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Protein energy malnutrition

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] ; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Synonyms and keywords: Edematous malnutrition; Protein malnutrition; Protein-calorie malnutrition; Malignant malnutrition; Kwashiorkor; Marasmus; Severe acute malnutrition; Protien energy malnutrition

Overview

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Overview

Protein energy malnutrition is defined by measurements that fall below 2 standard deviations under the normal weight for age (underweight), height for age (stunting) and weight for height (wasting). Protein energy malnutrition is a nutritional deficiency resulting from either inadequate energy (caloric) or protein intake and manifesting as either marasmus or kwashiorkor. Marasmus is characterized by wasting of body tissues, particularly muscles and subcutaneous fat, and is usually a result of severe restrictions in energy intake. Kwashiorkor affects mainly children, is characterized by edema (particularly ascites), and is usually the result of severe restrictions in protein intake. However, both types can be present simultaneously (marasmic-kwashiokor) and mask malnutrition due to the presence of edema. Treatment involves prompt resuscitation, identification of co-morbidities like dehydration and infections. The presence of severe of hypoproteinemia, hypoalbuminemia, electrolyte imbalance or an underlying HIV infection is associated with poorer prognosis among patients with protein energy malnutrition.

Historical Perspective

The first clinical description of protein-energy malnutrition was made in 1865 in Spanish language which led to little dissemination of the information. In 1932, kwashiorkor was first described by Dr. Cicely Williams, working with African children on the Gold Coast. The word kwashiorkor comes from the Ga language of Accra, Ghana meaning the ‘diseaseof the deposed baby when the next one is born’. The term marasmus is derived from the Greek word ‘marasmos‘, which means withering or wasting.

Classification

Protein energy malnutrition may be classified according to the ‘Gomez classification’ based on weight for age, or the ‘Waterlow classification’ based on stunting and wasting, or the ‘Welcome classification’ based on the presence or absence of edema.

Pathophysiology

Protein-energy malnutrition represents a shift of the body from fed to fasting/starvation state. Starvation leads to a decreased basal plasma insulin concentration and in decrease of glucose-stimulated insulin secretion. Prolonged fasting results in a deficiency in amino acids used for gluconeogenesis. It is thought that kwashiorkor is produced by a deficiency in the adequate consumption of protein-rich foods during the weaning process. However, the associated edema is not fully understood. Several theories have been put forward to explain this finding. Marasmus on the other hand is thought to be due to the total caloric deficiency leading to wastingin a child. Marasmus always results from a negative energy balance.

Causes

Protein energy malnutrition may be caused by reduced breast feedingpoor weaning practices, limited availability of food and inadequate child care in cases of extreme poverty. This classically affects several poor people in regions of poor social and economic background. Other environmental causes such as infections, drought and earthquakes leading to decreased availability of food have also been identified.

Differentiating Kwashiorkor from other Diseases

Protein-energy malnutrition must be differentiated from other diseases that cause failure to thriveedemawasting recurrent infectionsskin and hair changes. It is important to also differentiate kwashiorkor from marasmus as the two diseases are casued by protein- energy malnutrition and share similar features such as, weight loss, muscle wasting, low blood glucose levels and growth retardation.

Epidemiology and Demographics

The prevalence of protein-energy malnutrition in children under 5 is estimated to be 150 million cases annually. In Nigeria, the prevalence is as high as 41,600 per 100,000 children. Protein-energy malnutrition is majorly a disease of the developing countries. There is no racial or sexual predisposition.

Risk Factors

Common risk factors in the development of protein-energy malnutrition may be classified as maternal and environmental.

Screening

There is insufficient evidence to recommend routine screening for protein-energy malnutrition.

Natural History, Complications and Prognosis

If left untreated, all children with protein energy malnutrition will progress to develop permanent stunting (height for age), poorly developed immune system which causes overwhelming bacteremia and sepsis which is the cause of death in most malnourished individuals.

Diagnosis

History and Symptoms

The history of protein-energy malnutrition includes a failure to thrive in children under 1 year of age especially after they have just been weaned of breast milk. Some common signs and symptoms include failure to thrivefatigueirritability, changes in skin and hair pigmentdecreased muscle massdiarrhea, increased occurrence of severe infectionsdue to damaged immune systemedema and hepatomegaly.

Physical Examination

Physical examination of patients with kwashiorkor is usually remarkable for rounded prominence of the cheeks known as the moon face, and distended abdomen due to an enlarged liverhyperkeratosis and hyperpigmentation of the skingeneralized edema especially on the dependent areas of the body like the feet. On the other hand, patients with marasmus usually look listlessemaciated with monkey-like faces due to absence of subcutaneous fat pad in the cheeks. The skin looks atrophic and dry.

