Objectives: Upon completion of this CE activity, the nurse will be able to:
- Describe the statistical data regarding endocrine disorders in the US, including prevalence and significance
- Articulate the pathophysiology, risk factors, clinical presentation, diagnosis, evidence-based management, and potential complications of hypothalamus and pituitary disorders, including growth hormone excess, hyperprolactinemia, and syndrome of inappropriate antidiuretic hormone secretion (SIADH)
- Define the pathophysiology, risk factors, clinical presentation, diagnosis, evidence-based management, and potential complications of polycystic ovary syndrome (PCOS)
- Explore the pathophysiology, risk factors, clinical presentation, diagnosis, evidence-based management, and potential complications of parathyroid dysfunction
- Recognize the pathophysiology, risk factors, clinical presentation, diagnosis, evidence-based management, and potential complications of multiple endocrine neoplasia type 1 (MEN1)
The purpose of this module is to provide the nurse with an overview of the pathophysiology, risk factors, clinical presentation, diagnosis, evidence-based management guidelines, and potential complications of primary endocrine disorders leading to hormonal excess, including acromegaly, gigantism, hyperprolactinemia, syndrome of inappropriate antidiuretic hormone secretion, polycystic ovary syndrome, hyperparathyroidism, and multiple endocrine neoplasia type 1. Please see the first part of this endocrine series for a review of the anatomy and physiology of the endocrine system (Figure 1).
Alterations in Endocrine Function
There are many disorders of the endocrine system, and an imbalance or disorder of one part of the endocrine system can lead to disorders within other parts. Identifying the primary etiology of the disorder is vital in determining the optimal treatment. Primary endocrine disorders originate within the gland, while secondary endocrine disorders are caused by problems outside of the glands, typically within the feedback mechanism. External problems may be due to trauma, surgery, infection, tumors, or certain drugs. Causes of endocrine disorders vary but typically involve either an excess or deficiency in hormone secretion or insensitivity of the target tissue to the hormone (Hopper, 2015; Ignatavicius et al., 2018).
The growth hormone (GH) is produced by the pituitary gland in response to the secretion of GH-releasing hormone (GHRH) by the hypothalamus gland. GH then triggers the synthesis of insulin-like growth factor (IGF-1), which is predominantly accomplished by the liver (Chapman, 2019). In healthy individuals, a negative feedback loop exists in which high circulating IGF-1 inhibits the secretion of GH, as well as the secretion of the thyroid hormones T3 and T4 (El Sayed et al., 2020). Acromegaly and gigantism occur when the pituitary gland produces excessive amounts of GH (hypersomatotropism). The prevalence is estimated at between 40 and 125 cases per million people (Shahid et al., 2020). While acromegaly and gigantism are similar chronic and progressive conditions and the terms are often used interchangeably, they have a few important distinctions. Gigantism occurs in children before the closure of their epiphyses; it is extremely rare, with a prevalence of 3-4 cases per million per year worldwide (Schwartz, 2020). Acromegaly is more common but often overlooked, with a prevalence of 2.8 to 13.7 cases per 100,000 people worldwide. It is diagnosed in adults after the epiphyses’ closure; most patients present in the 20-40s with distinct facial and body characteristics. Prompt treatment is needed because this condition can lead to life-threatening complications such as hypertension (HTN), cardiomyopathy, diabetes mellitus (DM), spinal cord compression, and vision loss (Chapman, 2019; Mayo Clinic, 2019).
Acromegaly most often affects middle-aged adults but can develop at any age. It is most often caused by a benign pituitary adenoma. Nonpituitary GHRH-producing tumors in the pancreas or lung may also cause acromegaly, stimulating the pituitary to make more GH. If excess GH is produced by the pituitary, more IGF-1 is also produced. This causes abnormal growth of the soft tissues, skeleton, and other classic signs of acromegaly. The earlier the condition is diagnosed, the fewer complications will ensue (Chapman, 2019; Mayo Clinic, 2019).
