are today [4].

Antibiotics have two opposing effects: they can kill bacteria that cause diseases that are fatal, or they can prevent death. But overuse of these drugs leads to the rapid spread of antibiotic resistance, which is now considered one of the biggest global threats to human health [5]. Antibiotic resistance occurs when bacteria adapt so they no longer respond to an antibiotic that is designed to target them. These microbes evolve in response to pressures such as exposure to antibiotics and other stressors, leading to small changes in their DNA that make them resistant to drug pressure. These silent mutations can be found in any gene, including those encoding for proteins directly targeted by the antibiotic [6].

Bacterial genetics plays a role in the process behind the spread of antibiotic resistance. Antibiotic resistance genes are frequently found on mobile genetic components that are passed between two cells [7]. The exchange method known as horizontal gene transfer (HGT), which can take place between two different species, is dangerous. Microorganisms have a very rapid rate of generation compared to either animals or plants. It implies that after HGT took place, a population of resistant cells rather than simply one would exist within a short period after the event [8].

2 Silent mutations: What are they?

Silent mutations are modifications to the DNA sequence that do not affect the protein’s amino acid sequence. These mutations are “silent” because they don’t change the function of the protein. The majority of silent mutations take place in introns and intergenic regions of DNA, which do not impact the encoded protein. The coding sections of the DNA (exons), where certain silent mutations might arise and alter the protein’s function [9]. Silent mutations can be neutral (neither good nor bad for the function of the protein) or they can be deleterious (bad for the function of the protein). Neutral silent mutations occur more frequently than deleterious silent mutations because they are less likely to change the function of the protein. Deleterious silent mutations can cause disease by changing the function of the protein [10]. For example, a silent mutation in the BRCA1 gene has been linked to an increased risk of breast cancer. While silent mutations may not directly affect the protein’s function, they can still have an indirect effect by altering the structure of the protein. This can alter the function of the protein or make it more susceptible to disease [11].

3 What is the difference between a silent mutation and a point mutation?

There are two main types of mutations: silent mutations and point mutations. Silent mutations have no impact on the protein that is produced, while point mutations can result in a change in the amino acid sequence of the protein. Point mutations usually have a bigger impact on the function of the protein than silent mutations. However, both types of mutations can potentially cause problems. Silent mutations may accumulate over time and eventually have an impact on the protein’s function. Point mutations can cause a protein to function improperly or not at all [12].

Mutations are important to consider when studying genes and proteins. They can help to explain why certain diseases occur and how they are passed down in families. Mutations can also be used to create new proteins with desired characteristics [13].

4 What are the ways that bacteria acquire silent mutations?

There are several ways that bacteria can acquire silent mutations. Silent mutations are changes to the DNA that don’t result in any changes to the proteins that are produced. Even though these changes don’t alter the proteins, they can still be important. Silent mutations can affect things like how well the protein works, how stable it is, and how likely it is to be affected by other mutations [14].

One way that bacteria can acquire silent mutations is through something called horizontal gene transfer. This is when DNA is transferred from one bacterium to another. This can happen through things like plasmids, which are small pieces of DNA that can be transferred between cells. Horizontal gene transfer is one of the main ways that bacteria can share information and acquire new mutations [15].

Another way that bacteria can acquire silent mutations is through mistakes that occur when the DNA is copied. These mistakes, called point mutations, can change a single nucleotide in the DNA. Most of the time, these changes don’t result in any changes to the proteins. However, sometimes, these changes can affect how well the protein works [16].

Even though silent mutations don’t usually have any visible effects, they can still be important. These mutations can accumulate over time and eventually lead to changes in the proteins that are produced. These changes can eventually have a big impact on the bacterium, and may even help it to adapt to new environments [17].

Silent mutations can occur through several mechanisms, including:

Spontaneous mutations: These are mutations that occur randomly, with no apparent environmental trigger [18].

Back-mutation: This is when a previously mutated gene reverts to its original sequence [19].

Gene conversion: This is when one sequence is converted into another through a mistake during replication [20].

Frameshift mutations: These are insertions or deletions of DNA that alter the reading frame of the gene [21].

Point mutations: These are single base pair changes that can alter the function of a gene.

While silent mutations may not have a visible effect on the phenotype of an organism, they can still be important. Silent mutations can accumulate over time and eventually lead to a change in the protein sequence. This can have a significant impact on the function of the protein and the overall fitness of the organism [22].

5 Bacteria evade antibiotics with silent mutations

Bacteria are evolving to evade antibiotics faster than we can create new ones, making infections increasingly difficult to treat. This is a major public health concern, as antibiotic-resistant bacteria are more likely to cause life-threatening infections [23].

Bacteria are constantly evolving and evolving ways to evade antibiotics. One of the ways they do this is by developing silent mutations. Silent mutations are mutations that don’t change the bacteria’s phenotype, or how the bacteria look and function. These mutations don’t make the bacteria resistant to antibiotics, but they do make it harder for antibiotics to kill them. The bacteria can pass these mutations on to their offspring, and over time, the population can become more and more resistant to antibiotics [24].

There are a few ways to prevent bacteria from developing resistance to antibiotics. One is to use a combination of different antibiotics so that if one antibiotic fails, the others can still kill the bacteria [25]. Another is to use antibiotics wisely, only prescribing them when they’re needed and not using them unnecessarily.

We need to be aware of the ways that bacteria are evolving and evolving ways to evade antibiotics. We also need to be careful about how we use antibiotics so that we don’t inadvertently contribute to the development of antibiotic resistance [26].

6 How do bacteria evade antibiotics through silent mutations?

The researchers discovered that bacteria can use silent mutations to evade beta-lactams by mutating specific DNA sequences, known as recognition sequences, in their genome [27]. These sequences are the target of specific antibiotics, which bind and interfere with the DNA sequences to prevent bacterial growth. Bacteria can evade these antibiotics by mutating their recognition sequences to avoid binding by beta-lactam [28]. The researchers found that bacteria can use silent mutations to evade beta-lactams by mutating their recognition sequences [29]. Specifically, bacteria can change GATC sequences into GATCT sequences. This seemingly minor DNA change allows bacteria to chemically modify the beta-lactam, which prevents the antibiotic from binding to the cell wall and killing the bacteria [30].

7 Limitations of the study and future directions

The results of this study shed important light on how bacteria evade antibiotics through silent mutations. However, they only focus on one resistance pathway against one type of antibiotic [31]. There are many other ways bacteria can evade antibiotics, so future studies should examine these methods as well. In addition, future studies could also explore how bacteria might evade antibiotics through silent mutations when the bacteria have been exposed to multiple antibiotics. This could be an important factor in the spread of antibiotic resistance because many individuals infected with bacteria are treated with multiple antibiotics. Finally, future studies should explore the impact of this resistance pathway on the efficacy of antibiotics and bacterial virulence in vivo. Bacterial virulence is the degree to which a bacteria is harmful to its host.

8 Conclusion

The results of this study highlight the importance of detecting and understanding silent mutations in bacterial DNA. Silent mutations are believed to be uncommon, but they are especially dangerous because they can lead to antibiotic resistance without changing the amino acid sequence of proteins targeted by antibiotics. This makes silent mutations difficult to detect using standard laboratory methods. The findings of this study suggest that bacteria can evade antibiotics through silent mutations that change specific DNA sequences targeted by antibiotics. To prevent the spread of antibiotic resistance, it is therefore important to carefully select antibiotics that target specific bacterial DNA sequences.

Conflict of interest

The authors have no conflict of interest to report.

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