Laboratory Findings

There are no specific laboratory tests, group of tests, or indices that are satisfactory for the assessment of protein-energy malnutrition. However, laboratory findings that may aid in the diagnosis of protein-energy malnutrition include abnormally low blood glucosehypoalbuminemia (10-25 g/L), hypoproteinemia (transferrinessential amino acidslipoprotein) and hypoglycemia.

X ray

There are no chest X ray findings associated with protein energy malnutrition.

CT

There are no CT scan findings associated with protein energy malnutrition.

MRI

There are no MRI findings associated with protein energy malnutrition. However, a MRI may be helpful in the diagnosis of complications of protein-energy malnutrition which include cerebral atrophy and ventricular dilation.

Echocardiography or Ultrasound

Echocardiography findings may be helpful in the diagnosis of protein-energy malnutrition. Findings on an echocardiography suggestive of protein-energy malnutrition include decrease of R wave and QTc interval, decreased cardiac index which improved significantly after rehabilitation.

Other Imaging Findings

There are no other imaging findings associated with protein-energy malnutrition.

Other Diagnostic Studies

There are several parameters that can be used in the assessment of a child with protein-energy malnutrition. Malnutrition can be assessed according to the WHO based on mid upper arm circumference into moderate and severe malnutrition. Other parameters include the Z-score which assesses linear growth and weight for length.

Treatment

Medical Therapy

In some cases, protein-energy malnutrition may be complicated by dehydration and specific infections, such as pneumonia and septicemia. In such cases, protein-energy malnutrition is a is a medical emergency and requires prompt treatment with antibiotics.

Surgery

Surgical intervention is not recommended for the management of protein-energy malnutrition.

Primary Prevention

To prevent kwashiorkor, make sure the diet has enough carbohydrates, fat (at least 10% of total calories), and protein (12% of total calories).

Secondary Prevention

The secondary prevention of protein-energy malnutrition is the same as primary prevention.

References

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Patient information

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Overview

What causes protein energy malnutrition

What are the symptoms of protein energy malnutrition

Diagnosis

Treatment options

Possible complications

When to contact a medical professional

Prevention

Alternative names

Historical Perspective

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Overview

The first clinical description of protein-energy malnutrition was made in 1865 in Spanish language which led to little dissemination of the information. In 1932, kwashiorkor was first described by Dr. Cicely Williams, working with African children on the Gold Coast. The word kwashiorkor comes from the Ga language of Accra, Ghana meaning the ‘disease of the deposed baby when the next one is born’. The term marasmus is derived from the Greek word ‘marasmos‘, which means withering or wasting.

Historical Perspective

  • Prior to 1959, the term protein-energy malnutrition (PEM), or protein-calorie malnutrition was attributed principally to dietary deficiency and therefore it could be prevented or treated by dietary measures alone.[1]
  • The disease called kwashiorkor in the “Ga” language of Accra, Ghana means ‘the disease of the deposed baby’. The term signifies sickness an elder child may suffer from when a younger one is born.[2]
  • In 1932, kwashiorkor was first described by Dr. Cicely Williams, while working with African children on the Gold Coast.[3]
  • Williams identified a relationship between the low-protein maize diet of the children and the occurrence of the protein-energy malnutrition.[3]
  • In 1933, kwashiorkor was first described in the classic way as a ‘well-marked syndrome of the deposed infant’ in the literature.[4]
  • In the 1950s kwashiorkor became a major topic of debate in medicine, in South Africa and also in the international arena.
  • In 1970s, nutritionists were the first to focus on the development of high protein foods for weaning the disease.
  • The term marasmus is a derivative of the ‘marasmos‘, a Greek word. This ancient word means withering or wasting, that is thought to be used for the same conditions in ancient Greek.[5]

References

  1. Keusch GT (2003). “The history of nutrition: malnutrition, infection and immunity”. J. Nutr. 133 (1): 336S–340S. PMID 12514322.
  2. “Feeding practices and malnutrition at the Princess Marie Louise Children’s hospital, Accra: what has changed after 80 years? | BMC Nutrition | Full Text”.
  3. 3.0 3.1 Heikens GT, Manary M (2009). “75 years of Kwashiorkor in Africa”. Malawi Med J. 21 (3): 96–8. PMC 3717488. PMID 20345016.
  4. “Mother and Child Health: Delivering the Services – Cicely D. Williams, Naomi Baumslag, Derrick Brian Jelliffe – Google Books”.
  5. Theoharides TC (1971). “Galen on marasmus”. J Hist Med Allied Sci. 26 (4): 369–90. PMID 4946290.

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Classification

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2], Syed Hassan A. Kazmi BSc, MD [3]

Overview

Protein energy malnutrition may be classified according to the ‘Gomez classification’ based on weight for age, or the ‘Waterlow’s classification’ based on stunting and wasting, or the ‘Welcome classification’ based on the presence or absence of edema.

