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   ICD9        = {{ICD9|250.6}} |
   ICD9        = {{ICD9|250.6}} |
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'''Diabetic neuropathies''' are [[neuropathy|neuropathic]] disorders that are associated with [[diabetes mellitus]]. These conditions are thought to result from diabetic microvascular injury involving small [[blood vessel]]s that supply nerves ([[vasa nervorum]]). Relatively common conditions which may be associated with diabetic neuropathy include [[third nerve palsy]]; [[mononeuropathy]]; mononeuropathy multiplex; diabetic [[amyotrophy]]; a [[Pain and nociception|painful]] polyneuropathy; [[autonomic]] neuropathy; and thoracoabdominal neuropathy.
'''Diabetic neuropathies''' are [[neuropathy|neuropathic]] disorders that are associated with [[diabetes mellitus]]. These conditions are thought to result from diabetic microvascular injury involving small blood vessels that supply nerves ([[vasa nervorum]]). Relatively common conditions which may be associated with diabetic neuropathy include [[third nerve palsy]]; [[mononeuropathy]]; mononeuropathy multiplex; diabetic [[amyotrophy]]; a [[Pain and nociception|painful]] polyneuropathy; [[autonomic]] neuropathy; and thoracoabdominal neuropathy.


==Epidemiology==
==Epidemiology==
{{Diabetes}}
In developed countries, [[diabetes mellitus]] is the leading known<ref>The largest group of neuropathy patients are of unknown cause, referred to as [[idiopathic]] in origin. Of the roughly 100 known causes, diabetes is by far the largest. Other known causes include genetic factors, damaging chemical agents such as chemotherapy drugs, and HIV.</ref> cause of neuropathy , and neuropathy is the most common complication and greatest source of [[morbidity]] and [[death|mortality]] in diabetes patients. It is estimated that the [[prevalence]] of neuropathy in diabetes patients is approximately 20%. Diabetic neuropathy is implicated in 50-75% of nontraumatic [[amputation]]s.
Diabetes is the leading known* cause of neuropathy in developed countries, and neuropathy is the most common complication and greatest source of [[morbidity]] and [[death|mortality]] in diabetes patients. It is estimated that the [[prevalence]] of neuropathy in diabetes patients is approximately 20%. Diabetic neuropathy is implicated in 50-75% of nontraumatic [[amputation]]s.


The main risk factor for diabetic neuropathy is [[hyperglycemia]]. In the DCCT (Diabetes Control and Complications Trial, 1995) study, the annual incidence of neuropathy was 2% per year, but dropped to 0.56% with intensive treatment of Type 1 diabetics. The progression of neuropathy is dependent on the degree of glycemic control in both Type 1 and Type 2 diabetes. Duration of diabetes, [[senescence|age]], [[cigarette]] smoking, [[hypertension]], height and [[hyperlipidemia]] are also risk factors for diabetic neuropathy.
The main risk factor for diabetic neuropathy is [[hyperglycemia]]. In the DCCT (Diabetes Control and Complications Trial, 1995) study, the annual incidence of neuropathy was 2% per year, but dropped to 0.56% with intensive treatment of Type 1 diabetics. The progression of neuropathy is dependent on the degree of glycemic control in both Type 1 and Type 2 diabetes. Duration of diabetes, [[senescence|age]], [[cigarette]] smoking, [[hypertension]], height and [[hyperlipidemia]] are also risk factors for diabetic neuropathy.
*The largest group of neuropathy patients are of unknown cause, referred to as [[idiopathic]] in origin. Of the roughly 100 known causes, diabetes is by far the largest. Other known causes include genetic factors, damaging chemical agents such as chemotherapy drugs, and HIV.


==Pathology and pathogenesis==
==Pathology and pathogenesis==
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===Microvascular disease===
===Microvascular disease===
Vascular and neural diseases are closely related and intertwined. [[Blood vessel]]s depend on normal [[nerve function]], and nerves depend on adequate [[blood flow]]. The first pathological change in the microvasculature is [[vasoconstriction]]. As the disease progresses, neuronal dysfunction correlates closely with the development of vascular abnormalities, such as [[capillary basement membrane thickening]] and [[endothelial hyperplasia]], which contribute to diminished [[oxygen tension]] and [[Hypoxia (medical)|hypoxia]]. [[Neuronal ischemia]] is a well-established characteristic of diabetic neuropathy. [[Vasodilator]] agents (e.g., [[angiotensin-converting-enzyme inhibitor]]s, α1-antagonists) can lead to substantial improvements in neuronal [[blood flow]], with corresponding improvements in [[Nerve conduction velocity|nerve conduction velocities]]. Thus, microvascular dysfunction occurs early in diabetes, parallels the progression of neural dysfunction, and may be sufficient to support the severity of structural, functional, and clinical changes observed in diabetic neuropathy.
Vascular and neural diseases are closely related and intertwined. Blood vessels depend on normal [[nerve function]], and nerves depend on adequate [[blood flow]]. The first pathological change in the microvasculature is [[vasoconstriction]]. As the disease progresses, neuronal dysfunction correlates closely with the development of vascular abnormalities, such as [[capillary basement membrane thickening]] and [[endothelial hyperplasia]], which contribute to diminished [[oxygen tension]] and [[Hypoxia (medical)|hypoxia]]. [[Neuronal ischemia]] is a well-established characteristic of diabetic neuropathy. [[Vasodilator]] agents (e.g., [[angiotensin-converting-enzyme inhibitor]]s, α1-antagonists) can lead to substantial improvements in neuronal [[blood flow]], with corresponding improvements in [[Nerve conduction velocity|nerve conduction velocities]]. Thus, microvascular dysfunction occurs early in diabetes, parallels the progression of neural dysfunction, and may be sufficient to support the severity of structural, functional, and clinical changes observed in diabetic neuropathy.


