4.8 Congenital Malformations of Genital Organs Hypospadias (Q54.0–Q54.9)

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Hypospadias is characterized by an abnormal (ventral) placement of the external urethral meatus in male infants. Normal placement of the urethral meatus is on the tip of the penis, whereas in hypospadias the meatus is ventrally and proximally displaced (on the underside of the penis). Hypospadias is classified by severity (see Fig. 4.31), depending on the location of the meatus: first-degree hypospadias includes the more distal forms, glanular and coronal; second-degree hypospadias includes subcoronal and penile shaft hypospadias; and third-degree – the most severe – includes scrotal and perineal hypospadias.

The shortening of the ventral side of the penis found in hypospadias can result in a curvature of the penis, known as chordee. Chordee is common in severe cases of hypospadias, but it can also occur independently. Chordee by itself is considered a minor anomaly.

Fig. 4.31. Hypospadias

Fig. 4.31. Hypospadias

Photograph source: 1, 2, 4, 5: Nelson Textbook of Pediatrics (http://www.slideshare.net/wadoodaref/congenital-anomalies-videosession-v3-11680674).

Relevant ICD-10 codes

Q54.0 Hypospadias, balanic (coronal, glanular)
Q54.1 Hypospadias, penile (includes subcoronal and midshaft)
Q54.2 Hypospadias, penoscrotal
Q54.3 Hypospadias, perineal
Q54.8 Hypospadias, other
Q54.9 Hypospadias, unspecified

Diagnosis

Prenatal. Hypospadias is difficult to diagnose prenatally by ultrasonography, and might be confused with micropenis, penile cyst, chordee or ambiguous genitalia. For this reason, a prenatal diagnosis of hypospadias should always be confirmed postnatally. When this is not possible (e.g. termination of pregnancy or unexamined fetal death), the programme should have criteria in place to determine whether to accept or not accept a case based solely on prenatal data.

Postnatal. A careful, systematic examination of the male newborn should allow a firm diagnosis of hypospadias. Note that the milder forms such as balanic (glanular) hypospadias are easily missed at delivery and might be discovered during circumcision. The surgical report might provide definitive detail of the urethral placement and whether chordee are present.

Clinical and epidemiologic notes

The diagnosis of hypospadias might be missed, especially with the less severe forms. Observing the flow of urine can aid in the diagnosis and in establishing the degree/severity of the condition. Identifying severity is important because of the different disease associations and the clinical impact. The most severe forms of hypospadias (e.g. scrotal hypospadias) are more often associated with syndromes compared to the milder forms (e.g. balanic [glanular]) of hypospadias.

Hypospadias is often an isolated (> 80%), non-syndromic anomaly. However, the proportion of isolated defects decreases with increasing severity (penile and scrotal) of hypospadias. For this reason, it is crucial to report all findings. Obtaining good clinical photographs is important for the expert reviewer but is not easy to do. Documenting the severity using drawing might help in selected cases.

Suggested non-genetic risk factors for hypospadias include advanced maternal age (> 35 years) and environmental exposure to certain chemicals (endocrine disruptors).

The birth prevalence of hypospadias varies widely, between 2 and 39 per 10 000 births.

Inclusions

Q54.0 Hypospadias, balanic (coronal, glanular)
Q54.1 Hypospadias, penile (includes subcoronal and midshaft)
Q54.2 Hypospadias, penoscrotal
Q54.3 Hypospadias, perineal
Q54.8 Hypospadias, other
Q54.9 Hypospadias, unspecified

Exclusions

Q54.4 Chordee (a minor anomaly if isolated)

Checklist for high-quality reporting

Hypospadias – Documentation Checklist
Describe in detail:
  • Location of urethral meatus – glanular, coronal, subcoronal, shaft, scrotal, perineal.
  • Testes present or absent (if not palpable, consider diagnoses of virilization in females, such as in cases of congenital
    adrenal hyperplasia).
  • Presence of chordee.

Include photographs: Show clearly the location of the urethra or use drawing; can be crucial for review.

Describe evaluations to find or rule out related and associated anomalies:

  • Report undescended testis (unilateral Q53.1, bilateral Q53.2).
  • Chordee – do not report cases of isolated chordee if no hypospadias.
  • Surgical reports – can be very helpful to identify type.
  • Other anomalies of urinary tract (renal) or genitalia.
  • Report if specialty consultations were done and if so, report the results.
  • Genetic/chromosomal/biochemical testing if syndrome suspected.

Report whether autopsy (pathology) findings are available and if so, report the results.