Classification

The three different classification schemes of protein-energy malnutrition are described below:[1][2]

(i) Gomez classification

General scheme

Definitions of general terms that are used in the classification of protein-energy malnutrition include the following:

Terminology Meaning
Undrweight Underweight for one’s age (Weight for age )
Stunted Too short for one’s age (Height for age )
Wasted Dangerously thin (Weight for height )
Micronutrient malnutrition Deficient in vitamins and minerals (Hidden Hunger )

Grading

Grade of PEM Weight for age (%) General considerations and formula
Normal 90-100
  • Normal reference child is the 50th centile of the Boston standard
  • Weight for age (%) = (Weight of the child / Weight of the normal child of same age ) X100
Mild malnutrition, Grade I 75-89
Moderate malnutrition, Grade II 60-74
Severe malnutrition, Grade III Less than 60

(ii) Waterlow’s classification

General scheme

Feature Basic definition
Stunting Drop in height for age (< 90%)
Wasting Drop in weight for height (<80%)
Under weight Drop in Weight for Age (<80%)

Grading

Grade of PEM Stunting

(low height for age)

Wasting

(low weight for height)

Normal 95 90
Mild malnutrition 87.5-95 80-90
Moderate malnutrition 80-87.5 70-80
Severe malnutrition Less than 80 Less than 70

(iii) Welcome’s classification

Weight for age With edema Without edema General considerations
60-80% Kwashiorkor Undernutrition
  • Weight for age +/- oedema
  • Reference standard (50th percentile)
<60% Marasmic kwashiorkor Marasmus

References

  1. Bhattacharyya AK (1986). “Protein-energy malnutrition (Kwashiorkor-Marasmus syndrome): terminology, classification and evolution”. World Rev Nutr Diet. 47: 80–133. PMID 3088855.
  2. Waterlow JC (1976). “Classification and definition of protein-energy malnutrition”. Monogr Ser World Health Organ (62): 530–55. PMID 824854.

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Pathophysiology

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2], Syed Hassan A. Kazmi BSc, MD [3]

Overview

Protein-energy malnutrition represents a shift of the body from fed to fasting/starvation state. Starvation leads to a decreased basal plasma insulin concentration and in decrease of glucose-stimulated insulin secretion. Prolonged fasting results in a deficiency in amino acids used for gluconeogenesis. It is thought that kwashiorkor is produced by a deficiency in the adequate consumption of protein-rich foods during the weaning process. However, the associated edema is not fully understood. Several theories have been put forward to explain this finding. Marasmus on the other hand is thought to be due to the total caloric deficiency leading to wastingin a child. Marasmus always results from a negative energy balance.

Pathophysiology

Several studies have shown that a deficiency in the consumption of protein, carbohydrates and fat is responsible for the development of protein-energy malnutrition. However, other studies have proposed that chronic infections such as helminthic infections are mainly responsible for the development of protein-energy malnutrition.[1] The underlying mechanisms include the following:

The pathologic changes involved in protein-energy malnutrition include:[2]

Pathogenesis

Hormonal and molecular mechanisms (fed to starvation state)

Insulin and glucagon in starvation

Eventual decreased gluconeogenesis in protein-energy malnutrition

  • Prolonged fasting results in a deficiency in amino acids used for gluconeogenesis.
  • Glucagon concentrations have been found to be lower in children with kwashiorkor compared with marasmus but similar to normal controls.[6]

Malnutrition, Leptin, and Immunity

Pathogenesis of marasmus

Pathogenesis of edema in kwashiorkor

Several theories have been postulated to explain the mechanism of edema seen in children with kwashiorkor. Some of them include:

1. Protein deficiency / hypoalbuminemia

It was initially believed that a deficiency in the consumption of protein was responsible for the development of kwashiorkor in children.

Multiple evidences have now shown that inadequate intake of dietary protein is not the primary trigger for edematous malnutrition.

2. Oxidant stress

3. Microbiome

Genetics

Protein-energy malnutrition is frequently reported in Cri du chat syndrome(CDS), a genetic disease that causes developmental delay and global growth retardation.

Associated conditions

Some of the conditions that are associated with kwashiorkor include:

Gross pathology

Post mortem examination of the liver shows the presence of fatty infiltration and necrosis which disappears with adequate treatment.[18]

Microscopic pathology

Both in kwashiorkor and marasmus hair analysis is therefore advocated as a useful diagnostic procedure for both conditions. In both cases, there is a decrease in the amount of melanin present in the scalp hair.