===Advanced glycated end products===
===Advanced glycated end products===
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===Sensorimotor polyneuropathy===
===Sensorimotor polyneuropathy===
Longer nerve fibers are affected to a greater degree than shorter ones, because nerve conduction velocity is slowed in proportion to a nerve's length. In this syndrome, decreased sensation and loss of reflexes occurs first in the toes bilaterally, then extends upward. It is usually described as glove-stocking distribution of numbness, sensory loss, [[dysesthesia]] and nighttime pain. The pain can feel like burning, pricking sensation, achy or dull. Pins and needles sensation is common. Loss of [[proprioception]], that is, the sense of where a limb is in space, is affected early. These patients cannot feel when they are stepping on a foreign body, like a splinter, or when they are developing a callous from an ill-fitting shoe. Consequently, they are at risk for developing [[ulcer]]s and infections on the feet and legs, which can lead to [[amputation]]. Similarly, these patients can get multiple fractures of the knee, ankle or foot, and develop a [[Charcot joint]]. Loss of motor function results in dorsiflexion [[contracture]]s of the toes, loss of the interosseous muscle function  and leads to contraction of the digits, so called [[hammer toe]]s. These contractures occur not only in the foot but also in the hand where the loss of the musculature makes the hand appear gaunt and skeletal. The loss of muscular function is progressive.
Longer nerve fibers are affected to a greater degree than shorter ones, because nerve conduction velocity is slowed in proportion to a nerve's length. In this syndrome, decreased sensation and loss of reflexes occurs first in the toes bilaterally, then extends upward. It is usually described as glove-stocking distribution of numbness, sensory loss, [[dysesthesia]] and nighttime pain. The pain can feel like burning, pricking sensation, achy or dull. Pins and needles sensation is common. Loss of [[proprioception]], that is, the sense of where a limb is in space, is affected early. These patients cannot feel when they are stepping on a foreign body, like a splinter, or when they are developing a callous from an ill-fitting shoe.
 
These patients are at risk for developing [[diabetic foot]] and [[foot ulcer]]s and infections on the feet and legs, which can lead to [[amputation]]. Similarly, these patients can get multiple fractures of the knee, ankle or foot, and develop a [[Charcot joint]]. Loss of motor function results in dorsiflexion [[contracture]]s of the toes, loss of the interosseous muscle function  and leads to contraction of the digits, so called [[hammer toe]]s. These contractures occur not only in the foot but also in the hand where the loss of the musculature makes the hand appear gaunt and skeletal. The loss of muscular function is progressive.


===Autonomic neuropathy===
===Autonomic neuropathy===
The [[autonomic nervous system]] is composed of nerves serving the [[heart]], [[gastrointestinal system]] and [[urinary-genital system]]. [[Autonomic neuropathy]] can affect any of these organ systems. The most commonly recognized autonomic dysfunction in diabetics is [[orthostatic hypotension]], or the uncomfortable sensation of [[fainting]] when a patient stands up. In the case of diabetic autonomic neuropathy, it is due to the failure of the heart and arteries to appropriately adjust heart rate and vascular tone to keep blood continually and fully flowing to the [[brain]][failure of the sensitivty of the baroreceptors]. This symptom is usually accompanied by a loss of sinus respiratory variation, that is, the usual change in heart rate seen with normal breathing. When these 2 findings are present, cardiac autonomic neuropathy is present.
The [[autonomic nervous system]] is composed of nerves serving the [[heart]], [[gastrointestinal system]] and [[urinary-genital system]]. [[Autonomic neuropathy]] can affect any of these organ systems. The most commonly recognized autonomic dysfunction in diabetics is [[orthostatic hypotension]], or the uncomfortable sensation of [[fainting]] when a patient stands up. In the case of diabetic autonomic neuropathy, it is due to the failure of the heart and arteries to appropriately adjust heart rate and vascular tone to keep blood continually and fully flowing to the [[brain]][failure of the sensitivity of the baroreceptors]. This symptom is usually accompanied by a loss of sinus respiratory variation, that is, the usual change in heart rate seen with normal breathing. When these 2 findings are present, cardiac autonomic neuropathy is present.


GI tract manifestations include [[delayed gastric emptying]], [[gastroparesis]], [[nausea]], [[bloating]], and [[diarrhea]]. Because many diabetics take oral medication for their diabetes, absorption of these medicines is greatly affected by the [[delayed gastric emptying]]. This can lead to [[hypoglycemia]] when an oral diabetic agent is taken before a meal and does not get absorbed until hours, or sometimes days later, when there is normal or low blood sugar already. Sluggish movement of the [[small instestine]] can cause [[bacteria]]l overgrowth, made worse by the presence of [[hyperglycemia]]. This leads to [[bloating]], gas and [[diarrhea]].
GI tract manifestations include [[delayed gastric emptying]], [[gastroparesis]], [[nausea]], [[bloating]], and [[diarrhea]]. Because many diabetics take oral medication for their diabetes, absorption of these medicines is greatly affected by the [[delayed gastric emptying]]. This can lead to [[hypoglycemia]] when an oral diabetic agent is taken before a meal and does not get absorbed until hours, or sometimes days later, when there is normal or low blood sugar already. Sluggish movement of the [[small intestine]] can cause [[bacteria]]l overgrowth, made worse by the presence of [[hyperglycemia]]. This leads to [[bloating]], gas and [[diarrhea]].