Suggested data quality indicators

Category Suggested Practices and Quality Indicators
Description and documentation Review sample for documentation of key descriptors – location of urethral meatus:
  • Use figure or photographs to document the specific location of the meatus.
Coding
  • Code penile urethral location specifically as Q54.X.
  • Track and minimize the use of Q54.9.
Clinical classification
  • Track any congenital anomalies and/or syndromes occurring with hypospadias (expect ~20% of cases).
  • Report and track proportion of cases among live births, stillbirths and pregnancy terminations.
  • If the fetus was stillborn, or a pregnancy termination performed, check for a pathology report and physical description at delivery.
Prevalence
  • Monitor prevalence overall and by degree: Prevalence might vary by country/region, country income level and race/ethnicity.
Key illustration
Illustration indicates all possible locations for the malformation, but typically a case will only have an opening in one location.

Note: Illustration indicates all possible locations for the malformation, but typically a case will only have an opening in one location.

RENAL AGENESIS/HYPOPLASIA (Q60.0–Q60.5)

Renal agenesis is a complete absence of one (unilateral) or both (bilateral) kidneys. If bilateral, renal agenesis is a lethal condition: the fetus will be stillborn or die shortly after delivery. In utero, bilateral renal agenesis leads to oligohydramnios (too little amniotic fluid), which causes Potter sequence (syndrome) – abnormal facies, talipes (clubfoot) and other contractures, and pulmonary hypoplasia.

Renal hypoplasia is a congenitally small kidney (< 50% of expected weight) without dysplasia, which can be bilateral or unilateral. Renal hypoplasia might be associated with hydronephrosis but is not usually associated with abnormal ureters or other urinary tract findings.

Renal agenesis must be distinguished from renal multicystic dysplasia (Q61.40 and Q61.41) – considered a specific developmental anomaly – and from polycystic renal disease (Q61.1, Q61.2, Q61.3, a single-gene disorder with infantile and later-onset forms).

Fig. 4.32. Renal agenesis/hypoplasia

Fig. 4.32. Renal agenesis/hypoplasia

These have different etiologies and ICD codes.

Relevant ICD-10 codes

Q60.0 Unilateral renal agenesis
Q60.1 Bilateral renal agenesis
Q60.2 Unspecified renal agenesis
Q60.3 Renal hypoplasia, unilateral
Q60.4 Renal hypoplasia, bilateral
Q60.5 Renal hypoplasia, unspecified
Q60.6 Potter sequence with renal agenesis

Diagnosis

Prenatal. Bilateral renal agenesis or severe hypoplasia should be suspected prenatally in a pregnancy with severe oligohydramnios (urine from fetal kidneys accounts for most of the amniotic fluid from 14 weeks’ gestations onward). Fetal kidneys might be small or absent, and the bladder might not be visualized (empty). In contrast, multicystic/polycystic kidneys tend to be large and “bright” on fetal ultrasound. Of note, in some cases, large dysplastic kidneys can reduce and disappear by the time of birth, and in others a kidney might be absent on one side and dysplastic on the contralateral side, suggesting that some cases of agenesis might have started as dysplasia.

Postnatal. At delivery, bilateral renal agenesis should be considered in an infant with features of Potter sequence (Q60.6), which include respiratory distress (due to pulmonary hypoplasia), characteristic facial traits (wide-set eyes, flat face, low-set large ears, small chin, loose or excessive skin), and joint contractures (talipes and others). Bilateral renal hypoplasia might or might not be recognized after delivery, depending on the severity and degree of residual kidney function. Renal agenesis or hypoplasia is conclusively diagnosed only through direct assessment by abdominal ultrasound, CT or MRI scan, surgery or autopsy.

Unilateral renal agenesis or hypoplasia can be clinically silent at delivery if the contralateral kidney is not impaired, such that the diagnosis might occur months or years after birth, if at all. Some unilateral cases are diagnosed only as incidental findings during evaluation for other conditions, or in screening of family members of a patient with bilateral renal agenesis.

Clinical and epidemiologic notes

At least half of cases of bilateral renal agenesis are estimated to be associated with other structural anomalies (e.g. urogenital, cardiac, skeletal, CNS) or syndromes (chromosomal or genetic). The non-syndromic multiple anomaly patterns include the VATER/ VACTERL association (vertebral, anus, cardiac, trachea, oesophagus, renal, limb (radial agenesis); Q87.26), MURCS (mulllerian, renal cervicothoracic, somite) association (Q51.8), sirenomelia (Q87.24), and caudal dysplasia “syndrome” (also seen in maternal pregestational diabetes). Renal agenesis is seen in hundreds of genetic conditions (Mendelian and chromosomal), including common trisomies, deletion 22q11, Melnick-Fraser syndrome, Fraser cryptophthalmos syndrome and branchio-oto-renal syndrome.

Bilateral renal agenesis occurs in 1 in 4000 births and is more common in stillbirths and in males. Unilateral renal agenesis is more common on the left side, is associated with an absent ureter on the same side, and at times with renal hypoplasia in the contralateral kidney. The frequency of unilateral agenesis is estimated as 1 in 3000 births but it is likely underdiagnosed. Nongenetic risk factors include maternal pregestational diabetes.