Kwashiorkor

Marasmus

References

  1. Cederholm T, Jägrén C, Hellström K (1995). “Outcome of protein-energy malnutrition in elderly medical patients”. Am J Med. 98 (1): 67–74. doi:10.1016/S0002-9343(99)80082-5. PMID 7825621.
  2. Lerner AB (1971). “On the etiology of vitiligo and gray hair”. Am J Med. 51 (2): 141–7. PMID 5095523.
  3. Saudek CD, Boulter PR, Arky RA (1973). “The natriuretic effect of glucagon and its role in starvation”. J. Clin. Endocrinol. Metab. 36 (4): 761–5. doi:10.1210/jcem-36-4-761. PMID 4686383.
  4. Hedeskov CJ, Capito K (1974). “The effect of starvation on insulin secretion and glucose metabolism in mouse pancreatic islets”. Biochem. J. 140 (3): 423–33. PMC 1168019. PMID 4155624.
  5. “Wiley: Metabolism at a Glance, 3rd Edition – J. G. Salway”.
  6. “Pediatric Research – Mechanisms Behind Decreased Endogenous Glucose Production in Malnourished Children”.
  7. Scrimshaw NS, SanGiovanni JP (1997). “Synergism of nutrition, infection, and immunity: an overview”. Am. J. Clin. Nutr. 66 (2): 464S–477S. PMID 9250134.
  8. Monk JM, Makinen K, Shrum B, Woodward B (2006). “Blood corticosterone concentration reaches critical illness levels early during acute malnutrition in the weanling mouse”. Exp. Biol. Med. (Maywood). 231 (3): 264–8. PMID 16514171.
  9. Auphan N, Didonato JA, Helmberg A, Rosette C, Karin M (1997). “Immunoregulatory genes and immunosuppression by glucocorticoids”. Arch. Toxicol. Suppl. 19: 87–95. PMID 9079197.
  10. Coulthard MG (2015). “Oedema in kwashiorkor is caused by hypoalbuminaemia”. Paediatr Int Child Health. 35 (2): 83–9. doi:10.1179/2046905514Y.0000000154. PMC 4462841. PMID 25223408.
  11. Golden MH (1998). “Oedematous malnutrition”. Br Med Bull. 54 (2): 433–44. PMID 9830208.
  12. Manary MJ, Heikens GT, Golden M (2009). “Kwashiorkor: more hypothesis testing is needed to understand the aetiology of oedema”. Malawi Med J. 21 (3): 106–7. PMC 3717490. PMID 20345018.
  13. Golden MH (2015). “Nutritional and other types of oedema, albumin, complex carbohydrates and the interstitium – a response to Malcolm Coulthard’s hypothesis: Oedema in kwashiorkor is caused by hypo-albuminaemia”. Paediatr Int Child Health. 35 (2): 90–109. doi:10.1179/2046905515Y.0000000010. PMID 25844980.
  14. Ciliberto H, Ciliberto M, Briend A, Ashorn P, Bier D, Manary M (2005). “Antioxidant supplementation for the prevention of kwashiorkor in Malawian children: randomised, double blind, placebo controlled trial”. BMJ. 330 (7500): 1109. doi:10.1136/bmj.38427.404259.8F. PMC 557886. PMID 15851401.
  15. Smith MI, Yatsunenko T, Manary MJ, Trehan I, Mkakosya R, Cheng J; et al. (2013). “Gut microbiomes of Malawian twin pairs discordant for kwashiorkor”. Science. 339 (6119): 548–54. doi:10.1126/science.1229000. PMC 3667500. PMID 23363771.
  16. Prentice AM, Nabwera H, Kwambana B, Antonio M, Moore SE (2013). “Microbes and the malnourished child”. Sci Transl Med. 5 (180): 180fs11. doi:10.1126/scitranslmed.3006212. PMID 23576812.
  17. Kau AL, Planer JD, Liu J, Rao S, Yatsunenko T, Trehan I; et al. (2015). “Functional characterization of IgA-targeted bacterial taxa from undernourished Malawian children that produce diet-dependent enteropathy”. Sci Transl Med. 7 (276): 276ra24. doi:10.1126/scitranslmed.aaa4877. PMC 4423598. PMID 25717097.
  18. Lefranc, Violaine; de Luca, Arnaud; Hankard, Régis (2016). “Protein-energy malnutrition is frequent and precocious in children with cri du chat syndrome”. American Journal of Medical Genetics Part A. 170 (5): 1358–1362. doi:10.1002/ajmg.a.37597. ISSN 1552-4825.

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Causes

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Overview

Protein energy malnutrition may be caused by reduced breast feeding, poor weaning practices, limited availability of food and inadequate child care in cases of extreme poverty. This classically affects several poor people in regions of poor social and economic background. Other environmental causes such as infections, drought and earthquakes leading to decreased availability of food have also been identified.