Urinary symptoms include urinary frequency, urgency, [[Urinary incontinence|incontinence]] and retention. Again, because of the retention of sweet [[urine]], [[urinary tract infections]] are frequent. Urinary retention can lead to [[bladder diverticula]], stones, [[reflux nephropathy]].
Urinary symptoms include urinary frequency, urgency, [[Urinary incontinence|incontinence]] and retention. Again, because of the retention of sweet [[urine]], [[urinary tract infections]] are frequent. Urinary retention can lead to [[bladder diverticula]], stones, [[reflux nephropathy]].
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==Screening==
==Screening==
The [[National Institute for Health and Clinical Excellence]] (NICE) has addressed screening and recommends annually:<ref>(2004) [http://guidance.nice.org.uk/CG10/Guidance/pdf/English CG10 Type 2 diabetes - footcare]. National Institute for Health and Clinical Excellence</ref><br/>
{{main|Diabetic foot}}
[[Physical examination]] of patients’ feet:
* testing of foot sensation using a 10 g monofilament or vibration
* palpation of foot pulses
* inspection of any foot deformity and footwear
 
Although NICE and others<ref name="pmid15644549">{{cite journal| author=Singh N, Armstrong DG, Lipsky BA| title=Preventing foot ulcers in patients with diabetes. | journal=JAMA | year= 2005 | volume= 293 | issue= 2 | pages= 217-28 | pmid=15644549
| url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&retmode=ref&cmd=prlinks&id=15644549 | doi=10.1001/jama.293.2.217 }} <!--Formatted by http://sumsearch.uthscsa.edu/cite/--></ref> have recommended monofilament testing, its role in the major [[randomized controlled trial]] is not clear.<ref name="pmid8498761">{{cite journal| author=Litzelman DK, Slemenda CW, Langefeld CD, Hays LM, Welch MA, Bild DE et al.| title=Reduction of lower extremity clinical abnormalities in patients with non-insulin-dependent diabetes mellitus. A randomized, controlled trial. | journal=Ann Intern Med | year= 1993 | volume= 119 | issue= 1 | pages= 36-41 | pmid=8498761
| url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&retmode=ref&cmd=prlinks&id=8498761 }} <!--Formatted by http://sumsearch.uthscsa.edu/cite/--></ref>
 
{{Image|Footscreensites-rgb.jpg|right|350px|Monofilament testing for diabetic neuropathy using preferred testing locations colored green.<ref name="pmid19595541">{{cite journal| author=Feng Y, Schlösser FJ, Sumpio BE| title=The Semmes Weinstein monofilament examination as a screening tool for diabetic peripheral neuropathy. | journal=J Vasc Surg | year= 2009 | volume= 50 | issue= 3 | pages= 675-82, 682.e1 | pmid=19595541
| url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&retmode=ref&cmd=prlinks&id=19595541 | doi=10.1016/j.jvs.2009.05.017 }} <!--Formatted by http://sumsearch.uthscsa.edu/cite/--></ref>}}
 
If screening with the monofilament is done, a three site test of the plantar surfaces of the great toe, the third metatarsal, and the fifth metatarsalsis is adequate according to a [[systematic review]]<ref name="pmid19595541">{{cite journal| author=Feng Y, Schlösser FJ, Sumpio BE| title=The Semmes Weinstein monofilament examination as a screening tool for diabetic peripheral neuropathy. | journal=J Vasc Surg | year= 2009 | volume= 50 | issue= 3 | pages= 675-82, 682.e1 | pmid=19595541
| url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&retmode=ref&cmd=prlinks&id=19595541 | doi=10.1016/j.jvs.2009.05.017 }} <!--Formatted by http://sumsearch.uthscsa.edu/cite/--></ref> of studies<ref name="pmid10417599">{{cite journal| author=Smieja M, Hunt DL, Edelman D, Etchells E, Cornuz J, Simel DL| title=Clinical examination for the detection of protective sensation in the feet of diabetic patients. International Cooperative Group for Clinical Examination Research. | journal=J Gen Intern Med | year= 1999 | volume= 14 | issue= 7 | pages= 418-24 | pmid=10417599
| url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&retmode=ref&cmd=prlinks&id=10417599 | pmc=PMC1496604 }} <!--Formatted by http://sumsearch.uthscsa.edu/cite/--></ref>. Another [[systemic review]] questions the test accuracy of the monofilament exam.<ref name="pmid19901316">{{cite journal| author=Dros J, Wewerinke A, Bindels PJ, van Weert HC| title=Accuracy of monofilament testing to diagnose peripheral neuropathy: a systematic review. | journal=Ann Fam Med | year= 2009 Nov-Dec | volume= 7 | issue= 6 | pages= 555-8 | pmid=19901316
| url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=clinical.uthscsa.edu/cite&email=badgett@uthscdsa.edu&retmode=ref&cmd=prlinks&id=19901316 | doi=10.1370/afm.1016 | pmc=PMC2775618 }} <!--Formatted by http://sumsearch.uthscsa.edu/cite/--></ref>


