Clinical factors affecting the determination of radiotherapy-induced skin toxicity in breast cancer

Clinical determinants of radiotoxicity

Article information

Radiat Oncol J. 2021;39(4):315-323

Publication date (electronic) : 2021 December 24

doi : https://doi.org/10.3857/roj.2020.00395

Elisa Eugenia Córdoba^,¹^,²

, Ezequiel Lacunza ³, Alba Mabel Güerci ¹^,²

¹Department of Physics, School of Exact Sciences, National University of La Plata, Argentina

²Veterinary Genetics Institute (National Scientific and Technical Research Council-National University of La Plata) School of Veterinary Sciences, La Plata, Argentina

³Basic and Applied Immunological Research Center, School of Medicine, National University of La Plata, Argentina

Correspondence: Elisa Eugenia Córdoba Veterinary Genetics Institute (National Scientific and Technical Research Council-National University of La Plata) School of Veterinary Sciences, La Plata, Calle 60 y 118 s/n (1900) La Plata, Buenos Aires, Argentina. Tel: +54-2215629081 E-mail: elisaecordoba@gmail.com

Received 2020 June 25; Revised 2021 October 9; Accepted 2021 October 19.

Abstract

Purpose

Radiotherapy is essential for the treatment of breast cancer (BC). However, adverse effects may occur in healthy tissue, during treatment and even after several months. Although it is known that this clinical radiosensitivity is multifactorial, the factors involved are unknown yet. In this study, we evaluated the effect of these factors on the development of radiodermatitis in patients undergoing radiotherapy.

Materials and Methods

Demographic and lifestyle data collected during face-to-face interviews of 122 BC patients and data from clinical records were investigated. Most patients underwent conventional three-dimensional radiotherapy treatment. A total dose of 50 Gy was administered (2 Gy/day), followed by a boost in a tumor bed with a total dose of 18 Gy (2 Gy/day). Radiotoxicity was evaluated weekly using the Radiation Therapy Oncology Group classification system (range, 0 to 4, according to the severity).

Results

In the present study, 75.4% of patients presented acute skin toxic effects with different degrees of severity. In 25% of cases, these effects manifested at the end of the fourth week at a cumulative dose of 40 Gy. The association of grade ≥2 acute skin reactions with body mass index (BMI) and breast size and between grade 3–4 and age was positive compared with controls. However, the role of the other factors could not be confirmed.

Conclusion

Analysis of the factors related to individual radiosensitivity suggests that age, BMI and breast size play an important role in the development of acute skin toxicity during treatment. Particular attention to patients who present these characteristics would help to control treatment effectiveness and therefore optimize their quality of life.

Keywords: Radiotherapy; Breast neoplasms; Radiation injuries; Radiodermatitis

Introduction

Although the quality of life of the patient is an essential component when considering cancer therapies, there are not many studies on the adverse effects of radiotherapy (RT) [1,2]. While ionizing radiation is an important tool for the treatment of several tumors, it usually induces pathological effects on healthy tissue, which limit the therapeutic dose. Since tissue radiosensitivity depends on cell proliferation, tissues with a greater regenerative capacity, such as the skin, will be more affected by irradiation [3]. In this way, it is understood that radiodermatitis is the most significant side effect of RT for breast cancer (BC) and responsible for the physical and emotional discomfort of the patient that interferes with the treatment [1,2,4].

These side effects of RT respond to a dynamic process that may include lesions of increasing complexity [5,6] and are classified according to their time of onset. Acute or early effects occur during the course of treatment or up to 6 months later and are generally reversible [7]. They manifest as erythema, dermatitis, wet or dry scaling, depilation, and ulceration [7-9]. On the other hand, late effects occur from 6 months to years after the end of the treatment, due to irreparable damage to the dermis. They include atrophy, fibrosis, telangiectasia, and pigmentation abnormalities [3,10,11].

Recent studies have emphasized the role of the RT-induced inflammatory response in the pathogenesis of normal tissue. Cellular injury resulting from oxidative stress produces infiltration of lymphocytes and macrophages with the release of various pro-inflammatory cytokines and fibroblast stimulation. This, in turn, leads to the production of reactive oxygen species (ROS) and generates a cyclical response that is perpetuated over time [12,13]. This inflammation process could be responsible for dermal edema and skin erythema due to permeability and capillary dilation. Furthermore, dryness and hair removal are the result of the destruction of sebaceous glands and hair follicles in the dermal layer. Hyperpigmented skin occurs by stimulation of epidermal melanocytes. Dry desquamation develops when stem cells from the basal layer are depleted in the treated area, while wet desquamation occurs when all stem cells are eradicated from the basal layer and are distinguished by exposure of the dermis and serous exudation. Some patients may also experience fatigue [14-16].