The diagnosis of acromegaly or gigantism is based on the patient's history, presenting signs and symptoms, and laboratory and imaging results. Gigantism is characterized by exaggerated bone growth velocity leading to abnormal increases in height. It typically causes soft tissue swelling and peripheral nerve enlargement and is often associated with hypogonadotropic hypogonadism (a gonadotropin-releasing hormone [GnRH] deficiency). It causes swelling of the hands and feet and coarsening of facial features (i.e., nasal bone hypertrophy, frontal bossing [prominent forehead], and prognathism [lower jaw protrusion]). The patient’s skin may darken or thicken, and they may report increased coarse body hair, perspiration, and body odor; the provider may find deepening of the voice due to vocal cord enlargement, as well as enlargement of the tongue, cartilage proliferation leading to joint destruction, organomegaly, and peripheral neuropathy (Chapman, 2019; Mayo Clinic, 2019). Acromegaly may also produce the following symptoms:
- skin tags
- fatigue or muscle weakness
- sleep apnea and severe snoring
- headaches (HAs)
- menstrual irregularities
- erectile dysfunction
- decreased libido (Mayo Clinic, 2019)
Lab tests should include fasting blood levels of GH, IGF-1, and blood glucose (BG). The serum IGF-1 may be 3 to 10 times the expected normal value. A radioimmunoassay of GH should be done in the morning after fasting overnight (reference range < 5 ng/mL or µg/L). The definitive test for acromegaly is the GH suppression test. After the fasting baseline GH and BG levels are drawn, the patient drinks a 75-g glucose solution. The solution must be consumed within 5 minutes to ensure the accuracy of the test but should not be ingested too quickly due to the risk of nausea. The patient’s GH and BG should be rechecked about 90 minutes after the patient finishes the glucose solution and may be taken every 30 or 60 minutes during this timeframe. Each sample should go to the lab immediately for processing. The GH in healthy patients will typically be reduced below 1-2 ng/mL or µg/L, and those with acromegaly/gigantism often have a substantially higher serum GH level, although the exact cutoff for the diagnosis is somewhat controversial and may vary. Imaging may include a CT scan, MRI, or X-rays of the skull or other bones to assess for cortical thickening, enlarged frontal sinuses and sella turcica (with possible erosion), or osteoporosis. Brain imaging should also assess for a pituitary or hypothalamus tumor (Chapman, 2019; Mayo Clinic, 2019).
Treatment involves lowering the production of GH and alleviating the negative effects of the tumor on surrounding structures (Mayo Clinic, 2019). Surgery may be indicated to remove the tumor; this may normalize GH production. Transsphenoidal resection is most common. If the tumor is in a location that precludes surgical removal, then radiation or other treatments may be indicated (Chapman, 2019).
Radiation may be recommended if part of the tumor remains after surgery or in cases of inoperable tumors. Radiation will destroy lingering tumor cells and help reduce GH levels. The following types of radiation may be used as therapy for acromegaly:
- Conventional radiation therapy is given every weekday over 4-6 weeks but could take up to 10 years to realize the full effect.
- Proton beam therapy delivers a targeted, high dose of radiation to the tumor and spares normal surrounding tissue.
- Stereotactic radiosurgery delivers a high dose of radiation to tumor cells in a single dose. It limits the amount of radiation exposure to normal surrounding tissue and may normalize GH levels within 5 years (Mayo Clinic, 2019).
Unfortunately, iatrogenic hypopituitarism may develop several years after radiation therapy (Chapman, 2019). Medications that lower or block GH production are as follows:
- Octreotide (Sandostatin), octreotide acetate (Sandostatin LAR), and lanreotide (Somatuline Depot) are somatostatin analogs, prompting a decrease in the secretion of GH by the pituitary.
- The dopamine agonists cabergoline (Dostinex) and bromocriptine (Parlodel) decrease levels of GH and IGF-1 less effectively than the somatostatin analogs. Nausea, postural hypotension, and mental fogginess are common side effects of both of these medications.