Causes

Protein energy malnutrition may be caused by:[1][2][3][4][5][6][7][8][9][10]

References

  1. Sachs JD, McArthur JW (2005). “The Millennium Project: a plan for meeting the Millennium Development Goals”. Lancet. 365 (9456): 347–53. doi:10.1016/S0140-6736(05)17791-5. PMID 15664232.
  2. de Waal A, Whiteside A (2003). “New variant famine: AIDS and food crisis in southern Africa”. Lancet. 362 (9391): 1234–7. doi:10.1016/S0140-6736(03)14548-5. PMID 14568749.
  3. Salama P, Spiegel P, Talley L, Waldman R (2004). “Lessons learned from complex emergencies over past decade”. Lancet. 364 (9447): 1801–13. doi:10.1016/S0140-6736(04)17405-9. PMID 15541455.
  4. Young H, Borrel A, Holland D, Salama P (2004). “Public nutrition in complex emergencies”. Lancet. 364 (9448): 1899–909. doi:10.1016/S0140-6736(04)17447-3. PMID 15555671.
  5. Greiner T (1994). “Maternal protein-energy malnutrition and breastfeeding”. SCN News (11): 28–30. PMID 12288233.
  6. “Maternal Nutrition and Birth Outcomes | Epidemiologic Reviews | Oxford Academic”.
  7. Ahmed T, Begum B, Badiuzzaman, Ali M, Fuchs G (2001). “Management of severe malnutrition and diarrhea”. Indian J Pediatr. 68 (1): 45–51. PMID 11237236.
  8. Aaby P, Coovadia H (1985). “Severe measles: a reappraisal of the role of nutrition, overcrowding and virus dose”. Med. Hypotheses. 18 (2): 93–112. PMID 3939698.
  9. “WHO | Global climate change: implications for international public health policy”.
  10. Bhutta ZA (2006). “Effect of infections and environmental factors on growth and nutritional status in developing countries”. J. Pediatr. Gastroenterol. Nutr. 43 Suppl 3: S13–21. doi:10.1097/01.mpg.0000255846.77034.ed. PMID 17204974.

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Differentiating Protein Energy Malnutrition from other Diseases

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Overview

Protein energy malnutrition must be differentiated from other diseases that cause failure to thrive, edema, wasting recurrent infections, skin and hair changes. It is important to also differentiate kwashiorkor from marasmus as the two diseases are caused by protein-energy malnutrition and share similar features such as, weight loss, muscle wasting, low blood glucose levels and growth retardation.

Differentiating Protein Energy Malnutrition From Other Diseases

Differentiating kwashiorkor from marasmus

Kwashiorkor must be differentiated from marasmus as the two diseases are caused by protein-energy malnutrition and share similar features such as, weight loss, muscle wasting, low blood glucose levels and growth retardation. The followwing table differentiates between the two:[1][2][3][4][5][6][7][8][9][10][11][12]

Distinguishing Features Kwashiorkor Marasmus
Cause Deficiency of protein in the diet of child Deficiency of protein as well as energy nutrients (that is carbohydrates and fats) in the diet
Age Occurs in children in the age group 1-5 years Typically occurs in children below the age of 1 year
Association More common in villages where there is small gap period between successive pregnancies More common in towns and cities where breast-feeding in discontinued quite early
Edema Presence of edema Absence of edema
Muscles Wasting of muscles Wasting of muscles is quite evident. The child is reduced to skin and bones
Skin changes Dermatitis and hyperpigmentation noticed Dry and atrophic skin but no changes in color
Serum cortisol Decreased/Normal Increased
Fasting blood glucose Decreased Decreased
Growth retardation Mildly retarded in growth Severely retarded in growth
Facial appearance Moon-like face Sunken eyes, maxillary prominence, loss of buccal fat pad
Abdomen Protuded Shrunken
Vitamin deficiency Present Present
Weight 60-80% of normal weight for age <60% of normal weight for age

Differential diagnosis of edema and wasting [13][14][15][16][17][18][19][20]

Disease Cause Age(years) Presentation Prevention Workup Prognosis Treatment
Kwashiorkor
  • < 1
Marasmus
  • < 5
: :
Protein losing enteropathy
  • All age groups
Anasarca 1-4 Good prognosis if the underlying cause is identified and treated early
HIV wasting syndrome HIV infection
  • All age groups
Prognosis is good with the use of highly active anti-retroviral therapy (HAART)
Chronic pancreatitis
  • 30 to 40 years
Pediatric nephrotic syndrome <16years
Portal cirrhosis 5th – 6th decade of life Prognosis is poor

Table adapted from CDC Pinkbook.[21]

