Germ Cell Tumors

Basics

Germ cell tumors (GCTs) are a heterogeneous group with a suspected common cell of origin, the primordial germ cell.

Their location can be gonadal or extragonadal.
The numerous histologic subtypes are broadly classified as mature or immature teratomas and malignant GCTs.
See “Brain Tumor” chapter for primary CNS GCT.

The incidence has a bimodal distribution with a smaller peak in early infancy and a larger peak in adolescence.

In children younger than 15 years of age, GCTs occur at a rate of 2.4 cases per million children, and they account for 2–3% of all malignancies.
Between 15 and 19 years of age, extracranial GCTs account for approximately 14% of cancer diagnoses.
Teratomas and germinomas are the predominant histologic subtypes of early infancy and adolescence respectively.
Sacrococcygeal teratomas account for 50% of childhood teratomas. They are most prevalent in infants (1:40,000 live births); with a female predominance (4:1)

Sex chromosome abnormalities are associated with an increased risk for GCTs.
Klinefelter syndrome is associated with an increased risk of mediastinal GCTs.
- Approximately 50% of adolescent mediastinal GCTs are associated with a cytogenetic diagnosis of Klinefelter syndrome.
Turner syndrome with any portion of Y chromosome material, Swyer syndrome, nonscrotal partial androgen insensitivity, Frasier syndrome, and males with Denys-Drash syndrome are all associated with streak gonads at increased risk for developing GCTs.
History of cryptorchidism is associated with an increased risk of testicular GCT.

Familial GCT has been described in 1.5–2% of adult GCTs and a similar contribution to adolescent GCTs is presumed.

Prophylactic gonadectomy is recommended for streak gonads in the specific syndromes mentioned above because of the increased risk of developing GCTs.
Guidelines on the management of cryptorchidism recommend the following to decrease the future risk of testicular GCT:
- Orchidopexy by 18 months of age
- Consideration of orchiectomy of an undescended testis in all boys with a normal contralateral testis when orchidopexy is not feasible
- Consider orchiectomy or biopsy in a post pubertal boy with cryptorchidism.
- Counsel all men with a history of cryptorchidism and/or their parents regarding the long-term risk of testicular cancer.

GCTs are hypothesized to originate from primordial germ cells containing neoplastic genetic aberrations.
Arrested migration of primordial germ cells is presumed to explain the midline location of extragonadal GCTs.
The postpubertal peak in the incidence of GCTs suggests hormonal factors are involved in their growth.
Isochromosome 12p or i(12)p is present in more than 80% of postpubertal GCTs. GCTs without the i(12)p typically have gain of 12p chromosomal material.
- Mature and immature ovarian tumors are biologically distinct in their lack of association with the i(12)p.
- A number of other genetic mutations have been observed in testicular GCTs.
Malignant GCTs in children younger than age 4 years typically contain cytogenetic abnormalities of chromosomes 1, 3, 6, and others.
- The i(12)p is rarely seen in this group.
- Deletion of 1q36 is present in 80–100% of infantile malignant GCTs in testicular and extragonadal sites.
- Recurrent genetic changes of infantile yolk sac tumors include loss of 6q24-qter, gain of 20q and 1q, loss of 1p, and c-myc or n-myc amplification.

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