==Treatment==
==Treatment==
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[[SSRI]]s include [[fluoxetine]], [[paroxetine]], [[sertraline]] and [[citalopram]]. They are less effective that TCAs in relieving pain, but are better tolerated. Side effects are rarely serious, and do not cause any permanent disabilities. They cause sedation and weight gain, which can worsen a diabetic's glycemic control. They can be used at dosages that also relieve the symptoms of [[clinical depression|depression]], a common concommitent of diabetic neuropathy.
[[SSRI]]s include [[fluoxetine]], [[paroxetine]], [[sertraline]] and [[citalopram]]. They are less effective that TCAs in relieving pain, but are better tolerated. Side effects are rarely serious, and do not cause any permanent disabilities. They cause sedation and weight gain, which can worsen a diabetic's glycemic control. They can be used at dosages that also relieve the symptoms of [[clinical depression|depression]], a common concommitent of diabetic neuropathy.


The [[SSNRI]] [[duloxetine]] (Cymbalta) is approved for diabetic neuropathy. By targeting both serotonin and norepinephrine, it targets the painful symptoms of diabetic neuropathy, and also treats depression if it exists. Typical dosages are between 60mg and 120mg.
The [[SSNRI]] [[duloxetine]] (Cymbalta) is approved for diabetic neuropathy, but is not better than TCAs.<ref name="pmid22991449">{{cite journal| author=Boyle J, Eriksson ME, Gribble L, Gouni R, Johnsen S, Coppini DV et al.| title=Randomized, Placebo-Controlled Comparison of Amitriptyline, Duloxetine, and Pregabalin in Patients With Chronic Diabetic Peripheral Neuropathic Pain: Impact on pain, polysomnographic sleep, daytime functioning, and quality of life. | journal=Diabetes Care | year= 2012 | volume= 35 | issue= 12 | pages= 2451-8 | pmid=22991449 | doi=10.2337/dc12-0656 | pmc=PMC3507552 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=22991449  }} </ref> By targeting both serotonin and norepinephrine, it targets the painful symptoms of diabetic neuropathy, and also treats depression if it exists. Typical dosages are between 60mg and 120mg.


===Anticonvulsants===
===Anticonvulsants===
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[[α-lipoic acid]], an [[anti-oxidant]] that is a non-prescription dietary supplement has shown benefit in a [[randomized controlled trial]] that compared once-daily oral doses of 600 mg to 1800 mg compared to [[placebo]], although nausea occurred in the higher doses.<ref name="pmid17065669">{{cite journal |author=Ziegler D, Ametov A, Barinov A, ''et al'' |title=Oral treatment with alpha-lipoic acid improves symptomatic diabetic polyneuropathy: the SYDNEY 2 trial |journal=Diabetes Care |volume=29 |issue=11 |pages=2365-70 |year=2006 |pmid=17065669 |doi=10.2337/dc06-1216}}</ref>
[[α-lipoic acid]], an [[anti-oxidant]] that is a non-prescription dietary supplement has shown benefit in a [[randomized controlled trial]] that compared once-daily oral doses of 600 mg to 1800 mg compared to [[placebo]], although nausea occurred in the higher doses.<ref name="pmid17065669">{{cite journal |author=Ziegler D, Ametov A, Barinov A, ''et al'' |title=Oral treatment with alpha-lipoic acid improves symptomatic diabetic polyneuropathy: the SYDNEY 2 trial |journal=Diabetes Care |volume=29 |issue=11 |pages=2365-70 |year=2006 |pmid=17065669 |doi=10.2337/dc06-1216}}</ref>


In addition to pharmacological treatment there are several other modalities that help some cases. While lacking double blind trials, these have shown to reduce pain and improve patient quality of life particularly for chronic neuropathic pain: Interferential Stimulation; Acupuncture; Meditation; Cognitive Therapy; and prescribed exercise. In more recent years, Photo Energy Therapy devices are becoming more widely used to treat neuropathic symptoms. Photo Energy Therapy devices emit near infrared light typically at a wavelength of 890nm. This wavelength is is believed to stimulate the release of [[Nitric Oxide]], an [[Endothelium-derived relaxing factor ]] into the bloodstream, thus vasodilating the capilaries and venuoles in the microcirculatory system. This increase in circulation has been shown effective in various clinical studies to decrease pain and improve sensation in diabetic and non-diabetic patients. Photo Energy Therapy devices seem to address the underlying problem of neuropathies, poor [[microcirculation]], which leads to pain and numbness in the extremities[http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=pubmed&dopt=Abstract&list_uids=14693984 4], [http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=pubmed&dopt=Abstract&list_uids=15251618 5].
In addition to pharmacological treatment there are several other modalities that help some cases. While lacking double blind trials, these have shown to reduce pain and improve patient quality of life particularly for chronic neuropathic pain: Interferential Stimulation; Acupuncture; Meditation; Cognitive Therapy; and prescribed exercise. In more recent years, Photo Energy Therapy devices are becoming more widely used to treat neuropathic symptoms. Photo Energy Therapy devices emit near infrared light typically at a wavelength of 890nm. This wavelength is believed to stimulate the release of [[nitric oxide]], or [[endothelium-derived relaxing factor ]] into the bloodstream, thus vasodilating the capilaries and venuoles in the microcirculatory system. This increase in circulation has been shown effective in various clinical studies to decrease pain and improve sensation in diabetic and non-diabetic patients. Photo Energy Therapy devices seem to address the underlying problem of neuropathies, poor [[microcirculation]], which leads to pain and numbness in the extremities[http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=pubmed&dopt=Abstract&list_uids=14693984 4], [http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=pubmed&dopt=Abstract&list_uids=15251618 5].


