β‐subunit of each that confers biological specificity.
Box 1.4 Major hormone groups
Peptides and proteins
Amino acid derivatives
Steroids
Figure 1.3 The structures of vasopressin and oxytocin are remarkably similar, yet the physiological effects of the two hormones differ profoundly.
Amino acid derivatives
These hormones are small water‐soluble compounds. Melatonin is derived from tryptophan, whereas tyrosine derivatives include thyroid hormones, catecholamines, and dopamine, which regulates prolactin secretion in the anterior pituitary. The catecholamine hormones, epinephrine (also called adrenaline) and norepinephrine (noradrenaline) are secreted by the adrenal medulla as well as being sympathetic neurotransmitters, emphasizing the close relationship between the nervous and endocrine systems (Figure 1.2). Like peptide hormones, they are stored in granules prior to release.
Steroid hormones
Steroid hormones are lipid‐soluble molecules derived from cholesterol. Cholesterol is present in all cells as a basic constituent of the cell membrane. However, in the steroid hormone synthesizing cells of the adrenal cortex, gonad and placenta, it is also extracted from the circulation and stored intracellularly as cholesterol esters. Steroid hormones are insoluble in water and circulate largely bound to plasma proteins.
Control systems regulating hormone production
The synthesis, release and circulating level of hormones are regulated by control systems, similar to those used in engineering. These mechanisms ensure that hormone signals can be limited in amplitude and duration. Central to the regulation of many different endocrine organs is the anterior pituitary gland, which, in turn, is controlled by several hormones and factors released from specialized hypothalamic neurones (Chapter 5). Thus, the body’s major endocrine axes comprise the hypothalamus, anterior pituitary and an end organ, the adrenal cortex, thyroid, testis or ovary. An understanding of these control mechanisms is crucial for appreciating endocrine physiology and its clinical investigation.
Simple control
An elementary control system is one in which the signal itself is limited, either in magnitude or duration, so as to trigger only a transient response. Certain neural impulses are of this type. Responsiveness of the target cell is set to discriminate between a positive signal, when a cell responds, and background ‘noise’, when a response is not triggered. An example is the pulsatile release of gonadotrophin‐releasing hormone (GnRH) from the hypothalamus.
Negative feedback
Negative feedback is the commonest form of regulation used by biological systems. For example, in enzymology, the product frequently inhibits its own catalyzed reaction. In endocrinology, a hormone may act on its target cell to elicit a response (often secretion of another hormone) that then inhibits production of the original hormone (Figure 1.4a). The same effect can come from a metabolic process. For instance, the pancreatic β‐cell makes insulin in response to high surrounding glucose levels. The effect is to lower glucose, which, in turn, inhibits further insulin production. The hypothalamic–anterior pituitary–end organ axes are a slightly more complex extension of this model. The hypothalamic hormone [e.g. corticotrophin‐releasing hormone (CRH)] stimulates release of the anterior pituitary hormone (e.g. ACTH), which, in turn, increases peripheral hormone production (e.g. cortisol). The peripheral hormone then feeds back via the circulation to inhibit further production of the anterior pituitary and hypothalamic hormones. Figure 1.4b illustrates the anterior pituitary and end‐organ components of this model where hormone 1 could be ACTH and hormone 2 could be cortisol.
Positive feedback
Under certain more unusual circumstances, hormone feedback enhances, rather than inhibits, the initial response. This is called positive feedback (illustrated alongside the more usual negative feedback by the plus sign in Figure 1.4a). This is intrinsically unstable and always has built‐in self‐limiting features. Transiently, it can be beneficial. For instance, the action of oestrogen on the pituitary gland induces the ovulatory surge of LH and FSH, further stimulating oestrogen production in the developing follicle (Chapter 7). During childbirth, stretch receptors and nerves from the distended vagina stimulate the posterior pituitary to release oxytocin. The rise in oxytocin causes more uterine contraction, further activating the stretch receptors. The role of oxytocin in the suckling–milk ejection reflex is similar. In each instance, the positive feedback amplifies a signal until there is a break in the circuit, either ovulation, birth of the baby or the cessation of suckling.
Figure 1.4 Control systems regulating hormone production and circulating levels. (a) The endocrine organ releases a hormone, which acts on the target tissue to stimulate a response. The response usually feeds back to inhibit () the endocrine organ and decrease further supply of the hormone. Occasionally, the feedback can act to enhance the hormone secretion (, positive feedback). (b) In this slightly more complex scenario, the endocrine organ produces hormone 1, which acts on a second endocrine gland to release hormone 2. In turn, hormone 2 acts dually on the target tissue to induce the response and feeds back negatively onto the original endocrine organ to inhibit further release of hormone 1. This model is illustrative of the axes between the anterior pituitary and the peripheral end‐organ targets.
Box 1.5 Endocrine cycles
Circadian = 24‐h cycle
Circa = about, dies = day
Ultradian < 24‐h cycle
E.g. GnRH release
Infradian > 24‐h cycle
E.g. menstrual cycle
Inhibitory control
The secretion of some hormones is under inhibitory as well as stimulatory control. Somatostatin, a hypothalamic hormone, prevents the secretion of GH so that when somatostatin