- Pegvisomant (Somavert) is a new GH receptor antagonist that can be administered as a daily injection if other treatments are not effective. This drug can normalize IGF-1 levels and relieve symptoms, but it does not lower GH levels or reduce tumor size (Chapman, 2019; Mayo Clinic, 2019; Snyder, 2020b).
The nurse should educate patients in the following areas:
- instruction on reducing stress as much as possible prior to the GH suppression test, as stress can artificially elevate GH levels;
- instruction on the treatment regime, ensuring the patient and their family understand the importance of compliance;
- alerting the patient and their family regarding the dangers of OTC drugs, herbals, and other medications that may interact with prescribed treatment;
- instruction to wear a medical alert bracelet to alert caregivers of diagnosis; and
- annual follow-up with labs and imaging studies, if appropriate, is crucial for managing acromegaly and avoiding long-term and potentially life-threatening complications (Mayo Clinic, 2019).
Prolactin (PRL) is a hormone produced by lactotrophs in the anterior pituitary. It targets the gonads and mammary glands. It manages the growth and development of mammary glands in pubescent girls, as well as milk production in postpartum women. Its secretion is regulated by the hypothalamus, predominantly through inhibition (via the secretion of PIH, or dopamine), as well as PRH and TRH, which increase secretion to a lesser degree (El Sayed et al., 2020).
Hyperprolactinemia, or an excess of circulating PRL, is often caused by a PRL-secreting adenoma (termed a prolactinoma), medications, pregnancy, lactation, increased stress, or cranial radiation therapy (El Sayed et al., 2020). It may also be caused by hypothalamic dysfunction, specifically a reduction in the secretion of dopamine (Shahid et al., 2020). An elevation in the PRL level inhibits the secretion of GnRH by the hypothalamus, luteinizing hormone/follicle-stimulating hormone (LH/FSH) by the anterior pituitary, and eventually estrogen/progesterone by the ovaries, leading to anovulation, amenorrhea, and other menstrual irregularities (El Sayed et al., 2020).
Due to the secondary decrease in estrogen and progesterone, the most common signs and symptoms of hyperprolactinemia in premenopausal women include hypogonadism, as well as occasional galactorrhea and HA. In men, hyperprolactinemia may cause decreased libido, erectile dysfunction, infertility, gynecomastia/galactorrhea, and other signs of hypogonadism. Postmenopausal women are typically asymptomatic, as they are hypogonadotropic at baseline. An elevated fasting morning serum PRL level is typically considered diagnostic (Shahid et al., 2020; Snyder, 2020a).
If medications are believed to be the underlying cause, they should be adjusted when possible. In the event of a lactotroph adenoma, a surgical consult is recommended to determine whether the lesion can be removed surgically, particularly for patients who are not responding to or cannot tolerate pharmacological treatment. As previously mentioned, surgery is typically performed via transsphenoidal resection. Lactotroph microadenomas (under 1 cm) and macroadenomas under 3 cm in size are typically treated pharmacologically with a dopamine agonist such as cabergoline (Dostinex) or bromocriptine (Parlodel). Cabergoline has been more effective in inducing menstruation and facilitating pregnancy with fewer side effects, although it does carry an increased risk of valvular heart disease at higher doses. As mentioned above, both medications involve side effects of nausea, postural hypotension, and mental fogginess. Less frequently, these agents can cause an adverse effect of compulsive behaviors such as gambling. Nausea is significantly more common with bromocriptine (Parlodel). Alternatives for women who do not respond to or cannot tolerate treatment with dopamine agonist therapy and are not seeking fertility include exogenous estradiol and progesterone therapy. Similarly, men with hyperprolactinemia who do not respond to or cannot tolerate treatment with dopamine agonist therapy can receive exogenous testosterone if they are not seeking fertility; human chorionic gonadotropin (hCG [Novaerl]) may be considered if the patient seeks fertility. For additional information on the treatment of hypogonadism, refer to the next section. For patients with microadenomas, the serum PRL level is typically rechecked monthly while on pharmacologic therapy until they are stable and then at least yearly (Snyder, 2020b).