Despite the use of uniform protocols, this patient response ranges from mild to severe toxicity based on individual radiosensitivity [8,17,18]. Although genetic factors are elementary in their establishment and the main signaling pathways have been identified by radiogenomics, numerous elements must be considered when addressing this multifactorial trait. These are mainly related to physics (radiation dose, dose rate, inhomogeneity of dose and treatment volume), treatment (interaction with other therapies such as surgery, chemotherapy and hormonal therapy) and the patient (age, hemoglobin levels, smoking, comorbidities such as diabetes, obesity and vascular diseases) [10,18,19].

Understanding that beyond the technological advances that made it possible to improve the administration of radiation, the development of radiotoxicity in normal tissue is always possible, understanding the individual differences in this response, can allow the adaptation of medical care to the needs of each patient and thus achieve a better therapeutic result [2,20,21]. Bearing in mind the prevalence of BC in our region, the objective of this study was to expand our knowledge of the factors involved in radiotoxicity, given the profound impact that this trait can have for some patients.

Materials and Methods

1. Study sample

Patients with BC from the city of La Plata and its surroundings undergoing RT at the Instituto de Terapia Radiante, Centro Integrado de Oncología (CIO), La Plata, Argentina, were studied. The sample included 122 individuals receiving conservative treatment/post-mastectomy therapy. None of the patients had previously received RT.

Face-to-face interviews were used for patient data collection on personal, demographic and lifestyle data: age, place of birth, ethnicity, smoking habit, alcohol consumption, weight, height, size of the breast, comorbidities such as diabetes, hypertension and anemia, and family history of BC or any other type of neoplasia. Other relevant information was collected from patient clinical records.

2. Ethical considerations

The study was conducted exclusively with patients who gave their consent. Each patient was informed about the protocol of the study, both verbally and in writing in accordance with the Declaration of Helsinki, promulgated by the World Medical Association. The main project of the present study was approved by the Ad-hoc Committee of Ethics of the Human Genetics Association of the city of Mar del Plata, Buenos Aires, Argentina.

3. Radiation therapy

Most BC patients (98/122) underwent three-dimensional (3D) conservative treatment, after quadrantectomy. Whole-breast RT was delivered with a linear accelerator of 4 or 6 MV photons (Clinac; Varian Medical Systems, Palo Alto, CA, USA) in conventional 50 Gy doses fractionated in daily 2 Gy doses. The treatment was followed by a 12–18 Gy boost to the tumor bed in fractionated doses of 2 Gy/day in 85.7% of cases (84/98). Besides hypofractionated RT treatment was administered to 9/122 BC patients (after quadrantectomy) over age 60 years and at an early tumor stage in 42.56 Gy doses, fractionated at 2.66 Gy/day and without boost. Standard RT was delivered to the costal wall of 12/122 post-mastectomy patients using tangential fields as daily 1.8–2 Gy doses, up to a total dose of 50 Gy. In most cases, the axillary-supraclavicular cavity was also treated. Finally, two patients without surgical intervention were the exception: one with a conventional treatment palliative 60 Gy plus 50.4 Gy in the axillo-supraclavicular cavity and another as a pre-surgical treatment in 50 Gy doses.

4. Radiotoxicity evaluation

Acute radiotoxicity was analyzed by the team of radio-oncologists at CIO-La Plata, who weekly recorded the clinical evolution of treatment. To control the appearance of radio-induced side effects, moisturizing cream with vitamin A was prescribed. The classification system of the Radiation Therapy Oncology Group (RTOG) was used to evaluate the severity of acute skin reactions [22] (Table 1). The development of grade ≥2 acute side effects was indicative of patients with greater sensitivity, while individuals with minimal or no skin reaction (Grades 0 and 1) were included in the control group. The occurrence and severity of acute skin reactions were determined during and after the RT treatment, taking into account the highest degree of radiotoxicity for the statistical analysis. In case of pruritus or eczema, corticosteroids or allantoin were prescribed and sodium borate diluted 6:1000 was indicated to treat moist dermatitis.

Table 1.

