Mr.C’s numbness of his feet is most likely due to
symmetric polyneuropathy affecting the distal axons.
Although diabetic neuropathy is most frequently
symmetric, it may also be focal (more common in Type II
older diabetics) and often involves the autonomic
nervous system (Inzucchi & Sherwin, 2008). Our initial
introduction to Mr. C indicated he had numbness to both
feet for an unspecified period of time. Mr. C’s symptoms
of numbness to both feet is not unusual for diabetics as
peripheral neuropathies are present in approximately 50%
of all diabetics (Inzuccchi & Sherwin, 2008). 

What types of neuropathy are there and how do they
differ?

The simplest definition of neuropathy as defined by
Stedman’s Medical Dictionary (2005) includes, “any
disorder that affects the nervous system, specifically
diseases involving the cranial nerves, peripheral or
autonomic nervous systems” (p.999).  The peripheral
nervous system (PNS) is a large communication network
which relays information from the brain and spinal cord
(CNS) to every other part of the body and sends sensory
information back the CNS. “Damage to the peripheral
nervous system interferes with vital connections
[similar to] static on a telephone line”
(http://www.ninds.nih.gov/), causing a distortion and
sometimes interruption in the messages between the brain
and the rest of the body. Individuals who present with
peripheral neuropathies have decreased nerve growth
factor that impacts the degree of possible nerve
regeneration. Acute neuropathy has a better prognosis
towards resolution than chronic neuropathy.  “Chronic,
more insidious neuropathies may be mediated by metabolic
factors, whereas the more acute, self-limiting
neuropathies most likely have a vascular component”
(Inzuccchi & Sherwin, 2008, p. 1745).  Autonomic
neuropathies are complex and carry a poor prognosis. 
They accompany other pathologic complications in the
various organs impacted. For example, the
parasympathetic nervous system is responsible for
cardiovascular complications such as diminished heart
rate and myocardial ischemia, whereas  altered
gastrointestinal function such as diarrhea is  impacted
by an impaired sympathetic inhibition (Inzuccchi &
Sherwin, 2008). Other autonomic presentations may be
include the loss of sweating, postural hypotension,
sexual dysfunction, bowel and bladder dysfunction, and
impaired gastric emptying (NINDS, 2008). There are more
than 100 different types of peripheral neuropathies.
Identifying these neuropathies is simplified by placing
the various pathologies into a classification system
that identifies the different nerve fibers that are
affected. According to Boss (2006) neuropathies may be
classified into three broad categories;  1.	Generalized
symmetric polyneuropathies; 2.	Generalized neuropathies;
 3.	focal or multiple neuropathies. (p. 594) Generalized
symmetric polyneuropathies (GSPN) include symmetrical
sides of the body (e.g. numbness to both feet) and may
include the sensory, motor, or autonomic fibers.
Polyneuropathies refer to diffuse disorders of many
peripheral nerves.  Further, GSPN may be furthered
divided into distal axonal polyneuropathy or
demyelinating polyneuropathy.  Distal axonal
(sensori-motor) neuropathy  is the most common
neuropathy in diabetics (Boss, 2006). All somatic nerves
are impacted as well as the distal sensori-motor nerves
in the feet and hands (Inzuccchi & Sherwin, 2008). Both
the small unmyelinated C fibers that transmit pain and
temperature, as well as the larger myelinated fibers
(touch, vibration, and proprioception) are affected
(Inzuccchi & Sherwin, 2008). A more complex range of
symptoms occur as a result of sensory nerve damage
(NINDS, 2008). Initially, people are asymptomatic as
changes are very subtle but with progression of nerve
degeneration people complain of burning pain, tingling,
and numbness of the feet. In addition to the general
symptoms, damage to the small nerve fibers cause
decreased somatic pain and temperature sensation. Over
time, damage to large sensory nerve fibers will result
in a continuous decline in individuals ability to
discriminate light touch, vibration, and sense of
position (Inzuccchi & Sherwin, 2008; NINDS, 2008).  The
two primary causes are diabetes mellitus and alcoholism.
Diabetic polyneuropathy is often related tot the degree
and duration of uncontrolled diabetes. Diabetic
neuropathy is usually chronic and is often as a result
of metabolic factors. General symptoms include weakness
or sensory loss in the sensory nerves first. Often
diabetics will experience neuropathies in both their