References

  1. Müller O, Krawinkel M (2005). “Malnutrition and health in developing countries”. CMAJ. 173 (3): 279–86. doi:10.1503/cmaj.050342. PMC 1180662. PMID 16076825.
  2. Manary MJ, Heikens GT, Golden M (2009). “Kwashiorkor: more hypothesis testing is needed to understand the aetiology of oedema”. Malawi Med J. 21 (3): 106–7. PMC 3717490. PMID 20345018.
  3. Henry FJ, Briend A, Fauveau V, Huttly SA, Yunus M, Chakraborty J (1993). “Gender and age differentials in risk factors for childhood malnutrition in Bangladesh”. Ann Epidemiol. 3 (4): 382–6. PMID 8275214.
  4. Coulthard MG (2015). “Oedema in kwashiorkor is caused by hypoalbuminaemia”. Paediatr Int Child Health. 35 (2): 83–9. doi:10.1179/2046905514Y.0000000154. PMC 4462841. PMID 25223408.
  5. RAO KS, SWAMINATHAN MC, SWARUP S, PATWARDHAN VN (1959). “Protein malnutrition in South India”. Bull. World Health Organ. 20: 603–39. PMC 2537781. PMID 14436226.
  6. Barus ST, Rani R, Lubis NU, Hamid ED, Tarigan S (1990). “Clinical features of severe malnutrition at the pediatric ward of Dr. Pirngadi Hospital Medan”. Paediatr Indones. 30 (11–12): 286–92. PMID 2077461.
  7. Rodríguez L, Cervantes E, Ortiz R (2011). “Malnutrition and gastrointestinal and respiratory infections in children: a public health problem”. Int J Environ Res Public Health. 8 (4): 1174–205. doi:10.3390/ijerph8041174. PMC 3118884. PMID 21695035.
  8. Latham MC (1991). “The dermatosis of kwashiorkor in young children”. Semin Dermatol. 10 (4): 270–2. PMID 1764353.
  9. McLaren DS (1987). “Skin in protein energy malnutrition”. Arch Dermatol. 123 (12): 1674–1676a. PMID 3120652.
  10. Jaya Rao KS, Srikantia SG, Gopalan C (1968). “Plasma cortisol levels in protein-calorie malnutrition”. Arch. Dis. Child. 43 (229): 365–7. PMC 2019952. PMID 4297407.
  11. Muniz-Junqueira MI, Queiroz EF (2002). “Relationship between protein-energy malnutrition, vitamin A, and parasitoses in living in Brasília”. Rev. Soc. Bras. Med. Trop. 35 (2): 133–41. PMID 12011921.
  12. Donnen P, Brasseur D, Dramaix M, Vertongen F, Ngoy B, Zihindula M, Hennart P (1996). “Vitamin A deficiency and protein-energy malnutrition in a sample of pre-school age children in the Kivu Province in Zaire”. Eur J Clin Nutr. 50 (7): 456–61. PMID 8862482.
  13. Cho EJ, Kim MY, Lee JH, Lee IY, Lim YL, Choi DH; et al. (2015). “Diagnostic and Prognostic Values of Noninvasive Predictors of Portal Hypertension in Patients with Alcoholic Cirrhosis”. PLoS One. 10 (7): e0133935. doi:10.1371/journal.pone.0133935. PMC 4511411. PMID 26196942.
  14. Cuzzoni E, De Iudicibus S, Franca R, Stocco G, Lucafò M, Pelin M; et al. (2015). “Glucocorticoid pharmacogenetics in pediatric idiopathic nephrotic syndrome”. Pharmacogenomics. 16 (14): 1631–48. doi:10.2217/pgs.15.101. PMID 26419298.
  15. DiMagno MJ, DiMagno EP (2013). “Chronic pancreatitis”. Curr Opin Gastroenterol. 29 (5): 531–6. doi:10.1097/MOG.0b013e3283639370. PMC 4387887. PMID 23852141.
  16. Keithley JK, Swanson B (2013). “HIV-associated wasting”. J Assoc Nurses AIDS Care. 24 (1 Suppl): S103–11. doi:10.1016/j.jana.2012.06.013. PMID 23290370.
  17. Nahlen BL, Chu SY, Nwanyanwu OC, Berkelman RL, Martinez SA, Rullan JV (1993). “HIV wasting syndrome in the United States”. AIDS. 7 (2): 183–8. PMID 8466680.
  18. Vogelaar JL, Loar RW, Bram RJ, Fischer PR, Kaushik R (2014). “Anasarca, hypoalbuminemia, and anemia: what is the correlation?”. Clin Pediatr (Phila). 53 (7): 710–2. doi:10.1177/0009922814526990. PMID 24647692.
  19. Amiot A (2015). “[Protein-losing enteropathy]”. Rev Med Interne. 36 (7): 467–73. doi:10.1016/j.revmed.2014.12.001. PMID 25618488.
  20. Ramírez Prada D, Delgado G, Hidalgo Patiño CA, Pérez-Navero J, Gil Campos M (2011). “Using of WHO guidelines for the management of severe malnutrition to cases of marasmus and kwashiorkor in a Colombia children’s hospital”. Nutr Hosp. 26 (5): 977–83. doi:10.1590/S0212-16112011000500009. PMID 22072341.
  21. “Epidemiology and Prevention of Vaccine-Preventable Diseases”.