Severity of acute skin reactions according to the EORTC/RTOG criteria

5. Statistical analysis

The association of each variable with radiodermatitis was analyzed using the χ2 test. Relative risk was estimated by calculating the odds ratio (OR) with 95% and 99% confidence intervals. Multivariate analysis was carried out using principal component analysis (PCA) [23]. The SPSS program version 22 (IBM SPSS, Armonk, NY, USA) was used for data analysis.

Results

The demographic and clinical characteristics of the study sample are shown in Table 2. Mean BC patient age was 59.6 ± 12.5 years (range, 26 to 85 years; mode, 52 and 62 years; median, 61.5 years).

Table 2.

Clinical characteristics of breast cancer patients

Analysis of BC family history showed that 38% of patients had first- and second-degree relatives with BC, while 30% reported no history of any type of oncological pathology. Ancestry data analysis revealed that 60% of patients reported a European origin, mostly Italian (33%) and Spanish (18%), followed by Amerindians (39%) and other ethnic groups (1%).

Information about the clinical manifestations of radiotoxicity recorded by radiological oncologists demonstrated that 75.4% of patients (92/122) presented acute cutaneous toxic effects with different degrees of severity, while 24.6% of women (30/122) remained without skin changes (Fig. 1). On the other hand, these side effects could be seen in 8.69% of patients (8/92) after the end of the first week of treatment together with erythema and pruritus, at a cumulative dose of 10 Gy. In 25% of cases (23/92), these effects manifested at the end of the fourth week of treatment at a dose of 40 Gy, showing a decreasing trend (9.78%, 9/92) towards the seventh week at 70 Gy. These results showed the normal distribution of this quantitative trait (Fig. 2).

Fig. 1.

Percentage of breast cancer patients with radiodermatitis developed during treatment.

Fig. 2.

Radiodermatitis associated to the dose absorbed. A large number of patients developed radiodermatitis to the approximately 40 Gy dose during the fourth week of treatment.

The association analysis of the most relevant clinical variables and radiosensitivity showed that the age range of 46.8% of patients with grade ≥2 acute radiodermatitis was 56–70 years. When we analyze the patients by degree of radiodermatitis and age, young patients (<59.6 years) and older patients (≥59.6 years), it was observed that there is a tendency to develop more severe effects with increasing to age (Fig. 3). However, it was not significant.

Fig. 3.

Percentage of old and young patients (above and below the mean age) according to the different degrees of radiodermatitis.

The association of grade ≥2 acute skin reactions with body mass index (BMI) and breast size was positive (OR = 2.87, p = 0.026 and OR = 4.62, p = 0.005, respectively). Patients with medium and large breasts showed 4.62 times higher risk of developing radiodermatitis than those with small breast. Likewise, 69% of patients who developed grade ≥2 radiodermatitis were overweight or obese (BMI >25). Obese patients presented 2.87 times more risk of manifesting radiodermatitis than patients with a normal BMI (Table 3).

Table 3.

Association of potential risk factors with skin radiotoxicity

Regarding the association of smoking habit, alcohol consumption, multivitamin intake, anemia, hypertension, diabetes, skin color, chemotherapy, tamoxifen and type of planning with development of acute radiodermatitis, no significant differences were observed between both groups of patients (p < 0.05). The PCA performed with some of these variables showed that BMI and breast size contributed to the development of acute skin radiotoxicity during RT treatment, while the contribution of the other factors could not be confirmed (Fig. 4).

Fig. 4.

Principal component analysis. There was a close relationship between patient breast size and body mass index (BMI) with radiodermatitis grade ≥2 developed during the radiotherapy treatment.

Discussion and Conclusion

Individual radiosensitivity is a complex trait with multifactorial and polygenic inheritance. Therefore, the influence of the environment on its phenotypic expression is fundamental. Radiosensitivity refers to the level of toxicity in healthy tissue of individuals subjected to RT, since the development of adverse effects in patients undergoing similar protocols is variable [8,18]. This could be attributed to cell depletion and inhibition of cell repopulation in rapidly renewing tissues, such as the skin [24,25].

Although significant efforts have been made to evaluate radiodermatitis in BC patients, evidence in the literature is scarce compared with that on other symptoms related to side effects and quality of life [26], probably because most RT medical centers do not usually carry out registry of toxicity as a routine [18]. Therefore, our attention should be focused more on obtaining detailed, accurate and complete information about study participants during a more appropriate follow-up period in order to maximize the chances of finding an association between RT-induced toxicity and its determining factors [10]. Understanding the impact of radiodermatitis on patient quality of life is essential not only for the correct management of cutaneous reactions but also for the development of trials that can predict them.