For patients with a macroadenoma (greater than 1 cm in size) who are on dopamine agonist therapy, imaging should be repeated to assess for a decrease in the size of the lesion at 6-12 months. The serum PRL level should be rechecked monthly initially until this stabilizes, at 6 months, and then at least yearly. If the patient remains stable on the medication for at least 2 years and the MRI results are negative, the gradual discontinuation of the medication can be considered. As previously mentioned, a surgical consult is recommended for any patient who is not responding to pharmacological treatment. Postoperative radiation therapy may be indicated to prevent regrowth after the surgical debulking of larger macroadenomas that are resistant to dopamine agonist therapy (Snyder, 2020b).
Syndrome of Inappropriate Antidiuretic Hormone Secretion (SIADH)
The hypersecretion of antidiuretic hormone (ADH) leads to a reduction in water secretion by the kidneys, inducing hyponatremia, a decrease in serum osmolality, and an increase in urine osmolality (Thomas, 2019).
Increased secretion of ADH is typically related to a central nervous system disorder, such as a stroke, hemorrhage, infection, traumatic brain injury, malignancy, or medications. The medications most often associated with increased ADH secretion include chlorpropamide (Diabinese), carbamazepine (Tegretol), cyclophosphamide (Cytoxan), and selective serotonin reuptake inhibitors (SSRIs; Shahid et al., 2020).
SIADH typically presents with signs of hyponatremia, such as nausea or vomiting, HAs, difficulty thinking, weakness, and restlessness (Shahid et al., 2020). Patients may also present with ataxia or falls. Patients with chronic disease may present asymptomatically or appear minimally symptomatic. The classic diagnostic criteria by Bartter and Schwartz that were developed in 1967 are still applicable. Laboratory evaluation of SIADH patients typically indicates serum sodium below 135 mmol/L, serum osmolality below 280 mOsm/kg, and urine osmolality above 100 mOsm/kg (Thomas, 2019).
Hyponatremia related to SIADH should be corrected slowly (max 8-12 mEq/L in the first 24 hours) to avoid osmotic demyelination syndrome, which is also known as central pontine myelinolysis (CPM; Shahid et al., 2020; Thomas, 2019). The recommendations according to the American Expert Panel include:
- limiting the rate of correction if the condition is chronic;
- initiating fluid restriction as the first line of treatment, limiting intake to 500-1500 mL/day;
- considering pharmacological treatment only if serum sodium levels remain abnormally low after 24-48 hours of fluid restriction;
- avoiding fluid restrictions for patients on vasopressin-2 receptor antagonists (aquaretics or vaptans); and
- utilizing water, 5% dextrose, or desmopressin to slow the rate of correction if diuresis is profound (Thomas, 2019).
More aggressive management should occur for patients presenting with more severe symptoms of hyponatremia (e.g., seizures, a decreased level of consciousness, and respiratory arrest) or in cases involving acute moderate to severe hyponatremia (less than 48 hours in duration). This may include the infusion of 3% hypertonic saline solution. The treatment team should monitor the patient closely during this time for any changes in neurological status, in addition to regular monitoring of the serum sodium level. Alternative treatment options for acute sodium correction include the use of loop diuretics (e.g., furosemide [Lasix]) in combination with normal saline or 3% and V2 receptor antagonists. The same close monitoring techniques noted earlier are recommended for these patients. When treating chronic cases of SIADH, fluid restriction is the preferred first-line treatment. Medication, typically a V2 receptor antagonist (aquaretic or vaptan), should be considered if the patient’s sodium level does not increase by at least 2 mEq/L after 24 hours of a 1,000-mL fluid restriction. Conivaptan (Vaprisol) is only approved for use in hospitalized patients in an IV formula. Tolvaptan (Samsca) is available as an oral formula for the treatment of hypervolemic or euvolemic hyponatremia. Initial dosing should start at 15 mg daily, titrating up carefully to a max of 60 mg daily with no fluid restriction in place while titrating the dose. Patients can remain on tolvaptan (Samsca) long term if needed, or the medication can be tapered carefully a few weeks after the resolution of an underlying cause for SIADH, such as tumor removal, resolution of infection, or discontinuation of the implicated medication. Alternative medications for the treatment of chronic SIADH include loop diuretics or urea. Loop diuretics help increase the excretion of free water by inhibiting sodium and chloride resorption in the kidneys, while urea helps increase urine volume by increasing the urinary osmotic or solute load. It should be dosed based on weight (0.5 g/kg) and comes packaged as a powder that should be dissolved in water for convenient administration (Thomas, 2019).