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Epidemiology and Demographics
Protein energy malnutrition more prevalent among Africans http://phil.cdc.gov/phil/home.asp
Courtesy to CDC

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2] Mahshid Mir, M.D. [3]

Overview

The prevalence of protein-energy malnutrition in children under 5 years is estimated to be 150 million cases annually. In Nigeria, the prevalence is as high as 41,600 per 100,000 children. Protein-energy malnutrition is majorly a disease of the developing countries. There is no racial or sexual predisposition.

Epidemiology and Demographics

Prevalence

The prevalence of protein energy malnutrition in children under 5 years is estimated to be 41,600 per 100,000 children in developing countries like Nigeria.[1]

The table below show the prevalence of protein energy malnutrition in children under 5 years of age in developing countries in 1995.

Region Stunting (%) Underweight (%) Wasting (%)
Africa 39 28 8
Asia 41 35 10
Latin America and the caribbean 18 10 3
Oceania 31 23 5


Case fatality rate

The case-fatality rate of protein energy malnutrition is unknown.

Age

Protein energy malnutrition commonly affects children under 5 years of age.

Gender

There prevalence and incidence of protein energy malnutrition does not vary by gender.

Race

There is no racial predilection for protein energy malnutrition but it is a disease seen more frequently in Sub-Saharan Africa, Southeast Asia and Central America.

Developed countries

Protein energy malnutrition is almost never seen in developed countries. It is a disease of underdeveloped/developing countries. However, some studies conducted in 2005 – 2007 on children in United States that an estimated 3.5 million children under the age of 5 are at risk of hunger due to an underutilization of existing programs designed to address the issue of proper distribution such as food stamps or school meals.

Developing countries

Protein energy malnutrition is a disease prevalent in the underdeveloped/developing countries of the world. It is widespread in Sub-Saharan Africa and common in Southeast Asia and Central America occurring in young children living in areas with endemic food insecurity or famine. Some of the major countries stricken by kwashiorkor include but are not limited to India, China, Pakistan, Tanzania, North Korea, Nigeria and Kenya.

Disability-adjusted life years (DALY) lost from Protein-energy malnutrition in 2012 per million persons:

Courtesy to WHO
Source=Data from World Health Organization Disease Burden Estimates for 2000-2012
Vector map from BlankMap-World6, compact.svg by Canuckguy et al.


  15-130
  136-142
  146-146
  147-331
  379-1,046
  1,058-1,606
  1,736-2,773
  2,825-2,825
  2,849-11,341
  11,563-60,750


  • Countries are divided approximately by population into ten groups.
  • Dependencies of France, United Kingdom, United States of America, The Netherlands and Denmark are grouped with their respective countries.

References

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Risk Factors

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Overview

Common risk factors in the development of protein energy malnutrition may be classified as maternal and environmental.

Risk Factors

Common risk factors in the development of protein energy malnutrition may be classified as maternal and environmental.[1] The causes of protein energy malnutrition may be distributed unequally and thus, the degree of protein–energy malnutrition disorders including kwashiorkor and marasmus may vary in a given population depending on many factors including:[2][3][4]

  • The political and economical situation of the area
  • The level of education amongst the people
  • The sanitatary conditions
  • The climatic conditions
  • Food production and availability
  • Cultural food preferences in the area
  • Breast-feeding preference among the female population
  • Prevalence of infectious diseases
  • The existence and effectiveness of governmental nutrition programs
  • The quality of health services

Maternal factors:

  • Formal education of mother:
  • Number of children under 5 years:
    • Mothers who have three or more children under 5 years have an increased risk of having a child with protein energy malnutrition when compared to mothers who only have one
  • Young maternal age
  • Occupation of the mother
  • Marital status of the mother

Environmental and child factors:

References

  1. Uwaegbute, Ada C. (1991). “Weaning practices and weaning foods of the Hausas, Yorubas and Ibos of Nigeria”. Ecology of Food and Nutrition. 26 (2): 139–153. doi:10.1080/03670244.1991.9991197. ISSN 0367-0244.
  2. de Waal A, Whiteside A (2003). “New variant famine: AIDS and food crisis in southern Africa”. Lancet. 362 (9391): 1234–7. doi:10.1016/S0140-6736(03)14548-5. PMID 14568749.
  3. Salama P, Spiegel P, Talley L, Waldman R (2004). “Lessons learned from complex emergencies over past decade”. Lancet. 364 (9447): 1801–13. doi:10.1016/S0140-6736(04)17405-9. PMID 15541455.
  4. Young H, Borrel A, Holland D, Salama P (2004). “Public nutrition in complex emergencies”. Lancet. 364 (9448): 1899–909. doi:10.1016/S0140-6736(04)17447-3. PMID 15555671.
Screening

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Overview

There is insufficient evidence to recommend routine screening for protein energy malnutrition.