Our results are in agreement with those of Khanna et al. [27], who showed that radiodermatitis was the most commonly observed side effect during RT. Three quarters of the population analyzed presented skin toxicity, with a higher incidence of grades 1 and 2 (85%) compared with the more severe grades 3 and 4. Similarly, Schnur et al. [26] argued that most BC patients (74%) could experience radiodermatitis during the course of RT at high doses. Meanwhile, De Langhe et al. [28] estimated that 10% of cases suffered more severe effects such as moist desquamation or skin ulceration, and Pignol et al. [29] reported higher percentages of severe dermatitis (20%–25%).

The results obtained by our group showed that pruritus and erythema events occurred towards the end of the fourth week with 40 Gy doses in 25% of cases. However, these skin injuries progressed towards the first week in 8.69% of highly sensitive individuals with cumulative doses that reached 10 Gy (left side of the curve in Fig. 2). In the most tolerant individuals (9.78%), these effects were detected at doses greater than 70 Gy (right side of the curve in Fig. 2). Thus, individual radiosensitivity had a normal distribution and coincided with the theoretical description presented by Burnet et al. [30] and Barnett et al. [10].

In terms of development of RT-induced injuries, age is usually considered a risk factor [7]. However, there is contradictory evidence about its influence on the prevalence and severity of this feature [31-33]. In the present study, median age was not significantly different in patients with grade ≥2 radiotoxicity and asymptomatic patients with grade 1 radiotoxicity, arguing in favor of reports suggesting that RT is well tolerated in elderly patients [31,32]. However, when the analysis was performed in asymptomatic patients and grades 3 and 4 radiotoxicity, women older than 59 years had a higher tendency to present severe radiotoxicity (OR = 6.6; p = 0.02). Generally, advanced age is associated with a greater risk of toxicity due to the lower tolerance of healthy tissue as a result of the reduction in blood flow and DNA repair. In this regard, Lilla et al. [34] reported that the progressive reduction of functional reserves due to the depletion of tissue stem cells could increase tissue damage and the risk of complications.

Breast size was one of the first characteristics known to influence acute skin toxicity. Several studies report that it interferes with the incidence and severity of radiation of these effects [35]. Larger breasts require the application of higher radiation doses to reach the desired dose in deeper structures [32,36]. In addition, it has also been shown that BMI is associated with the development of individual radiosensitivity [9]. In this study, breast size and BMI were associated with an increased risk of developing radiodermatitis (OR = 4.62, p = 0.005 and OR= 2.87, p= 0.026, respectively). In agreement with other studies [35,37], our results corroborate that patients with medium and large breasts showed more severe skin reactions. With respect to BMI, Twardella et al. [38] reported that overweight/obesity (BMI ≥25) increased the likelihood of acute radiotoxicity. This was also seen in the current study, since obese women had 2.87 times increased risk compared with normonourished individuals, probably attributable to a lower healing efficiency due to poor vascularization of adipose tissue that compromises healing [39]. Obesity can also cause excessive wear of the skin through increased friction in movement, which would cause abrasion.

The association between smoking and radiodermatitis was not significant, probably due to the low incidence of smokers in this study (28%, 32/81). However, there is evidence that smoking increases clinical radiosensitivity in breast as well as in pelvic and head and neck cancer [35,36]. Furthermore, smoking may exacerbate radiodermatitis by impairing wound healing [40].

A study of 348 BC patients who underwent RT showed a decrease in acute skin toxicity in individuals who reported regular consumption of wine before starting treatment [41]. Our results could not corroborate such information because only 9% of the surveyed patients (10/103) drank alcohol during meals.

Among systemic diseases, diabetes mellitus and hypertension could be associated with a low tolerance to RT [18]. In the present study, despite 36% of women (42/117) were hypertensive, the severity of skin reactions was not significant. With regard to diabetes, only 12% of patients (14/117) had this condition. As reported in other studies, diabetes has not been shown to be a predisposing factor for adverse skin reactions [7,32]. In agreement with this report, Terrazzino et al. [36] indicated that there is no firm evidence that diabetes mellitus and hypertension represent predisposing factors for acute radiosensitivity [7,31].