The parathyroid glands are four small glands located just on the posterior surface of the thyroid gland (see Figures 1 and 4). As previously mentioned, these structures regulate circulating serum calcium and phosphorus via the secretion of PTH. While hypocalcemia related to a deficiency in PTH is possible, it is exceedingly rare. More commonly, an excess of PTH leads to hypercalcemia, which increases the risk of nephrolithiasis (kidney stones), osteopenia, and eventually fractures (National Institute of Diabetes and Digestive and Kidney Diseases [NIDDK], 2019).
Hyperparathyroidism may be primary (related to parathyroid gland pathology) or secondary to chronic kidney disease (CKD), chronic vitamin D deficiency, or altered absorption (e.g., inflammatory bowel disease). In the US, the incidence of primary hyperparathyroidism is approximately 100,000 new cases annually, with a prevalence of 1 in 600 to 1,000 people. Approximately 80% of these cases are caused by a benign adenoma in one of the parathyroid glands. A smaller portion (10-15%) of primary hyperparathyroidism patients are diagnosed with hyperplasia, in which all four glands are enlarged. Rarely, primary hyperparathyroidism may be caused by MEN1, familial hypocalciuric hypercalcemia, or malignancy of the parathyroid gland. Risk factors include age between 50 and 60, and the condition affects roughly three to four times more women than men. It is most common in patients with African American ethnicity, followed by Caucasian patients (NIDDK, 2019).
Most patients with hyperparathyroidism are asymptomatic. Symptoms may be mild and include muscle weakness, fatigue, depression, and painful joints/bones. Patients with more severe hyperparathyroidism may present with confusion, decreased appetite, nausea/vomiting, constipation, polyuria, and polydipsia. The diagnosis of hyperparathyroidism is typically made incidentally on routine laboratory testing. Patients with increased serum calcium should be further evaluated, and the diagnosis is typically confirmed by an elevated serum PTH level, elevated calcium (greater than 400 mg/d) on a 24-hour urine collection, and creatinine clearance below 60 mL/min. These patients should also undergo a DEXA scan to assess their BMD for possible osteopenia and a serum 25 hydroxyvitamin D test to assess for deficiency. Imaging studies—a CT scan, an ultrasound, or a sestamibi scan (using a parenteral radioactive tracer)—may be warranted to rule out nephrolithiasis and gather additional information for surgical planning (NIDDK, 2019).
The first-line treatment for primary hyperparathyroidism is the surgical excision of the affected gland (typically one of four). A focused or minimally invasive parathyroidectomy is usually performed as an outpatient or same-day procedure. Research indicates that surgical excision leads to both improved BMD and a reduced risk of nephrolithiasis. For parathyroid hyperplasia, surgery typically involves the excision of three and a half of the patient's four parathyroid glands via bilateral neck exploration. Patients who are not surgical candidates or opt to treat their condition more conservatively may be treated with cinacalcet (Sensipar) to reduce serum calcium levels (NIDDK, 2019).
Polycystic Ovary Syndrome
PCOS is the most common endocrine disorder affecting females during their reproductive years (Teede et al., 2018). PCOS affects 8-20% of females, many of whom are undiagnosed. About one in 10 females with PCOS will develop type 2 DM (T2DM), and 30-40% will develop impaired glucose tolerance by age 40 years; approximately 70% of ovulatory and fertility issues among premenopausal women is due to PCOS. There are no known causes of PCOS, but risk factors include genetics, insulin resistance, and low-grade inflammation that may lead to the disorder. Females who have a first-degree relative with PCOS (i.e., mother or sister) are more likely to develop the disorder than those without this family history. Several health risks are associated with PCOS. These include:
- insulin resistance and eventually T2DM;
- cardiac disease;
- sleep apnea;
- abnormal uterine bleeding;
- obesity that can lead to low self-esteem;
- metabolic syndrome, including HTN, hyperlipidemia, elevated BG, and increased waist circumference;
- steatohepatitis (non-alcoholic fatty liver);
- depression and anxiety; and
- endometrial cancer (Lucidi, 2019; Smith, 2018; Teede et al., 2018).
