Instigator / Pro
Somebody's avatar
0
Somebody
1438
rating
6
debates
0.0%
won
Topic
#551

Viruses don't exist

Status
Finished

The debate is finished. The distribution of the voting points and the winner are presented below.

Winner & statistics
Better arguments
0
6
Better sources
0
4
Better legibility
0
2
Better conduct
0
2

After 2 votes and with 14 points ahead, the winner is...

RationalMadman
Tags
Science
Parameters
Publication date
Last updated date
Type
Standard
Number of rounds
5
Time for argument
Three days
Max argument characters
30,000
Voting period
Two weeks
Point system
Multiple criterions
Voting system
Open
Contender / Con
RationalMadman's avatar
14
RationalMadman
1706
rating
562
debates
68.06%
won
Description

To prove that viruses don't exist. Answer these logic questions -

1. How did the first person to see a virus know that it was a virus without any references as to what a virus looks like?

2. How do viruses find their host if they have no legs, arms, eyes, ears, brains, sense of touch or means of locomotion?

3. How can something that is dead, suddenly come to life?

4. How can viruses survive in the atmosphere and sunlight without any walls for protection? (very fragile)

5. How does a entity (virus) that kills its host pass on its genes and what does it gain by killing the host?

6. If viruses are proteins, then why don't small insects like ants find them and eat them all?

Round 1
Somebody's avatar
Somebody
Pro
#1
To prove that viruses don't exist. Answer these logic questions -
1. How did the first person to see a virus know that it was a virus without any references as to what a virus looks like?
2. How do viruses find their host if they have no legs, arms, eyes, ears, brains, sense of touch or means of locomotion?
3. How can something that is dead, suddenly come to life?
4. How can viruses survive in the atmosphere and sunlight without any walls for protection? (very fragile)
5. How does a entity (virus) that kills its host pass on its genes and what does it gain by killing the host?
6. If viruses are proteins, then why don't small insects like ants find them and eat them all?

RationalMadman's avatar
RationalMadman
Con
#2
I think the entire case of Pro relies, erroneously on the notion that viruses haven't been actually seen, studied and observed in and of themselves. It's true that the discovery involved no sighting of a virus but it's a complete mistruth to say they haven't since been indisputably observed.

In the Dermatovenereology department, skin infections by bacteria, viruses, and fungi are very common in routine clinical practice. Discrimination and identification of these pathogens is a huge challenge and very important for patient’s disease diagnosis and treatment. Transmission electron microscopy (TEM) is a very strong tool for detection and observation of the pathogen from the clinical samples that help us obtain the direct proof of presence of the pathogen inside the skin samples of the lesion. Based on the detailed morphologic image, we can recognize the ultrastructures of the pathogen and understand the pathogenesis of the infectious skin diseases. During recent years, we collected several pathogenic microorganisms’ photographs which were taken by TEM; these pathogens included viruses (Herpes simplex virus, Varicella-zoster virus, Molluscum contagiosum virus), bacteria (Mycobacterium leprae), and fungi (Trichophyton violaceum, T. tonsurans, T. mentagrophytes, Trichosporon inkin, Penicillium marneffei). The diagnosis and clinical manifestation, the source of sample, and the image of the pathogen are summarized in Table 1.
- [4]

All samples for TEM were taken from clinical patients. These samples include blister wall, papule, infected hair, scales, and biopsy tissue. The samples were double-fixed in 2% glutaraldehyde and 2% osmium tetroxide for 3h at the room temperature, dehydrated in series of grade ethanol solutions and propylene oxide, then embedded in resin. Ultrathin longitudinal sections of infected hair were cut with an ultramicrotome and a diamond knife. Observation was carried out by TEM (Hitachi H-7650 microscope), which was operated at 120 kV and equipped with a LaB6 source.
- [4]

Go to the link if you don't believe what they found. The results show non-stop observation of viruses and this is an extremely reliable investigation that supports all other investigations into viruses and their results but does so in a visual 'yep, we see what's happening now' way.