In relation to elements concerned with RT treatment, chemotherapeutic agents are considered to enhance the effect of radiation and may increase the risk of secondary effects [42]. Although the use of RT in combination with chemotherapy improves overall survival, an increase in both acute and late toxicity is often observed. Many randomized controlled trials of chemoradiotherapy versus RT alone have shown increased acute, but not late, toxicity with the addition of chemotherapy [43]. Some drugs such as doxorubicin, actinomycin D, cisplatin, fluorouracil, apart from their own characteristic spectrum of side effects, may sensitize normal tissues to radiation damage. Such radiosensitization can occur even when chemotherapy is administered before or after the course of fractionated RT. Previous studies have shown a worse cosmetic result and higher late toxicity when chemotherapy is administered, and this seems to be more pronounced when administered simultaneously with RT [44]. In this study, despite some patients (31%, 35/113) performed neoadjuvant chemotherapy in addition to the radiant treatment, they did not present increased radiosensitivity compared with those only on RT.

Finally, the findings of this study should be considered in light of some limitations, such as, the small number of patients, and partial data obtained from other variables—estrogen receptor (ER), progesterone receptor (PR), and human epidermal growth factor receptor-2 (HER2/neu), the use of multivitamins, or certain chemotherapy drugs such as Herceptin—that were not fully available and therefore were not included in this study.

In conclusion, although it would be interesting to be able to strengthen the sampling, not only to validate the associations found but also to corroborate some suggestions made, this particular analysis of factors related to individual radiosensitivity suggests that age, BMI, and breast size play an important role in the development of acute skin toxicity during RT treatment. In consequence, the particular attention paid to these patients would help to better control treatment effectiveness and therefore optimize quality of life in oncology patients.

Notes

Conflict of Interest

No potential conflict of interest relevant to this article was reported.

Acknowledgements

The authors thank to Terapia Radiante Red CIO-La Plata for allowing data and samples collection. We also thank to A. DiMaggio for manuscript correction and editing.

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Acute radiodermatitis
Grade 0	Grade 1	Grade 2	Grade 3	Grade 4
No changes are observed	Follicular, mild diffuse erythema	Marked erythema	Confluent moist desquamation	Haemorrhages
	Epilation	Moist desquamation in circumscribed foci	Severe edema	Ulceration
	Pruritus	Moderate edema		Necrosis
	Dry desquamation
	Decreased sweating

Characteristic	Value
Age (yr)	59.6 ± 12.5 (26–85)
Sex
Female	122 (100)
Tumour location
Left breast	74 (60.7)
Right breast	48 (39.3)
Histological type of tumor
DCIS	12 (10)
LCIS	4 (3)
IDC	85 (71)
ILC	10 (8)
IDLC	6 (5)
Metaplastic	2 (2)
ITC	1 (1)
Neo-adjuvant chemotherapy
Yes	35 (31)
No	78 (69)
Tamoxifen
Yes	68 (69)
No	30 (31)
Diabetes
Yes	14 (12)
No	103 (88)
Hypertension
Yes	42 (36)
No	75 (64)
Smoking
Yes	32 (28)
No	81 (72)
Alcohol consumption^a)
Yes	10 (9)
No	103 (91)
BMI (kg/m²)
<25 (normal)	46 (41)
≥25 (overweight and obesity)	67 (59)
Breast size^b)
Small	26 (24)
Medium	49 (46)
Large	32 (30)

	n	Radiodermatitis		OR	CI	p-value
	n	Grade 0–1	Grade ≥2	OR	CI	p-value
Diabetes
No	103	64	39	1
Yes	14	9	5	0.91	0.28–2.91	0.87
Hypertension
No	75	50	25	1
Yes	42	23	19	1.2	0.76–3.58	0.20
Breast size
Small	26	22	4	1
Medium	49	28	21	4.1	1.23–13.48	0.016^*
Large	32	16	16	5.5	1.54–19.60	0.005^*
Medium-large	81	44	37	4.62	1.46–14.63	0.005^*
BMI
Normal	46	33	13	1
Overweight	35	22	13	1.5	0.58–3.83	0.39
Obesity	32	15	17	2.87	1.11–7.40	0.026^*
Skin color
Brown	74	4	4	1
Medium	31	21	10	0.68	1.69–2.88	0.42
Light	8	44	30	0.68	0.15–2.94	0.60
Medium-light	39	65	40	0.61	0.14–2.59	0.50
Chemotherapy
No	80	53	27	1
Yes	35	19	16	1.65	0.73–3.71	0.22
Type of treatment
2D	9	6	3	1
3D	113	69	44	1.27	0.30–5.36	0.73
Alcohol
No	103	65	38	1
Yes	10	5	5	1.71	0.46–6.29	0.41
Smoking
No	81	50	31	1
Yes	32	20	12	0.96	0.41–2.25	0.93