hands and feet referred to as “stocking and glove
sensory loss ” (NINDS, 2008). Axonal polyneuropathies
related to alcoholism usually involves a nutritional
deficiency with the most significant impact on thiamine
loss. With the correction of this deficiency and
abstinence from alcohol an improvement in symptoms occur
(Shy, 2008).  Individuals with axonal polyneuropathies
recover over a prolonged period of time depending on the
axonal regrowth. Axons grow approximately 1-3 mm/day
therefore regrowth is over an extended period of time
and is dependent upon the length of the nerve fiber
damaged (Zochodone, personal communication, date
unknown). As well, those with axonal neuropathy often
experience muscle wasting further complicating recovery.
	Demyelinating polyneuropathy occurs less often and
includes the myelin and Schwann cells. The axon is
preserved, however there is loss of the myelin sheath.
Demyelination can be internodal or paranodal (Shy,
2008).  In general, the predominant symptom is weakness
with more motor than sensory involvement. For example,
Guillain-Barre syndrome is an acquired inflammatory
disease resulting in demyelinating neuropathy of the
peripheral nerves (Boss, 2008). Guillain- Barre is often
preceded by an illness or vaccination and is
“characterized by acute onset of a motor paralysis,
usually of an ascending nature” (Boss, 2006). It is
thought that the neuropathic nature of this illness is
“both a humoral and cell-mediated immunologic reaction
directed by the peripheral nerve myelin” (Boss, 2006). 
Gillian-Barre has an acute onset of ascending weakness,
flaccidity, and areflexia involving both spinal and
cranial nerves, as well as sudden autonomic alterations
including pain and numbness (Shy, 2008).  People who
have demyelinating polyneuropathies generally will
experience  recovery however, 20% will have persistent
disabilities (Shy, 2008).  	Inherited polyneuropathies
affect both the sensory and motor neurons. Charcot Marie
Tooth Disease, leukodystrophy, Freidrich’s ataxia are
example of inherited polyneuropathies (Shy, 2008). 
	“Generalized neuropathies affect the cell body of only
one type of peripheral neuron” (Boss, 2006, p. 594).
Focal, asymmetric or distal symmetric distributions are
considered generalized neuropathies. Sensory
neuropathies affect the dorsal root ganglion causing
numbness. This numbness may result in a focal or
multifocal neuropathy affecting both the sensory and
motor fibers. Generally these neuropathies present with
pain, have a sudden onset, and commonly occur in nerves
of the oculomotor, median, radial, and lateral popliteal
(Inzuccchi & Sherwin, 2008).   Focal neuropathy may also
be referred to as mononeuropathy and is a disorder of
one peripheral nerve, root or plexus territory
(Zochodne, personal communication, date unknown). Focal
neuropathies may present with motor or sensory symptoms.
 Mononeuropathies may be a  result of trauma,
compression or entrapment, root disorders, plexus
disorders, or cranial neuropathies. For example Bell’s
Palsy is a result of cranial nerve involvement whereas
foot drop involves the peroneal nerve causing the
inability to dorsiflex foot. Carpel tunnel syndrome,
ulnar nerve compression, and sciatic nerve compression
are examples of focal neuropathies as well. Nerve
compression may lead to either demyelination or injury
to the axon. Injury may be caused from repetitive use
syndrome or trauma to the nerve
(http://www.medicinenet.com). The primary signs and
symptoms of focal neuropathies are dermatomal numbness,
pain, and possible muscle atrophy in Wallerian
degeneration caused by a lack of nerve input to the
muscle (Zochodne, personal communication, date unknown).
Sensory neuropathies include leprosy, industrial solvent
poisoning that effect the sensory neurons, hereditary
disorders, and toxicity to chemicals such as
chloramphenicol. Motor neuropathy affects the anterior
horn of the spinal tract causing muscle weakness that
can affect one or both sides of the body. Examples of 
motor neuropathies include amyotrophic lateral sclerosis
(ALS) or poliomyelitis (Boss, 2006, p. 594).  	 
References

Boss, B.J. (2006). Alterations of neurologic function.
In McCance & Huether, Pathophysiology: The biologic
basis for disease in adults and children (5th ed.).
Philadelphia: Elsevier Mosby. National Institute of
Neurological Disorders and Stroke (2008). Peripheral
neuropathy fact sheet.  	 Retrieved on May 25, 2008 form
http://www.ninds.nih.gov/ Shy, M.E. (2008). Peripheral
neuropathies. In Goldman & Ausiello, Cecil Medicine
(23rd ed.).     		   Philadelphia: Saunders Elsevier.