I will show a couple of visual findings just so you can't say I didn't show one or two.

Molluscum Contagiosum

Herpes Simplex

Now, since it's clarified that viruses have actually been observed, what's the real case that Pro is making? They have been observed, they have been explained via cycles of infection, replication and/or mutation. They run on RNA, are you saying that RNA is a conspiracy-invented thing that has no real existence? 

What's the point Pro is making?

Sources Continued:
[4] WARNING, ONE PART SHOWS AN INFECTED FEMALE'S GENITALIA BUT IT'S NECESSARY FOR THE SCIENCE Yuping Ran, Wengying Hu, Kaiwen Zhuang, Mao Lu, Jinghong Huang, Fengni Xu, Xiaoxi Xu, Xia Hua, Jebina Lama, Xin Ran, Yalin Dai and Song Lei (September 2nd 2015). Observation of Viruses, Bacteria, and Fungi in Clinical Skin Samples under Transmission Electron Microscopy, The Transmission Electron Microscope - Theory and Applications, Khan Maaz, IntechOpen, DOI: 10.5772/60957. Available from: https://www.intechopen.com/books/the-transmission-electron-microscope-theory-and-applications/observation-of-viruses-bacteria-and-fungi-in-clinical-skin-samples-under-transmission-electron-micro

Round 2
Somebody's avatar
Somebody
Pro
#3
Forfeited
RationalMadman's avatar
RationalMadman
Con
#4
Based on meta-knowledge of Pro's style, Con opts to give Pro less to rebuke.

Con leaves as is and notes that "sources continued" was a clerical error that occured to doing two debates if the same title at once.

Round 3
Somebody's avatar
Somebody
Pro
#5
Forfeited
RationalMadman's avatar
RationalMadman
Con
#6
How did the first person to see a virus know that it was a virus without any references as to what a virus looks like?
The Discovery of the Virus was done by Process of Elimination, not Direct Observation.

Two scientists D. Ivanovski and M. Beijerinck, used process of elimination to discover the first virus(es). Bacterium are a type of living organism (amongst the single celled organisms and such) known as 'contagium fixium' (in their native tongue) and in English this translates to 'infectious being fixed in place'  but they discovered a new kind of infectious being; 'contagium vivum fluidum' which, in English, is an infectious soluble agent.[1] This agent, be it for instance Agar Gel, renders the bacteria still and thus immovable as they can't migrate through it as the density is too high. The density, however, was not too high for the pathogens that Ivanovski and Beijerinck tested, this led to them naming this new type a Tobacco mosaic virus (the 'virus' being the key part of it).[1]

How do viruses find their host if they have no legs, arms, eyes, ears, brains, sense of touch or means of locomotion?
Pro is conceding that they can exist, and is merely asking me to clarify some specifics here.

Question 1: What makes viruses end up infecting one type of host-cell per type of virus?
Question 2: How do they do that and even move if they have no limbs or nerve-based senses?

Before I answer both, it is important to know the steps involved in the virus-infecting process in order to 'map-out' the events in your brain.

The Lyctic cycle is the way to answer the Question 1.[2]


During the lytic cycle of virulent phage, the bacteriophage takes over the cell, reproduces new phages, and destroys the cell. T-even phage is a good example of a well-characterized class of virulent phages. There are five stages in the bacteriophage lytic cycle (see Figure 1). Attachment is the first stage in the infection process in which the phage interacts with specific bacterial surface receptors (e.g., lipopolysaccharides and OmpC protein on host surfaces). Most phages have a narrow host range and may infect one species of bacteria or one strain within a species. This unique recognition can be exploited for targeted treatment of bacterial infection by phage therapy or for phage typing to identify unique bacterial subspecies or strains. The second stage of infection is entry or penetration. This occurs through contraction of the tail sheath, which acts like a hypodermic needle to inject the viral genome through the cell wall and membrane. The phage head and remaining components remain outside the bacteria.