Inclusions

Q60.0 Unilateral renal agenesis
Q60.1 Bilateral renal agenesis
Q60.3 Renal hypoplasia, unilateral
Q60.4 Renal hypoplasia, bilateral
Unilateral renal agenesis with contralateral renal hypoplasia

Renal agenesis is a defect reported as part of VATER or VACTERL association (vertebral, anus, cardiac, trachea, oesophagus, renal, limb (radial agenesis)).

Exclusions

Q61.1, Q61.19 Autosomal recessive, polycystic kidney, infantile type
Q61.11-Q61.3 Multicystic dysplastic kidney, multicystic renal dysplasia

Checklist for high-quality reporting

Renal Agenesis/Hypoplasia – Documentation Checklist
Describe in detail, including:
  • Unilateral (specify side) versus bilateral.
  • Agenesis and/or hypoplasia (unilateral renal agenesis with contralateral renal hypoplasia).

Take and report photographs of any external defects: Especially show clearly the location of the urethra; can be
crucial for review.

Describe evaluations to find or rule out related and associated anomalies:

  • Other anomalies of urinary tract (renal) or genital organs.
  •  Other unrelated anomalies (such as VATER, VACTERL).
  • Report if specialty consultations were done and if so, report the results.
  • Genetic or chromosomal testing if syndrome suspected.

Report whether autopsy (pathology) findings are available and if so, report the results.

Suggested data quality indicators

Category Suggested Practices and Quality Indicators
Description and documentation
  • Review sample for documentation of key descriptors: Side of renal agenesis and/or hypoplasia.
  • Take and attach photographs: Essential for review and correct classification.
  • Report and track proportion of cases among live births, stillbirths and pregnancy terminations.
Coding
  • Code renal agenesis and/or hypoplasia specifically Q60.x.
  • Track unilateral, bilateral agenesis with/without hypoplasia.
Clinical classification
  • Track any congenital anomalies and/or syndromes occurring with renal agenesis/hypoplasia.
  • If the fetus was stillborn, or a pregnancy termination performed, check for a pathology report and physical description at delivery.
Prevalence
  • Monitor prevalence overall and by sex.
  • Monitor prevalence by specific subtype (unilateral, bilateral).

Table of Contents

  1. Chapter 4: Diagnosing and Coding Congenital Anomalies
  2. 4.1 List of Selected External and Internal Congenital Anomalies to Consider for Monitoring
  3. 4.2 Congenital Malformations of the Nervous System: Neural Tube Defects
  4. 4.2a Anencephaly
  5. 4.2b Craniorachischisis (Q00.1)
  6. 4.2c Iniencephaly (Q00.2)
  7. 4.2d Encephalocele (Q01.0–Q01.83, Q01.9)
  8. 4.2e Spina Bifida (Q05.0–Q05.9)
  9. 4.3 Congenital Anomalies of the Nervous System: Microcephaly
  10. 4.4 Congenital Malformations of the Ear
  11. 4.5a Overview Congenital Heart D: Prenatal Diagnosis and Postnatal Confirmation
  12. 4.5b Common Truncus (Q20.0)
  13. 4.5c Transposition of Great Arteries (Q20.3)
  14. 4.5d Tetralogy of Fallot
  15. 4.5e Pulmonary Valve Atresia (Q22.0)
  16. 4.5f Tricuspid Valve Atresia (Q22.4)
  17. 4.5g Hypoplastic Left Heart Syndrome (Q23.4)
  18. 4.5h Interrupted Aortic Arch (q25.21, Preferred; Also Q25.2, Q25.4)
  19. 4.6 Orofacial Clefts
  20. 4.7 Congenital Malformations of the Digestive System
  21. 4.8 Congenital Malformations of Genital Organs Hypospadias (Q54.0–Q54.9)
  22. 4.9a Congenital Malformations and Deformations of the Musculoskeletal System: Talipes Equinovarus (Q66.0)
  23. 4.9b Congenital Malformations and Deformations of the Musculoskeletal System: Limb Reduction Defects/Limb Deficiencies
  24. 4.9c Limb Deficiency Amelia (Q71.0, Q72.0, Q73.0)
  25. 4.9d Limb Deficiency: Transverse Terminal (Q71.2, Q71.3, Q71.30, Q72.2, Q72.3, Q72.30)
  26. 4.9e Limb Deficiency: Transverse Intercalary (Q71.1, Q72.1, Q72.4)
  27. 4.9f Limb Deficiency: Longitudinal Preaxial (Tibia, Radius, First Ray) (Q71.31, Q71.4, Q72.31, Q72.5)
  28. 4.9g Limb Deficiency: Longitudinal Postaxial (Fibula, Ulna, Fifth Ray) (Q71.30, Q71.5, Q72.30, Q72.6)
  29. 4.9h Limb Deficiency: Longitudinal Axial Limb Deficiency – Split Hand and Foot (Q71.6, Q72.7)
  30. 4.10 Abdominal Wall Defects
  31. 4.11 Chromosomal Abnormalities