Patients with PCOS report a decreased quality of life, and the condition is associated with an increased risk of gestational DM, pregnancy-induced HTN (PIH), miscarriage, myocardial infarction (MI), and endometrial cancer (Smith, 2018; Teede et al., 2018).
An imbalance of reproductive hormones characterizes PCOS (see Figure 10). This hormonal imbalance leads to ovarian dysfunction. The ovaries normally release one egg each month during ovulation, as part of the menstrual cycle. In patients with PCOS, the egg may not develop completely or may not be released during ovulation. PCOS can prompt metrorrhagia (irregular menses) or amenorrhea, which can lead to infertility (Office on Women’s Health [OWH], 2019). While the pathophysiology of PCOS is not completely understood, it is characterized by relatively high levels of androgens (i.e., testosterone, androstenedione, and DHEA), which is likely due to an overproduction of LH by the anterior pituitary. An increase in LH leads to relatively low FSH and decreased production of estrogen by the ovaries (Lucidi, 2019).
Anovulation in patients with PCOS is likely due to the high levels of androgens, which can also cause excess hair growth and acne—both signs of PCOS. As patients with PCOS age, their menstrual cycles typically become increasingly regular as they near menopause; however, the hormonal imbalance does not improve with age and the other symptoms of PCOS persist. While the risk of type 2 DM, MI, and stroke increases with age among all women, the risk is even higher in women with PCOS (OWH, 2019).
PCOS should be suspected if symptoms of hyperandrogenism appear, including acne, alopecia (hair loss on the scalp), hirsutism (extra hair growth on the face, chin, or body), and metrorrhagia. Metrorrhagia is an expected finding within the first year following menarche, after which (Teede et al., 2018).
An hCG level should be drawn to rule out pregnancy for women with amenorrhea. Blood tests for androgen levels can include free androgen index, calculated free testosterone, or calculated bioavailable testosterone. The Rotterdam criteria are still the most widely utilized clinical diagnostic criteria for the diagnosis of PCOS in adults (Teede et al., 2018). The Rotterdam criteria include three qualifiers, two of which must be present for PCOS diagnosis: androgen excess, ovulatory dysfunction, and polycystic ovaries. While the diagnostic criteria for adolescents are not as clear, hyperandrogenemia (elevated systemic levels of androgens) is essential for the diagnosis in this age group (Lucidi, 2019).
LH and FSH levels should be assessed to rule out ovarian failure (Lucidi, 2019; OWH, 2019: Teede et al., 2018). Typically, a patient with PCOS will have a relatively elevated LH level for their Tanner stage, sex, or age; an FSH level that is normal or slightly below normal; and an LH:FSH ratio that is above 3 (Lucidi, 2019).
Patients diagnosed with PCOS should undergo cardiovascular disease risk evaluation, including a lipid profile for patients who are overweight, as well as glucose-tolerance testing (Teede et al., 2018). Thyroid function should be assessed using TSH and potentially FT4, and a fasting serum PRL is typically recommended (Lucidi, 2019).
Treatment for PCOS is multifactorial. It is important to discuss options for symptomatic control, the patient’s plans for having children, and the risks of long-term problems such as T2DM or heart disease. Goals should be set for symptom control, and the plan of care should be developed around those goals. Furthermore, referrals to a dietician for weight management, an endocrinologist, and reproductive specialists may be indicated depending on the severity of the patient’s PCOS. First-line treatment should consist of lifestyle changes such as exercise and diet (Lucidi, 2019). At least 150 minutes of moderate-intensity exercise per week is recommended, and behavioral therapy/programs may help achieve a 5-10% weight reduction in patients who are overweight or those with central obesity or insulin resistance (Teede et al., 2018).