While it is quite true that recognized treatment modalities backed up by double blind trials do not address the underlying causality of diabetic neuropathy, two other programs have had substantial although still anecdotal results. The first involves a program of nutritional supplements put forth in an Internet article researched and published by diabetic neuropathy patients themselves (although heavily referencing peer-reviewed research articles). This article is entitled "A Multidisciplinary Approach to Diabetic Neuropathy Treatment" and its treatment regimen has been instrumental in substantial reversal in individuals throughout the world.<ref>{{cite web |url=http://www.geocities.com/bsy53/dn/neuropat.html |title=A MULTIDISCIPLINARY APPROACH TO DIABETIC NEUROPATHY TREATMENT |accessdate=2007-07-25 |format= |work=}}</ref>
While it is quite true that recognized treatment modalities backed up by double blind trials do not address the underlying causality of diabetic neuropathy, two other programs have had substantial although still anecdotal results. The first involves a program of nutritional supplements put forth in an Internet article researched and published by diabetic neuropathy patients themselves (although heavily referencing peer-reviewed research articles). This article is entitled "A Multidisciplinary Approach to Diabetic Neuropathy Treatment" and its treatment regimen has been instrumental in substantial reversal in individuals throughout the world.<ref>{{cite web |url=http://www.geocities.com/bsy53/dn/neuropat.html |title=A MULTIDISCIPLINARY APPROACH TO DIABETIC NEUROPATHY TREATMENT |accessdate=2007-07-25 |format= |work=}}</ref>
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==References==
==References==
<references/>
{{reflist|2}}[[Category:Suggestion Bot Tag]]
 
==External links==
*[http://health.groups.yahoo.com/group/Neuropathy_Treatment_Testemonials/ Join a Neuropathy Support Group on Yahoo!]
*[http://www.diabetesincontrol.com/annodyne/burkeseries.php Nitric Oxide and its Role in Diabetes, Wound Healing and Peripheral Neuropathy]
*[http://www.nlm.nih.gov/medlineplus/diabeticnerveproblems.html Diabetic Nerve Problems]. MedlinePlus' extensive reference list of pertinent sites.
* [http://www.nlm.nih.gov/medlineplus/ency/article/000693.htm Diabetic Neuropathy]. Medical Encyclopedia, Medline Plus (US government public domain site, partially used here)
*[http://www.medscape.com/viewarticle/467524_3 Diabetic Neuropathy: An Intensive Review] in Medscape from WebMD (partially used in summarized form).
*[http://www.medscape.com/viewprogram/705 Diabetic Polyneuropathy] in Medscape from WebMD (partially used in summarized form).
*[http://diabetes.niddk.nih.gov/ National Diabetes Information Clearinghouse]
{{Endocrine pathology}}

Latest revision as of 16:00, 6 August 2024

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Diabetic neuropathy
ICD-10 E10.4, E11.4, E12.4, E13.4, E14.4
ICD-9 250.6

Diabetic neuropathies are neuropathic disorders that are associated with diabetes mellitus. These conditions are thought to result from diabetic microvascular injury involving small blood vessels that supply nerves (vasa nervorum). Relatively common conditions which may be associated with diabetic neuropathy include third nerve palsy; mononeuropathy; mononeuropathy multiplex; diabetic amyotrophy; a painful polyneuropathy; autonomic neuropathy; and thoracoabdominal neuropathy.

Epidemiology

In developed countries, diabetes mellitus is the leading known[1] cause of neuropathy , and neuropathy is the most common complication and greatest source of morbidity and mortality in diabetes patients. It is estimated that the prevalence of neuropathy in diabetes patients is approximately 20%. Diabetic neuropathy is implicated in 50-75% of nontraumatic amputations.

The main risk factor for diabetic neuropathy is hyperglycemia. In the DCCT (Diabetes Control and Complications Trial, 1995) study, the annual incidence of neuropathy was 2% per year, but dropped to 0.56% with intensive treatment of Type 1 diabetics. The progression of neuropathy is dependent on the degree of glycemic control in both Type 1 and Type 2 diabetes. Duration of diabetes, age, cigarette smoking, hypertension, height and hyperlipidemia are also risk factors for diabetic neuropathy.

Pathology and pathogenesis

There are four factors thought to be involved in the development of diabetic neuropathy:

  1. Microvascular disease,
  2. Advanced Glycation Endproduct,
  3. Protein kinase C, and the
  4. Polyol pathway.

Microvascular disease

Vascular and neural diseases are closely related and intertwined. Blood vessels depend on normal nerve function, and nerves depend on adequate blood flow. The first pathological change in the microvasculature is vasoconstriction. As the disease progresses, neuronal dysfunction correlates closely with the development of vascular abnormalities, such as capillary basement membrane thickening and endothelial hyperplasia, which contribute to diminished oxygen tension and hypoxia. Neuronal ischemia is a well-established characteristic of diabetic neuropathy. Vasodilator agents (e.g., angiotensin-converting-enzyme inhibitors, α1-antagonists) can lead to substantial improvements in neuronal blood flow, with corresponding improvements in nerve conduction velocities. Thus, microvascular dysfunction occurs early in diabetes, parallels the progression of neural dysfunction, and may be sufficient to support the severity of structural, functional, and clinical changes observed in diabetic neuropathy.

