"Function" in the human genome according to the evolution-free gospel of ENCODE
Dan Graur is an evolutionary and molecular biologist. In 2013 he and several others published a response to the 2012 results from the ENCODE team that > 80% of the genome is functional. They argued "progress in understanding the functional significance of DNA sequences can only be achieved by not ignoring evolutionary principles", although also highlighting signatures of function found by ENCODE that could be explained by other means.
Neutral Theory and Genetic Load
[The ENCODE consortium] put forward the idea that more than 80% of the human genome is functional. This claim flies in the face of current estimates according to which the fraction of the genome that is evolutionarily conserved through purifying selection is under 10%. Thus, according to the ENCODE Consortium, a biological function can be maintained indefinitely without selection, which implies that at least 80 – 10 = 70% of the genome is perfectly invulnerable to deleterious mutations, either because no mutation can ever occur in these “functional” regions, or because no mutation in these regions can ever be deleterious. This absurd conclusion was reached through various means....
only sequences that can be shown to be under selection can be claimed with any degree of confidence to be functional.... The absurd alternative, which unfortunately was adopted by ENCODE, is to assume that no deleterious mutations can ever occur in the regions they have deemed to be functional. Such an assumption is akin to claiming that a television set left on and unattended will still be in working condition after a million years because no natural events, such as rust, erosion, static electricity, and earthquakes can affect it.
there exists a misconception among functional genomicists that the evolutionary process can produce a genome that is mostly functional. Actually, evolution can only produce a genome devoid of “junk” if and only if the effective population size is huge and the deleterious effects of increasing genome size are considerable... In humans, there seems to be no selection against excess genomic baggage. Our effective population size is pitiful and DNA replication does not correlate with genome size.
Whether transcribed or not, the vast majority of transposons in the human genome are merely parasites, parasites of parasites, and dead parasites, whose main “function” would appear to be causing frameshifts in reading frames, disabling RNA-specifying sequences, and simply littering the genome.
Trial and Error
Graur et. al. quote François Jacob, writing in 2007:
[N]atural selection does not work as an engineer… It works like a tinkerer—a tinkerer who does not know exactly what he is going to produce but uses whatever he finds around him whether it be pieces of string, fragments of wood, or old cardboards… The tinkerer… manages with odds and ends. What he ultimately produces is generally related to no special project, and it results from a series of contingent events, of all the opportunities he had to enrich his stock with leftovers.
Appears to do Nothing
The human genome is populated by a very large number of transposable and mobile elements. Transposable elements, such as LINEs, SINEs, retroviruses, and DNA transposons, may, in fact, account for up to two thirds of the human genome
They quote a personal communication from T. Ryan Gregory:
The onion test is a simple reality check for anyone who thinks they can assign a function to every nucleotide in the human genome. Whatever your proposed functions are, ask yourself this question: Why does an onion need a genome that is about five times larger than ours?
How much is junk?
the proportion of the human genome that is functional is likely to be larger to some extent than the approximately 9% for which there exists some evidence for selection, but the fraction is unlikely to be anything even approaching 80%....
Ward and Kellis (2012) confirmed that ~5% of the genome is interspecifically conserved, and by using intraspecific variation, found evidence of lineage-specific constraint suggesting that an additional 4% of the human genome is under selection (i.e., functional), bringin the total fraction of the genome that is certain to be functional to approximately 9%.
At the end, Graur etl al. tell us their arguments are really only in opposition to ID proponents:
We urge biologists not be afraid of junk DNA. The only people that should be afraid are those claiming that natural processes are insufficient to explain life and that evolutionary theory should be supplemented or supplanted by an intelligent designer (e.g., Dembski 1998; Wells 2004)
Bradley Bernstein, an ENCODE researcher at Harvard University remarked in Science that "Graur wrote such a negative paper that it was hard to read... Graur’s criticism is so over-the-top that it’s not worthy."
On reddit, an ENCODE researcher pointed out [archive.is mirror] that Graur was incorrect in some of his accusations, such as ENCODE using HeLa cells (cancerous cells that continue to replicate outside humans) as tests for transcription:
The vast majority of the RNAseq was performed in GM12878 or K562 (but we looked at a lot of different cell types, see here... That assertion is completely false and I don't want that misinformation being spread... We used K562 because it is transcriptionally normal