Pharmacological treatment options for those with hyperandrogenism and menstrual irregularities include combined oral contraceptives (COCs) with 20 mcg ethinyl estradiol and progestin (norethindrone [Loestrin, Junel, Microgestin]). If lifestyle modifications and COCs are not effective, 1500 mg daily of metformin (Glucophage) may be tried, especially for those patients with impaired glucose tolerance. An antiandrogen (aromatase inhibitor) treatment such as letrozole (Femara) may be considered for the management of hirsutism (Teede et al., 2018).
For patients with PCOS who are seeking fertility, ovulation-induction agents may be trialed, but the patient should first be informed that these medications are currently considered off-label. This includes the aromatase inhibitor letrozole (Femara), metformin (Glucophage), and clomiphene citrate (Clomid; Teede et al., 2018). If these medications are ineffective, exogenous gonadotropins could be considered to induce fertility. Laparoscopic ovarian surgery could also be considered a second-line treatment for clomiphene citrate (Clomid)-resistant patients with only PCOS and anovulatory infertility. More invasive reproductive procedures, such as in-vitro fertilization, may be considered if these options have been unsuccessful (Teede et al., 2018). Statins may be indicated for patients with dyslipidemia (Lucidi, 2019).
Patient education should include the importance of consistent follow-ups, as PCOS is a lifelong disease with many complications. Early intervention for untoward sequelae should be the goal. The patient should receive education regarding the risks of pregnancy for those who conceive, including gestational DM, PIH, C-section delivery, preterm and post-term delivery, newborns who are large for gestational age, and stillbirth (Lucidi, 2019).
Multiple Endocrine Neoplasia Type 1 (MEN1)
This rare (prevalence 1 in 30,000) endocrine disorder most often affects the parathyroid gland, the pancreas, and/or the pituitary gland. It is typically familial and based on a genetic defect that is inherited in an autosomal dominant pattern, although as many as 10% of cases may be due to a random mutation (NIDDK, 2020).
MEN1 is characterized by multiple benign tumors located throughout the endocrine and gastrointestinal systems. Most patients with MEN1 initially present with signs and symptoms of hyperparathyroidism in their early 20s, but the average age of diagnosis is not until the fifth decade of life. The vast majority (95%) of MEN1 patients develop parathyroid tumor(s) by age 50, while 40% develop tumors in the pancreas, duodenum, or another gastrointestinal organ (gastrinoma or insulinoma), and 33% develop an anterior pituitary tumor (prolactinoma). Initially, these tumors cause hypersecretion of the gland's hormone(s); if the tumor(s) grow significantly, it/they may eventually cause hyposecretion (NIDDK, 2020).
The presenting signs and symptoms of MEN1 mimic those previously discussed throughout this module and vary depending on the organs affected (parathyroid gland versus anterior pituitary) and the severity/stage of the disease (hypersecretion initially, followed by hyposecretion during later stages; NIDDK, 2020).
Any patients with suspected MEN1 should be referred to an endocrinologist with experience managing MEN1 cases. Treatment plans for patients with MEN1 typically include regular laboratory monitoring of serum calcium, PTH, PRL, and gastrin. Advanced imaging studies, including MRIs or CT scans, are typically performed to assess for tumors throughout the endocrine and gastrointestinal organs. If possible, surgical procedures to excise or debulk tumors will be performed, similar to treatment options listed above for other benign endocrine tumors (NIDDK, 2020).
For learners who are eager to access additional content related to the endocrine system and endocrine disorders, please see the following NursingCE courses:
- Endocrine and Hormonal Disorders Part 1: Anatomy and Physiology
- Endocrine and Hormonal Disorders Part 2: Hypopituitarism and Other Hormone Deficiencies
- Endocrine and Hormonal Disorders Part 4: Adrenal Gland Disorders
- Thyroid Dysfunction
- Sexual Dysfunction
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