Advanced glycated end products

Elevated intracellular levels of glucose cause a non-enzymatic covalent bonding with proteins, which alters their structure and destroys their function. Certain of these glycosylated proteins are implicated in the pathology of diabetic neuropathy and other long term complications of diabetes.

Protein kinase C (PKC)

PKC is implicated in the pathology of diabetic neuropathy. Increased levels of glucose cause an increase in intracellular diacylglycerol, which activates PKC. PKC inhibitors in animal models will increase nerve conduction velocity by increasing neuronal blood flow.

Polyol pathway

Also called the Sorbitol/Aldose Reductase Pathway, the Polyol Pathway may be implicated in diabetic complications that result in microvascular damage to nervous tissue, and also to the retina and kidney which also have lots of microvasculature themselves.

Glucose is a highly reactive compound, and it must be metabolized or it will find tissues in the body to react with. Increased glucose levels, like those seen in Diabetes, activates this alternative biochemical pathway, which in turn causes a decrease in glutathione and an increase in reactive oxygen radicals. The pathway is dependent on the enzyme aldose reductase. Inhibitors of this enzyme have demonstrated efficacy in animal models in preventing the development of neuropathy.

While most body cells require the action of insulin for glucose to gain entry into the cell, the cells of the retina, kidney and nervous tissues are insulin-independent. Therefore there is a free interchange of glucose from inside to outside of the cell, regardless of the action of insulin, in the eye, kidney and neurons. The cells will use glucose for energy as normal, and any glucose not used for energy will enter the polyol pathway and be converted into sorbitol. Under normal blood glucose levels, this interchange will cause no problems, as aldose reductase has a low affinity for glucose at normal concentrations.

However, in a hyperglycemic state (Diabetes), the affinity of aldose reductase for glucose rises, meaning much higher levels of sorbitol and much lower levels of NADPH, a compound used up when this pathway is activated. The sorbitol can not cross cell membranes, and when it accumulates, it produces osmotic stresses on cells by drawing water into the cell. Fructose does essentially the same thing, and it is created even further on in the chemical pathway.

The NADPH, used up when the pathway is activated, acts to promote nitric oxide and glutathione production, and its conversion during the pathway leads to reactive oxygen molecules. Glutathione deficiencies can lead to hemolysis caused by oxidative stress, and we already know that nitric oxide is one of the important vasodilators in blood vessels. NAD+, which is also used up, is necessary to keep reactive oxygen species from forming and damaging cells.

In summary, excessive activation of the Polyol pathway leads to increased levels of sorbitol and reactive oxygen molecules and decreased levels of nitric oxide and glutathione, as well as increased osmotic stresses on the cell membrane. Any one of these elements alone can promote cell damage, but here we have several acting together.

Experimental evidence has yet to confirm that the polyol pathway actually is responsible for microvasculature damage in the retina, kidney and/or neurons of the body. However, physiologists are fairly certain that it plays some role in neuropathy.

Clinical manifestations

Diabetic neuropathy affects all peripheral nerves: pain fibers, motor neurons, autonomic nerves. It therefore necessarily can affect all organs and systems since all are innervated. There are several distinct syndromes based on the organ systems and members affected, but these are by no means exclusive. A patient can have sensorimotor and autonomic neuropathy or any other combination. Symptoms vary depending on the nerve(s) affected and may include symptoms other than those listed. Symptoms usually develop gradually over years.

Usual symptoms may be:

Sensorimotor polyneuropathy

Longer nerve fibers are affected to a greater degree than shorter ones, because nerve conduction velocity is slowed in proportion to a nerve's length. In this syndrome, decreased sensation and loss of reflexes occurs first in the toes bilaterally, then extends upward. It is usually described as glove-stocking distribution of numbness, sensory loss, dysesthesia and nighttime pain. The pain can feel like burning, pricking sensation, achy or dull. Pins and needles sensation is common. Loss of proprioception, that is, the sense of where a limb is in space, is affected early. These patients cannot feel when they are stepping on a foreign body, like a splinter, or when they are developing a callous from an ill-fitting shoe.

These patients are at risk for developing diabetic foot and foot ulcers and infections on the feet and legs, which can lead to amputation. Similarly, these patients can get multiple fractures of the knee, ankle or foot, and develop a Charcot joint. Loss of motor function results in dorsiflexion contractures of the toes, loss of the interosseous muscle function and leads to contraction of the digits, so called hammer toes. These contractures occur not only in the foot but also in the hand where the loss of the musculature makes the hand appear gaunt and skeletal. The loss of muscular function is progressive.

Autonomic neuropathy

The autonomic nervous system is composed of nerves serving the heart, gastrointestinal system and urinary-genital system. Autonomic neuropathy can affect any of these organ systems. The most commonly recognized autonomic dysfunction in diabetics is orthostatic hypotension, or the uncomfortable sensation of fainting when a patient stands up. In the case of diabetic autonomic neuropathy, it is due to the failure of the heart and arteries to appropriately adjust heart rate and vascular tone to keep blood continually and fully flowing to the brain[failure of the sensitivity of the baroreceptors]. This symptom is usually accompanied by a loss of sinus respiratory variation, that is, the usual change in heart rate seen with normal breathing. When these 2 findings are present, cardiac autonomic neuropathy is present.

