That’s a very nice review of review. And note that recombination can not create new genes...
Yes it can, kleinman. Recombination is just another source of variation in a population, and it is this variation which leads to new genes. If mutations can cause new genes to arrise (which it can), so can recombination (which it does).
...and that recombination with natural selection can cause the loss of alleles.
What? No! Recombination does not lead to a loss of anything!
Selection can lead to a loss of alleles.
Genetic drift can lead to a loss of alleles. Hell, even
mutation *might* lead to the loss of an allele (if every individual had the same mutation at that locus), although the likelyhood of that happening is tiny. But recombination
never leads to a loss of genetic data. The data is still there.
Recombination and selection is a much, much more rapid process for giving variation in a population as seen with animal breeding than is mutation and selection. You don’t seem to understand this despite your schooling.
Actually, I think you'll find that I know this quite well. But what this has to do with your claim that my model uses "recombination and selection" is beyond me.
And recombination and selection deals with alleles and does not increase the information content in the gene pool while mutation and selection does have the capability of increasing information in the gene pool but at an extremely slow rate. You would understand this if you studied the mathematics that ev reveals.
I hope you understand, kleinman, that "information" is hardly ever used by evolutionary genetic scientists. Why? Because it is a meaningless concept. But for the sake of argument,
variation is information. Recombination increases variation. Therefore, recombination increases information. QED.
The only thing you have cleared up is you have absolutely no idea of the mathematics of mutation and selection.
Recombination can only make new combinations of linked genes by crossing over between their loci.
Wrong. Recombination can, and does, occur
inside a gene, thus breaking it. It can join new genes together, insert parts of one gene into another, duplicate genes to reduce evolutionary pressures, and much more. Recombination leads to increased variation within a population, and thus "increased information".
You can create variation in the population but you can not create new genes.
Why not? Mutation increases variation in the population, and that variation leads to new genes. How is the variation created through mutation different from the variation created from recombination? Hint: It isn't.
A mutation is a permanent heritable change in the genetic material usually defined as a change in a single gene (point mutation) or more broadly for any structural change in a chromosome.
Wrong. A mutation is simply the change to the genetic basepair sequence. This can occur in many ways, including, but not limited to, point mutations, indel mutations, inversions, duplications and insertions.
The mathematical behavior of these two mechanisms of variation is completely different.
Not really, but I won't get into that. Recombination equations are long and boring.
Recombination and selection involves alleles where as mutation and selection involves a change in a particular allele, usually at a single loci.
Mutations can occur which duplicate a large portion of a chromosome, kleinman. Mutation is not single basepair effecting only.
Oh, the basic concept of selection for recombination and mutation may be the same, that is beneficial alleles and beneficial mutations enhance reproductive fitness. Where they differ is in the rate at which variations can be achieved.
Yes, but does that matter? No. Because "recombination and selection" and "mutation and selection" are not two different things acting independently on evolution. What you really have is "recombination, mutation, reproduction (etc) and selection" which can be shortened to "variation and selection". It doesn't matter how variation arrises, what matters is that it is there. Variation caused by recombination is no different from variation caused by mutation. It is all variation.
In the case of recombination, you can select alleles that give you Chihuahuas to Great Danes and a myriad of other breeds of dogs in only 5000 generations...
You do not "use recombination". You use variation. The variation in the population came about through a combination of mutation, reproduction and mutation. Also, please note, that by and large recombination
just moves genes around, although as I said earlier this isn't always the case. Once again, it matters not whence variation arose, only that it exists.
...yet they are all still dogs.
Can you explain what you mean by this? How are you defining what is a dog and what isn't? Be very specific.
You have no mathematical way of explaining the transformation of a reptile genome to a bird genome in the number of generations available.
Let us assume that we don't for the sake of argument. So? Does this mean it didn't happen? No, because it plainly did. There is more evidence that reptiles and birds shared a common ancestor then there is for us landing on the moon.
Mutation and selection is far too slow a process...
Not at all. Only if you take one form of mutation, point mutations, then perhaps it is. But mutations do not just act on a single locus.
...and you don’t have a selection pressure to do this...
Even if we can't, at the moment, describe a single selection pressure which caused birds to arise (the thought that it was only one is idiotic at best), does this mean it didn't happen? No. See above.
...and multiple selection pressures slow this process.
No they don't. Multiple selection pressures cause stronger selection, which increases the rate which allele frequences change over time. This is evolution.
Selection of alleles is very rapid; selection of mutations is a much, much slower process.
And here you show your fundamental lack of knowledge of genetics. An allele is just a specific sequence at a specific loci. New mutations give rise to new alleles. An allele is just like a name on a map. Some people have "new york" at that place, and some people have "washington" instead. Each different "name" at each location on the map which is present in a population is an allele. This can be a single basepair difference, or it can be many basepairs in length. A mutation which causes a basepair difference (i.e. all of them) at a specific locus generates a new allele.
Do you understand now?
Stephen J Gould’s concept of punctuated equilibrium is only applicable to recombination and selection; it has no applicability to mutation and selection.
No, kleinman, because there is no difference between "mutation and selection" and "recombination and selection". There is only "variation and selection".
Some day the differences in the mathematics of recombination and selection and mutation and selection will sink in with you evolutionists.
That isn't very likely, because this is all very well understood already, and it is known that different causes of variation all cause variation which is acted upon by selection. There is no difference.
Stop whining, I have to listen to your mathematically deficient understanding of recombination and selection and mutation and selection.