Screening

There is insufficient evidence to recommend routine screening for protein energy malnutrition.

References

Natural history, complications and prognosis

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Omodamola Aje B.Sc, M.D. [2]

Overview

If left untreated, all children with protein energy malnutrition will progress to develop a failure to thrive, poorly developed immune system which causes overwhelming bacteremia and sepsis which is the cause of death in most malnourished individuals.

Natural history, Complications, and Prognosis

Natural history

The symptoms of protein energy malnutrition usually develop between the first and fifth year of life, and start with symptoms such as lethargy, irritability, failure to thrive, decreased muscle mass, diarrhea, and recurrent infections due to decreased immunity. Without treatment patients with protein energy malnutrition which comprises of kwashiorkor and marasmus present with changes in their facial appearance with children with kwashiorkor having moon faces while those with marasmus develop monkey-like face due to loss of subcutaneous fat pad in the cheeks. There is generalized edema, hepatomegaly, changes in skin, hair color and texture, recurrent infections like diarrhea with kwashiorkor which will eventually lead to overwhelming shock and sepsis and death.[1][2][3]

Complications

Complications that can develop as a result of protein energy malnutrition are:[4][5][6][7][8]

Prognosis

The presence of severe of hypoproteinemia, hypoalbuminemia, electrolyte imbalance or an underlying HIV infection is associated with poorer prognosis among patients with protein energy malnutrition.[9]

References

  1. Bourke CD, Berkley JA, Prendergast AJ (2016). “Immune Dysfunction as a Cause and Consequence of Malnutrition”. Trends Immunol. doi:10.1016/j.it.2016.04.003. PMC 4889773. PMID 27237815.
  2. Rytter MJ, Kolte L, Briend A, Friis H, Christensen VB (2014). “The immune system in children with malnutrition–a systematic review”. PLoS ONE. 9 (8): e105017. doi:10.1371/journal.pone.0105017. PMC 4143239. PMID 25153531.
  3. Scrimshaw NS (2003). “Historical concepts of interactions, synergism and antagonism between nutrition and infection”. J. Nutr. 133 (1): 316S–321S. PMID 12514318.
  4. Bagga A, Tripathi P, Jatana V, Hari P, Kapil A, Srivastava RN, Bhan MK (2003). “Bacteriuria and urinary tract infections in malnourished children”. Pediatr. Nephrol. 18 (4): 366–70. doi:10.1007/s00467-003-1118-0. PMID 12700964.
  5. Jones KD, Berkley JA (2014). “Severe acute malnutrition and infection”. Paediatr Int Child Health. 34 Suppl 1: S1–S29. doi:10.1179/2046904714Z.000000000218. PMC 4266374. PMID 25475887.
  6. Ahmed M, Moremi N, Mirambo MM, Hokororo A, Mushi MF, Seni J, Kamugisha E, Mshana SE (2015). “Multi-resistant gram negative enteric bacteria causing urinary tract infection among malnourished underfives admitted at a tertiary hospital, northwestern, Tanzania”. Ital J Pediatr. 41: 44. doi:10.1186/s13052-015-0151-5. PMC 4472394. PMID 26084628.
  7. Doherty JF, Adam EJ, Griffin GE, Golden MH (1992). “Ultrasonographic assessment of the extent of hepatic steatosis in severe malnutrition”. Arch. Dis. Child. 67 (11): 1348–52. PMC 1793750. PMID 1471885.
  8. Silverman JA, Chimalizeni Y, Hawes SE, Wolf ER, Batra M, Khofi H, Molyneux EM (2016). “The effects of malnutrition on cardiac function in African children”. Arch. Dis. Child. 101 (2): 166–71. doi:10.1136/archdischild-2015-309188. PMID 26553908.
  9. Munthali T, Jacobs C, Sitali L, Dambe R, Michelo C (2015). “Mortality and morbidity patterns in under-five children with severe acute malnutrition (SAM) in Zambia: a five-year retrospective review of hospital-based records (2009-2013)”. Arch Public Health. 73 (1): 23. doi:10.1186/s13690-015-0072-1. PMC 4416273. PMID 25937927.

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Diagnosis

History and Symptoms | Physical Examination | Laboratory Findings | x Ray | echocardiography or ultrasound | CT | MRI | Other imaging findings | Other Diagnostic Studies

Treatment

Treatment

Medical Therapy | Primary Prevention | Secondary Prevention | Cost-Effectiveness of Therapy | Future or Investigational Therapies

Case Studies

Case Studies

References

References

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