Microsoft Word Kurzweil, Ray The Singularity Is Near doc

Analyses conducted by Rob Freitas and others show that it is quite feasible to restrict the width of such a 
manipulator to under twenty nanometers. 
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Another approach is to keep the nanobots in the capillaries and use noninvasive scanning. For example, the 
scanning system being designed by Finkel and his associates can scan at very high resolution (sufficient to see 
individual interconnections) to a depth of 150 microns, which is several times greater than we need. Obviously 
this type of optical-imaging system would have to be significantly miniaturized (compared to contemporary 
designs), but it uses charge-coupled device sensors, which are amenable to such size reduction. 
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Another type of noninvasive scanning would involve one set of nanobots emitting focused signals similar to 
those of a two-photon scanner and another set of nanobots receiving the transmission. The topology of the 
intervening tissue could be determined by analyzing the impact on the received signal. 
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Another type of strategy, suggested by Robert Freitas, would be for the nanobot literally to barge its way past the 
BBB by breaking a hole in it, exit the blood vessel, and then repair the damage. Since the nanobot can be 
constructed using carbon in a diamondoid configuration, it would be far stronger than biological tissues. Freitas 
writes, "To pass between cells in cell-rich tissue, it is necessary for an advancing nanorobot to disrupt some 
minimum number of cell-to-cell adhesive contacts that lie ahead in its path. After that, and with the objective of 
minimizing biointrusiveness, the nanorobot must reseal those adhesive contacts in its wake, crudely analogous to 
a burrowing mole."
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Yet another approach is suggested by contemporary cancer studies. Cancer researchers are keenly interested in 
selectively disrupting the BBB to transport cancer-destroying substances to tumors. Recent studies of the BBB 
show that it opens up in response to a variety of factors, which include certain proteins, as mentioned above; 
localized hypertension; high concentrations of certain substances; microwaves and other forms of radiation; 
infection; and inflammation. There are also specialized processes that ferry out needed substances such as 
glucose. It has also been found that the sugar mannitol causes a temporary shrinking of the tightly packed 
endothelial cells to provide a temporary breach of the BBB. By exploiting these mechanisms, several research 
groups are developing compounds that open the BBB.
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Although this research is aimed at cancer therapies, 
similar approaches can be used to open the gateways for nanobots that will scan the brain as well as enhance our 
mental functioning. 
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We could bypass the bloodstream and the BBB altogether by injecting the nanobots into areas of the brain that 
have direct access to neural tissue. As I mention below, new neurons migrate from the ventricles to other parts of 
the brain. Nanobots could follow the same migration path. 
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Rob Freitas has described several techniques for nanobots to monitor sensory signals.
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These will be important 
both for reverse engineering the inputs to the brain, as well as for creating full-immersion virtual reality from 
within the nervous system. 
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To scan and monitor auditory signals, Freitas proposes "mobile nanodevices ... [that] swim into the spiral 
artery of the ear and down through its bifurcations to reach the cochlear canal, then position themselves as 
neural monitors in the vicinity of the spiral nerve fibers and the nerves entering the epithelium of the organ 
of Corti [cochlear or auditory nerves] within the spiral ganglion. These monitors can detect, record, or 
rebroadcast to other nanodevices in the communications network all auditory neural traffic perceived by 
the human ear." 
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For the body's "sensations of gravity, rotation, and acceleration," he envisions "nanomonitors positioned at 
the afferent nerve endings emanating from hair cells located in the ... semicircular canals." 
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For "kinesthetic sensory management ... motor neurons can be monitored to keep track of limb motions 
and positions, or specific muscle activities, and even to exert control." 
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"Olfactory and gustatory sensory neural traffic may be eavesdropped [on] by nanosensory instruments." 
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"Pain signals may be recorded or modified as required, as can mechanical and temperature nerve impulses 
from ... receptors located in the skin." 

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Freitas points out that the retina is rich with small blood vessels, "permitting ready access to both 
photoreceptor (rod, cone, bipolar and ganglion) and integrator ... neurons." The signals from the optic 
nerve represent more than one hundred million levels per second, but this level of signal processing is 
already manageable. As MIT's Tomaso Poggio and others have indicated, we do not yet understand the 
coding of the optic nerve's signals. Once we have the ability to monitor the signals for each discrete fiber 
in the optic nerve, our ability to interpret these signals will be greatly facilitated. This is currently an area 
of intense research. 
As I discuss below, the raw signals from the body go through multiple levels of processing before being 
aggregated in a compact dynamic representation in two small organs called the right and left insula, located deep in the 
cerebral cortex. For full-immersion virtual reality, it may be more effective to tap into the already-interpreted signals 
in the insula rather than the unprocessed signals throughout the body. 
Scanning the brain for the purpose of reverse engineering its principles of operation is an easier action than 
scanning it for the purpose of "uploading" a particular personality, which I discuss further below (see the "Uploading 
the Human Brain" section, p. 198). In order to reverse engineer the brain, we only need to scan the connections in a 
region sufficiently to understand their basic pattern. We do not need to capture every single connection. 
Once we understand the neural wiring patterns within a region, we can combine that knowledge with a detailed 
understanding of how each type of neuron in that region operates. Although a particular region of the brain may have 
billions of neurons, it will contain only a limited number of neuron types. We have already made significant progress 
in deriving the mechanisms underlying specific varieties of neurons and synaptic connections by studying these cells 
in vitro (in a test dish), as well as in vivo using such methods as two-photon scanning. 
The scenarios above involve capabilities that exist at least in an early stage today. We already have technology 
capable of producing very high-resolution scans for viewing the precise shape of every connection in a particular brain 
area, if the scanner is physically proximate to the neural features. With regard to nanobots, there are already four major 
conferences dedicated to developing blood cell-size devices for diagnostic and therapeutic purposes.
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As discussed in 
chapter 2, we can project the exponentially declining cost of computation and the rapidly declining size and increasing 
effectiveness of both electronic and mechanical technologies. Based on these projections, we can conservatively 
anticipate the requisite nanobot technology to implement these types of scenarios during the 2020s. Once nanobot-
based scanning becomes a reality, we will finally be in the same position that circuit designers are in today: we will be 
able to place highly sensitive and very high-resolution sensors (in the form of nanobots) at millions or even billions of 
locations in the brain and thus witness in breathtaking detail living brains in action. 

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