Since there is no such thing, I find this hard to believe. I say again,
selection acts on variation in a population, not how that variation arose.
Last I heard, genes in humans are formed by recombination (including genomes with the hemoglobin S gene)...
No, genes in humans (and everything) arose through selection acting on
variation.
...and if the a particular allele is beneficial, it will increase propagate, spread, proliferate, increase in frequency in the population. So your immature attempt at parsing words adds nothing to the discussion.
I'm not "parsing words", I'm pointing out that you are using the words incorrectly. And you plainly do not understand them, because you are comparing apples to appletrees. One is a fruit, and one causes fruit.
And learn how to spell propagate.
My spelling has nothing to do with the argument. Also, for everyone else, I'm fairly sure I have never used that word. Please point out where I have.
Once you do that, learn the differences in the mathematics of recombination and selection and mutation and selection.
I don't need to, because there is no such difference. There is only variation and selection, and both mutation and recombination give rise to variation. There is nothing different between the two "types" of variation. Variation is variation.
Then once you do that, do a google search with the following terms; combination "selection pressures" resistance and you will find a huge number of papers that show that combination selection pressures slow the evolution of resistant strains of a wide variety of different types of life forms. No need to parse words to try to make this point.[/SIZE][/FONT]
The first three results are as follows:
The incidence of trimethoprim resistance was correlated with changes in prescription behaviour in the Nottingham area from 1978-1985. The prevalence of trimethoprim resistance among Enterobacteriaceae isolated from patients with urinary tract infection rose from 5% to 15% of total strains examined. Strains resistant to trimethoprim but susceptible to sulfamethoxazole appeared from 1980 onward and represented 35% of the total trimethoprim-resistant strains examined in 1985. Co-trimoxazole (trimethoprim + sulfamethoxazole) has been generally available for prescription in the United Kingdom since 1969, whereas trimethoprim alone was released in October 1979. By 1983, prescriptions in the form of trimethoprim alone accounted for approximately 50% (in hospitals) and 15% (in the community) of total trimethoprim usage in the Nottingham area. Although the introduction of trimethoprim alone seems to have had only a minor effect on overall resistance levels, it has greatly increased the proportion of trimethoprim-resistant strains which are susceptible to sulfamethoxazole. This was particularly evident in strains of Proteus spp., in which 52% of the total trimethoprim-resistant strains were sulfamethoxazole-susceptible in 1985.
Source
Nothing in here about "multiple selection pressures slowing evolution".
WILD-TYPE reverse transcriptase has evolved for the survival of human immunodeficiency virus type 1 (HIV-1) by natural selection1. In contrast, therapy relying on inhibitors of reverse transcriptase by nucleosides like zidovudine (AZT) or dideoxyinosine (ddl), and by non-nucleosides like pyridinones or nevirapine2–6, may exert different selection pressures on this enzyme. Therefore the acquisition of resistance to reverse transcriptase inhibitors by selection of mutations in the pol gene7–15 may require compromises in enzyme function that affect viral replication. As single mutations are unlikely to confer broad resistance when combinations of reverse transcriptase inhibitors are used, multiple mutations may occur that result in further compromises. Certain drug combinations may prevent the co-existence of adequate reverse transcription function and multi-drug resistance (MDR). Unlike bacterial or eukaryotic drug resistance, retroviral drug resistance is conferred only by mutations in its own genome16 and is limited by genome size. Combining drugs directed against the same essential viral protein may thus prevent HIV-1 MDR, whereas the conventional approach of targeting different HIV-1 proteins for combination therapy may not, because genomes with resistance mutations in different HIV-1 genes might recombine to develop MDR17. Here we show that several mutations in the HIV-1 reverse transcriptase gene that confer resistance to inhibitors of this enzyme can attenuate viral replication. We tested whether combinations of mutations giving rise to single-agent resistance might further compromise or even abolish viral replication, and if multidrug-resistant viruses could be constructed. Certain combinations of mutations conferring resistance to AZT, ddl and pyridinone are incompatible with viral replication. These results indicate that evolutionary limitations exist to restrict development of MDR. Furthermore, a therapeutic strategy exploiting these limitations by using selected multidrug regimens directed against the same target may prevent development of MDR. This approach, which we call convergent combination therapy, eliminated HIV-1 replication and virus breakthrough in vitro, and may be applicable to other viral targets. Moreover, elimination of reverse transcription by convergent combination therapy may also limit MDR.
Source
Nothing in here about multiple selection pressures slowing evolution either. Please note that this paper is about multiple resistance development causing a functional change to a protein which inhibits viral reproduction.
The evolution of herbicide resistance within a weed population is based on selection pressure. The more frequently a herbicide is used, the more pressure placed on a weed population, and the sooner resistance will appear at a troublesome level in the population. Using alternative modes of action can reduce the potential for selecting resistant weeds by placing different selection pressures on weed populations. In a system relying only on glyphosate, a weed possessing a trait allowing it to survive glyphosate will rapidly increase in frequency. But if a second herbicide is used with glyphosate, this alternative herbicide may kill the weed with the glyphosate resistant trait and prevent it from increasing within the weed population. Theoretically this approach is sound and can reduce the potential for herbicide resistance.
Source
Nothing in here about multiple selection pressures slowing evolution. In fact, if you note the bolded section added by me, it actually says that increased selection pressure
speeds up the evolution of resistance.
So, where exactly are all these "huge numbers" of papers?