Step 1 is attachment when the phage attaches to the surface of the host. The bacteriophage is shown sitting on the surface of the bacterial host cell.
Step 2 is penetration when the viral DNA enters the host cell. The image shows DNA from within the virus being injected into the host DNA.
Step 3 is biosynthesis when the phage DNA replicates and the phage proteins are made.
Step 4 is maturation when the new phage particles are assembled. This shows the viral components being put together in the cell.
Step 5 is lysis when the cell lyses and the newly made phages are released. This shows the cell bursting and built viruses being released. A virulent phage shows only the lytic cycle pictured here. In the lytic cycle, the phage replicates and lyses the host cell.

The third stage of infection is biosynthesis of new viral components. After entering the host cell, the virus synthesizes virus-encoded endonucleases to degrade the bacterial chromosome. It then hijacks the host cell to replicate, transcribe, and translate the necessary viral components (capsomeres, sheath, base plates, tail fibers, and viral enzymes) for the assembly of new viruses. Polymerase genes are usually expressed early in the cycle, while capsid and tail proteins are expressed later. During the maturation phase, new virions are created. To liberate free phages, the bacterial cell wall is disrupted by phage proteins such as holin or lysozyme. The final stage is release. Mature viruses burst out of the host cell in a process called lysis and the progeny viruses are liberated into the environment to infect new cells.
- [2]

In a lysogenic cycle, the phage genome also enters the cell through attachment and penetration. A prime example of a phage with this type of life cycle is the lambda phage. During the lysogenic cycle, instead of killing the host, the phage genome integrates into the bacterial chromosome and becomes part of the host. The integrated phage genome is called a prophage. A bacterial host with a prophage is called a lysogen. The process in which a bacterium is infected by a temperate phage is called lysogeny. It is typical of temperate phages to be latent or inactive within the cell. As the bacterium replicates its chromosome, it also replicates the phage’s DNA and passes it on to new daughter cells during reproduction. The presence of the phage may alter the phenotype of the bacterium, since it can bring in extra genes (e.g., toxin genes that can increase bacterial virulence). This change in the host phenotype is called lysogenic conversion or phage conversion. Some bacteria, such as Vibrio cholerae and Clostridium botulinum, are less virulent in the absence of the prophage. The phages infecting these bacteria carry the toxin genes in their genome and enhance the virulence of the host when the toxin genes are expressed. In the case of V. cholera, phage encoded toxin can cause severe diarrhea; in C. botulinum, the toxin can cause paralysis. During lysogeny, the prophage will persist in the host chromosome until induction, which results in the excision of the viral genome from the host chromosome. After induction has occurred the temperate phage can proceed through a lytic cycle and then undergo lysogeny in a newly infected cell.
- [2]

To answer question 2, we need to understand something; viruses can stay still for a while before dying but they don't 'move' all that much without some kind of fluid. They do not, however, totally lack limbs. This is an assumption Pro erroneously made. They are a bit robot-like in how their limbs look:

Bacteriophage Virus appearance

See the 'legs'?

Overall, viruses are NOT land 'animals' so to speak. They are much more fish-like in their operations. They move via fluid carrying them around and explore the cells, hoping to find one matching their Capsid-protein configuration.

The sequence of events that occurs when you come down with the flu or a cold is a good demonstration of how a virus works:

An infected person sneezes near you.
You inhale the virus particle, and it attaches to cells lining the sinuses in your nose.
The virus attacks the cells lining the sinuses and rapidly reproduces new viruses.
The host cells break, and new viruses spread into your bloodstream and also into your lungs. Because you have lost cells lining your sinuses, fluid can flow into your nasal passages and give you a runny nose.
Viruses in the fluid that drips down your throat attack the cells lining your throat and give you a sore throat.
Viruses in your bloodstream can attack muscle cells and cause you to have muscle aches.
- [3]

3. How can something that is dead, suddenly come to life?
4. How can viruses survive in the atmosphere and sunlight without any walls for protection? (very fragile)
5. How does a entity (virus) that kills its host pass on its genes and what does it gain by killing the host?
6. If viruses are proteins, then why don't small insects like ants find them and eat them all?
'They just do/don't' is literally the overall answer-mechanism to these. Please expand on why we should have speculation here and why that would lead us to conclude they don't exist (rather than that they exist and that we have yet to work these out). I will counter these either by explaining the answer or explaining why we don't know yet.