GI tract manifestations include delayed gastric emptying, gastroparesis, nausea, bloating, and diarrhea. Because many diabetics take oral medication for their diabetes, absorption of these medicines is greatly affected by the delayed gastric emptying. This can lead to hypoglycemia when an oral diabetic agent is taken before a meal and does not get absorbed until hours, or sometimes days later, when there is normal or low blood sugar already. Sluggish movement of the small intestine can cause bacterial overgrowth, made worse by the presence of hyperglycemia. This leads to bloating, gas and diarrhea.

Urinary symptoms include urinary frequency, urgency, incontinence and retention. Again, because of the retention of sweet urine, urinary tract infections are frequent. Urinary retention can lead to bladder diverticula, stones, reflux nephropathy.

Cranial neuropathy

When cranial nerves are affected, oculomotor (3rd) neuropathies are most common. The oculomotor nerve controls all of the muscles that move the eye with the exception of the lateral rectus and superior oblique muscles. It also serves to constrict the pupil and open the eyelid. The onset of a diabetic third nerve palsy is usually abrupt, beginning with frontal or periorbital pain and then diplopia. All of the oculomotor muscles innervated by the third nerve may be affected, except for those that control pupil size. This is because pupillary function within CNIII is found on the periphery of the nerve (in terms of a cross sectional view), which makes it less susceptible to ischemic damage (as it is closer to the vascular supply). The sixth nerve, the abducens nerve, which innervates the lateral rectus muscle of the eye (moves the eye laterally), is also commonly affected but fourth nerve, the trochlear nerve, (innervates the superior oblique muscle, which moves the eye downward) involvement is unusual. Mononeuropathies of the thoracic or lumbar spinal nerves can occur and lead to painful syndromes that mimic myocardial infarction, cholecystitis or appendicitis. Diabetics have a higher incidence of entrapment neuropathies, such as carpal tunnel syndrome.

Screening

For more information, see: Diabetic foot.


Treatment

Despite advances in the understanding of the metabolic causes of neuropathy, treatments aimed at interrupting these pathological processes have been limited by side effects and lack of efficacy. Thus, with the exception of tight glucose control, treatments are for reducing pain and other symptoms and do not address the underlying problems.

Agents for pain control include tricyclic antidepressants (TCAs), serotonin reuptake inhibitors (SSRIs) and antiepileptic drugs (AEDs). A systematic review concluded that "tricyclic antidepressants and traditional anticonvulsants are better for short term pain relief than newer generation anticonvulsants." [2]

Tight glucose control

Treatment of early manifestations of sensorimotor polyneuropathy involves improving glycemic control.[3] Tight control of blood glucose can reverse the changes of diabetic neuropathy, but only if the neuropathy and diabetes is recent in onset. Conversely, painful symptoms of neuropathy in uncontrolled diabetics tend to subside as the disease and numbness progress. Of course, these uncontrolled patients are at great risk for diabetic foot ulcers and amputation because of neuropathy.

Tricyclic antidepressants

TCAs include imipramine, amitriptyline, desipramine and nortriptyline. These drugs are effective at decreasing painful symptoms but suffer from multiple side effects that are dosage dependent. One notable side effect is cardiac toxicity, which can lead to fatal arrhythmias. At low dosages used for neuropathy, toxicity is rare, but if symptoms warrant higher doses, complications are more common. Among the TCAs, amitriptyline is most widely used for this condition, but desipramine and nortriptyline have fewer side effects.

In a randomized controlled trial of patients with diabetic neuropathy, amitriptyline was better than fluoxetine [4] In this trial, amitriptyline was effective in patients regardless of whether they had depression, whereas fluoxetine was effective only in depressed patients.

In a randomized crossover trial of patients with diabetic neuropathy, amitriptyline provided moderate or greater pain relief in 67% of patients as compared to 52% with gabapentin. In this small study, this result was statistically insignificant.[5]

Serotonin reuptake inhibitor

SSRIs include fluoxetine, paroxetine, sertraline and citalopram. They are less effective that TCAs in relieving pain, but are better tolerated. Side effects are rarely serious, and do not cause any permanent disabilities. They cause sedation and weight gain, which can worsen a diabetic's glycemic control. They can be used at dosages that also relieve the symptoms of depression, a common concommitent of diabetic neuropathy.

The SSNRI duloxetine (Cymbalta) is approved for diabetic neuropathy, but is not better than TCAs.[6] By targeting both serotonin and norepinephrine, it targets the painful symptoms of diabetic neuropathy, and also treats depression if it exists. Typical dosages are between 60mg and 120mg.

Anticonvulsants

Anticonvulsants, especially gabapentin and the related pregabalin, are options.

Gabapentin is similar to amitriptyline in terms of efficacy, and may be safer. Its main side effect is sedation, which does not diminish over time and may in fact worsen. It needs to be taken three times a day, and it sometimes causes weight gain, which can worsen glycemic control in diabetics.

Carbamazepine (Tegretol®) is effective but not necessarily safe for diabetic neuropathy. Its first metabolite, oxcarbazepine, is both safe and effective in other neuropathic disorders, but has not been studied in diabetic neuropathy.

Pregabalin has similar effectiveness to amitriptyline but causes less sedation.[7]

Topiramate has not been studied in diabetic neuropathy, but has the beneficial side effect of causing mild anorexia and weight loss, and is anecdotally beneficial.

