Originally posted by LiveFreeOrDie
Please answer the questions below. For each answer, please indicate the objective evidence and reasoning that supports your answer.
1. How old is the Earth?
2. Where did all the species we observe today come from?
Really, I'm not all that concerned with the age of the Earth per se, but more with the age of the geologic column. The earth itself may in fact be about 4.5 billion years old, but that really is a non-issue with me. I take issue with the idea that the geologic column was formed over the past several hundred million years. It seems to me that the geologic column was formed relatively rapidly as well as recently. For details as to why I think this visit:
"http://naturalselection.0catch.com/Files/The%20Geologic%20Column.html"
As far as the species on earth, many times various forms are given different species names based on phenotypic variations that are not necessarily outside the range for creatures that do in fact share a common gene pool.
For example, if the bulldog phenotype where found only in the fossil record and the German Shepherd were living today, would they be classed in the same species or even genus groups when compared side-by-side? I doubt it.
Since a single gene pool can produce "drastic" differences in phenotypic forms, how are scientists so sure of their fossil classification models? Often only slight phenotypic differences are enough to place a fossil creature in a different species, genus or even family group than its modern-day counterpart or than its counterpart found elsewhere in the geologic column. The problem is that differences, even fairly significant differences are known to exist between members of the same gene pool. Because of this fact, taxonomic classification models can be quite subjective and even misleading.
For example, scientists from Berkeley have noted that, "the planktonic larvae of many marine invertebrates are commonly described as separate species when they are first discovered in the ocean. Only later when they can be reared in the laboratory can the link to their adult form be recognized. Similarly, the different life stages of many fungi are given different names because they have different physical forms and hosts. Only through detailed inoculation studies can mycologists work out which forms are members of the same life cycle. Since some fungi may have more than five discrete life cycle stages, this can be a long process. Similar problems exist for some marine algae and multiple-host parasitic organisms of many kinds. Even among well-studied vertebrates, some tropical birds have been described as separate species until they are observed to mate and rear young together."
"http://www.ucmp.berkeley.edu/IB181/VPL/Pres/Pres1.html"
Also, a "Detailed study of large sympatric populations and fossil assemblages of the highly variable species Elphidium excavatum (Terquem) [Benthic foraminifera] collected from 20 widely spaced locations indicates that a variety of morphotypes of Elphidium can be linked to one another in a number of interlocking intergradational series. Ten morphotypes are recognized and grouped as formae (ecophenotypes) of Elphidium excavatum (Terquem); these morphotypes were previously considered as 22 independent taxa by various authors. Although all of these formae belong to the same species, it is suggested [by the authors] that the distinction among them should be retained because of their potential as a valuable interpretive tool in paleo-ecological and biostratigraphic studies of Holocene and Pleistocene sediments."
"http://www.dal.ca/~es/abstract/ab_th_83.htm"
Likewise, the classifications of plants is classically prone to give different names to very similar plants or even parts of the same plant. Bill DiMichele, a paleobotanist, notes, "The problem of organ association is one of the reasons why paleobotanists insist on so many different names for isolated parts of the same whole plant. Furthermore, there are phenotypic convergences that can cause great confusion, such leaves of virtually identical morphology borne on ferns and seed plants. Separate names for each fossil plant organ can be carried to extremes, however, and not all paleobotanists, myself included, favor the attribution of separate names to organs otherwise known in attachment (yes, this is still done routinely, no kidding)."
"http://www.ngdc.noaa.gov/mgg/sepm/palaios/9810/dimichele.html"
The Mazon Creek flora is incredibly diverse. Over 400 species from at least 130 genera have been identified from Mazon Creek nodules. However, the number of different kinds of plants represented is very difficult to determine. There are at least two reasons for this difficulty. The first reason is the convention among paleobotanists that separate plant parts receive different names. This procedure tends to inflate the number of plant names. The second reason is that paleobotanists are still trying to determine which taxa are valid.
"http://www.museum.state.il.us/exhibits/mazon_creek/about_mazon_creek.html"
The point is that many of the different "species" that we observe today could have descended from a smaller group of relatively static gene pools. Relatively static gene pools can and do give rise to a huge variety of forms or phenotypes. Each one of these different forms is simply an expression of part of a larger gene pool of phenotypic options. The gene pool itself need not have evolved to give rise to the variations. For example, the various breeds of dogs cover a very large range of different phenotypic forms, and yet such variations are not based on the acquisition of new genetic information into the gene pool. In other words, a non-evolving gene pool can rapidly give rise to a huge variety of different forms via some selection process that is not dependent upon allelic mutations or the gain of new information.
It seems to me that various gene pools are isolated by neutral gaps in genetic functions that cannot be crossed with the aid of natural selection in what anyone would consider to be a reasonable amount of time. Of course, studies done with galactosidase and nylonase evolution in bacteria have been hailed as clear example of evolution in action. To a point, I would agree. However, a closer look at what is actually involved with these cases also shows a clear limit to what functions such evolution can evolve. The gaps that are crossed by such mutations are one or at most two point mutations wide. Many might argue that the evolution of nylonase arose via a frame-shift mutation that involved changing hundreds of amino acids. This is true, but it was a change in only one amino acid that caused the frame shift. Thus, the gap between what was already there, and the new nylonase function, was crossed by a single mutation of one base pair position. Such a gap is not much a problem for random mutations like this to cross. It is only one random mutational step wide. The problem for evolution comes when new functions cannot be realized in just one or two steps, but are separated from all current functions by gaps of neutral mutations that are wider than two or three of these neutral steps.
For example, in an experiment with colonies of
E. coli bacteria B.G. Hall deleted the lacZ genes. Of course, the lacZ genes are the genes responsible for the production the lactase enzyme. Hall then grew these mutated bacteria on selective lactose enriched media. In a very short time, they "evolved" the ability to utilize lactose for energy again. What happened is that another gene with an unknown function evolved to produce a brand new enzyme with the lactase function after experiencing a single point mutation (ebgA evolved beta galactosidase). Hall was happy for the success of his experiment, but disappointed that only a single point mutation was all that was needed to evolve the new lactase enzyme. What is especially interesting is that he then proceeded to delete both the lacZ genes and the newly evolved ebgA gene in some of his
E. coli to see if these double mutants would evolve the lactase enzyme if placed on lactose media. They didn't and they haven't despite observation for over 20 years now. Hall described these bacteria as having, "limited evolutionary potential."
So, what is it that limits the evolutionary potential of a living organism? I propose that the blockade to evolution can be found in gaps of neutral function that are simply too wide to cross without the aid of natural selection in what anyone would consider a reasonable amount of time... even given an evolutionary time scale of billions of years.
For a more detailed discussion of this topic see:
"http://naturalselection.0catch.com/Files/Galactosidase%20Evolution.html"
Anyway, I hope this helps you understand my position better.
Sean
. I'm quite busy these days at work, but I will respond as much as I can because I really do find forums such as this quite interesting. 