Now, for some more proof of the 2 viruses I provided proof of in Round 1.

Molluscum Contagiosum (click figure # to get images of the virus at varying zooms and angles)
Molluscum contagiosum is a disease caused by a poxvirus. It is more prevalent in children up to 5 years of age. There is a second peak of incidence in young adults. In order to examine its ultrastructure, three lesions were curetted without disruption, cut transversely with a scalpel, and routinely processed for scanning electron microscopy (SEM). The oval structure of molluscum contagiosum could be easily identified. In its core, there was a central umbilication and just below this depression, there was a keratinized tunnel. Under higher magnification, a proliferation similar to the epidermis was seen. Moreover, there were areas of cells disposed like a mosaic. Under higher magnification, rounded structures measuring 0.4 micron could be observed at the end of the keratinized tunnel and on the surface of the lesion.
- [5]

Under lower magnification, the oval structure of MC could be easily identified. In its core, there was a central umbilication and just below this depression, there was a keratinized tunnel (Figure 1). Under higher magnification, it was possible to observe the epidermis and the stratum corneum; underneath the epidermis, there was a proliferation similar to the epidermis (Figure 2). Moreover, there were areas of cells disposed like a mosaic (Figure 3).
- [5]

Herpes Simplex
Although capsids of herpes simplex virus were encountered within phagocytic vesicles, they were more commonly observed free within the cytoplasm. Stages in the release of virus from vesicles were not seen. There appeared to be five distinct steps in the process whereby the virus initiates infection: attachment, digestion of the viral envelope, digestion of the cell wall, passage of the capsid directly into the cytoplasm, and digestion of the capsid with release of the core. Antibody probably interferes with the first two stages.
- [6]

  1. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC375640/?page=3
  2. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC375640/?page=4
  3. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC375640/?page=5
  4. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC375640/?page=7
  5. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC375640/?page=8
Sources [credit to http://www.citethisforme.com/ for help with formatting of sources 1 and 2]:
[1] H, L. (2001). [Discovery of the first virus, the tobacco mosaic virus: 1892 or 1898?]. - PubMed - NCBI. [online] Ncbi.nlm.nih.gov. Available at: https://www.ncbi.nlm.nih.gov/pubmed/11570281 [Accessed 23 Feb. 2019].
[2] Courses.lumenlearning.com. (2018). The Viral Life Cycle | Microbiology. [online] Available at: https://courses.lumenlearning.com/microbiology/chapter/the-viral-life-cycle/ [Accessed 25 Feb. 2019].
[3] Craig Freudenrich, Ph.D. "How Viruses Work" 19 October 2000.
[4] Relevant to Round 1 and found at the bottom of it.
[5] Almeida, H. L., Abuchaim, M. O., Schneide, M. A., Marques, L., & Castro, L. A. (2013). Scanning electron microscopy of molluscum contagiosum. Anais brasileiros de dermatologia, 88(1), 90-3.
Download as: RISN
[6] Morgan, C., Rose, H. M., & Mednis, B. (1968). Electron microscopy of herpes simplex virus. I. Entry. Journal of virology, 2(5), 507-16.
Round 4
Somebody's avatar
Somebody
Pro
#7
Forfeited
RationalMadman's avatar
RationalMadman
Con
#8
If my opponent brings any new points and/or evidence in the final Round it is still bad conduct but entitles me to do the same back (I must, in order to rebuke).
Round 5
Somebody's avatar
Somebody
Pro
#9
Forfeited
RationalMadman's avatar
RationalMadman
Con
#10
End.