Other treatments

Methylcobalamin, a special form of Vitamin B12, is being studied now for treatment of neuropathy, both injected and oral. Initial studies[1] and anecdotal evidence in cats[2] have been very encouraging.[3]. A systematic review of randomized controlled trials suggested benefit, but the trials were not of good quality and the possibility of publication bias exists.[8]

α-lipoic acid, an anti-oxidant that is a non-prescription dietary supplement has shown benefit in a randomized controlled trial that compared once-daily oral doses of 600 mg to 1800 mg compared to placebo, although nausea occurred in the higher doses.[9]

In addition to pharmacological treatment there are several other modalities that help some cases. While lacking double blind trials, these have shown to reduce pain and improve patient quality of life particularly for chronic neuropathic pain: Interferential Stimulation; Acupuncture; Meditation; Cognitive Therapy; and prescribed exercise. In more recent years, Photo Energy Therapy devices are becoming more widely used to treat neuropathic symptoms. Photo Energy Therapy devices emit near infrared light typically at a wavelength of 890nm. This wavelength is believed to stimulate the release of nitric oxide, or endothelium-derived relaxing factor into the bloodstream, thus vasodilating the capilaries and venuoles in the microcirculatory system. This increase in circulation has been shown effective in various clinical studies to decrease pain and improve sensation in diabetic and non-diabetic patients. Photo Energy Therapy devices seem to address the underlying problem of neuropathies, poor microcirculation, which leads to pain and numbness in the extremities4, 5.

While it is quite true that recognized treatment modalities backed up by double blind trials do not address the underlying causality of diabetic neuropathy, two other programs have had substantial although still anecdotal results. The first involves a program of nutritional supplements put forth in an Internet article researched and published by diabetic neuropathy patients themselves (although heavily referencing peer-reviewed research articles). This article is entitled "A Multidisciplinary Approach to Diabetic Neuropathy Treatment" and its treatment regimen has been instrumental in substantial reversal in individuals throughout the world.[10]

The second method involves a combination of a vegan diet combined with moderate walking exercise. It has been used over several decades to affect both Type II diabetes as well as diabetic peripheral neuropathy.

Prognosis

The mechanisms of diabetic neuropathy are poorly understood. At present, treatment alleviates pain and can control some associated symptoms, but the process is generally progressive.

As a complication, there is an increased risk of injury to the feet because of loss of sensation (see diabetic foot). Small infections can progress to ulceration (skin and soft tissue breakdown) and this may require amputation. In addition, motor nerve damage can lead to muscle breakdown and imbalance.

References

  1. The largest group of neuropathy patients are of unknown cause, referred to as idiopathic in origin. Of the roughly 100 known causes, diabetes is by far the largest. Other known causes include genetic factors, damaging chemical agents such as chemotherapy drugs, and HIV.
  2. Wong MC, Chung JW, Wong TK (2007). "Effects of treatments for symptoms of painful diabetic neuropathy: systematic review". BMJ 335 (7610): 87. DOI:10.1136/bmj.39213.565972.AE. PMID 17562735. Research Blogging.
  3. (1995) "The effect of intensive diabetes therapy on the development and progression of neuropathy. The Diabetes Control and Complications Trial Research Group". Ann. Intern. Med. 122 (8): 561-8. PMID 7887548[e]
  4. Max MB, Lynch SA, Muir J, Shoaf SE, Smoller B, Dubner R (May 1992). "Effects of desipramine, amitriptyline, and fluoxetine on pain in diabetic neuropathy". N. Engl. J. Med. 326 (19): 1250–6. PMID 1560801[e]
  5. Morello CM, Leckband SG, Stoner CP, Moorhouse DF, Sahagian GA (September 1999). "Randomized double-blind study comparing the efficacy of gabapentin with amitriptyline on diabetic peripheral neuropathy pain". Arch. Intern. Med. 159 (16): 1931–7. PMID 10493324[e]
  6. Boyle J, Eriksson ME, Gribble L, Gouni R, Johnsen S, Coppini DV et al. (2012). "Randomized, Placebo-Controlled Comparison of Amitriptyline, Duloxetine, and Pregabalin in Patients With Chronic Diabetic Peripheral Neuropathic Pain: Impact on pain, polysomnographic sleep, daytime functioning, and quality of life.". Diabetes Care 35 (12): 2451-8. DOI:10.2337/dc12-0656. PMID 22991449. PMC PMC3507552. Research Blogging.
  7. Bansal D, Bhansali A, Hota D, Chakrabarti A, Dutta P (2009). "Amitriptyline vs. pregabalin in painful diabetic neuropathy: a randomized double blind clinical trial.". Diabet Med 26 (10): 1019-26. DOI:10.1111/j.1464-5491.2009.02806.x. PMID 19900234. Research Blogging.
  8. Sun Y, Lai MS, Lu CJ (2005). "Effectiveness of vitamin B12 on diabetic neuropathy: systematic review of clinical controlled trials". Acta neurologica Taiwanica 14 (2): 48-54. PMID 16008162[e]
  9. Ziegler D, Ametov A, Barinov A, et al (2006). "Oral treatment with alpha-lipoic acid improves symptomatic diabetic polyneuropathy: the SYDNEY 2 trial". Diabetes Care 29 (11): 2365-70. DOI:10.2337/dc06-1216. PMID 17065669. Research Blogging.
  10. A MULTIDISCIPLINARY APPROACH TO DIABETIC NEUROPATHY TREATMENT. Retrieved on 2007-07-25.